Your search keyword '"alpha interferon"' showing total 359 results

1. Hepatitis C Virus Evades Interferon Signaling by Suppressing Long Noncoding RNA Linc-Pint Involving C/EBP-β

Author

Mousumi Khatun, Ranjit Ray, Ratna B. Ray, and Jinsong Zhang

Subjects

Immunology, Cellular Response to Infection, Alpha interferon, Hepacivirus, Biology, Virus Replication, Microbiology, DEAD-box RNA Helicases, 03 medical and health sciences, Immune system, Interferon, Virology, Enhancer binding, medicine, Humans, Transcription factor, 030304 developmental biology, 0303 health sciences, Innate immune system, 030306 microbiology, CCAAT-Enhancer-Binding Protein-beta, Interferon-alpha, Interferon-beta, Hepatitis C, Immunity, Innate, Cell biology, Insect Science, Hepatocytes, IRF7, RNA, Long Noncoding, Signal transduction, medicine.drug

Abstract

Hepatitis C virus (HCV) regulates many cellular genes in modulating the host immune system for benefit of viral replication and long-term persistence in a host for chronic infection. Long noncoding RNAs (lncRNAs) play an important role in the regulation of many important cellular processes, including immune responses. We recently reported that HCV infection downregulates lncRNA Linc-Pint (long intergenic non-protein-coding RNA p53-induced transcript) expression, although the mechanism of repression and functional consequences are not well understood. In this study, we demonstrate that HCV infection of hepatocytes transcriptionally reduces Linc-Pint expression through CCAAT/enhancer binding protein β (C/EBP-β). Subsequently, we observed that the overexpression of Linc-Pint significantly upregulates interferon alpha (IFN-α) and IFN-β expression in HCV-replicating hepatocytes. Using unbiased proteomics, we identified that Linc-Pint associates with DDX24, which enables RIP1 to interact with IFN-regulatory factor 7 (IRF7) of the IFN signaling pathway. We furthermore observed that IFN-α14 promoter activity was enhanced in the presence of Linc-Pint. Together, these results demonstrated that Linc-Pint acts as a positive regulator of host innate immune responses, especially IFN signaling. HCV-mediated downregulation of Linc-Pint expression appears to be one of the mechanisms by which HCV may evade innate immunity for long-term persistence and chronicity. IMPORTANCE The mechanism by which lncRNA regulates the host immune response during HCV infection is poorly understood. We observed that Linc-Pint was transcriptionally downregulated by HCV. Using a chromatin immunoprecipitation (ChIP) assay, we showed inhibition of transcription factor C/EBP-β binding to the Linc-Pint promoter in the presence of HCV infection. We further identified that Linc-Pint associates with DDX24 for immunomodulatory function. The overexpression of Linc-Pint reduces DDX24 expression, which in turn results in the disruption of DDX24-RIP1 complex formation and the activation of IRF7. The induction of IFN-α14 promoter activity in the presence of Linc-Pint further confirms our observation. Together, our results suggest that Linc-Pint acts as a positive regulator of host innate immune responses. Downregulation of Linc-Pint expression by HCV helps in escaping the innate immune system for the development of chronicity.

Published

2021

2. Understanding Hepatitis B Virus Dynamics and the Antiviral Effect of Interferon Alpha Treatment in Humanized Chimeric Mice

Author

Tje Lin Chung, Susan L. Uprichard, Harel Dahari, Karina Durso-Cain, Kazuaki Chayama, Vladimir Reinharz, Masataka Tsuge, Alan S. Perelson, Yuji Ishida, and Chise Tateno

Subjects

Male, Hepatitis B virus, Immunology, Alpha interferon, Mice, SCID, Biology, medicine.disease_cause, Microbiology, Antiviral Agents, Virus, Polyethylene Glycols, 03 medical and health sciences, 0302 clinical medicine, Virology, medicine, Animals, Humans, Secretion, Mode of action, Serum Albumin, 030304 developmental biology, 0303 health sciences, Transplantation Chimera, Lamivudine, virus diseases, Infant, Interferon-alpha, Models, Theoretical, Acquired immune system, Hepatitis B, digestive system diseases, Recombinant Proteins, Virus-Cell Interactions, Liver Transplantation, Disease Models, Animal, Kinetics, Insect Science, Child, Preschool, DNA, Viral, 030211 gastroenterology & hepatology, Female, Intracellular, medicine.drug

Abstract

Whereas the mode of action of lamivudine (LAM) against hepatitis B virus (HBV) is well established, the inhibition mechanism(s) of interferon alpha (IFN-α) is less completely defined. To advance our understanding, we mathematically modeled HBV kinetics during 14-day pegylated IFN-α-2a (pegIFN), LAM, or pegIFN-plus-LAM (pegIFN+LAM) treatment of 39 chronically HBV-infected humanized uPA/SCID chimeric mice. Serum HBV DNA and intracellular HBV DNA were measured frequently. We developed a multicompartmental mathematical model and simultaneously fit it to the serum and intracellular HBV DNA data. Unexpectedly, even in the absence of an adaptive immune response, a biphasic decline in serum HBV DNA and intracellular HBV DNA was observed in response to all treatments. Kinetic analysis and modeling indicate that the first phase represents inhibition of intracellular HBV DNA synthesis and secretion, which was similar under all treatments with an overall mean efficacy of 98%. In contrast, there were distinct differences in HBV decline during the second phase, which was accounted for in the model by a time-dependent inhibition of intracellular HBV DNA synthesis, with the steepest decline observed during pegIFN+LAM treatment (1.28/day) and the slowest (0.1/day) during pegIFN monotherapy. Reminiscent of observations in patients treated with pegIFN and/or LAM, a biphasic HBV decline was observed in treated humanized mice in the absence of an adaptive immune response. Interestingly, combination treatment did not increase the initial inhibition of HBV production but rather enhanced second-phase decline, providing insight into the dynamics of HBV treatment response and the mode of action of IFN-α against HBV. IMPORTANCE Chronic hepatitis B virus (HBV) infection remains a global health care problem, as we lack sufficient curative treatment options. Elucidating the dynamics of HBV infection and treatment response at the molecular level could facilitate the development of novel, more effective HBV antivirals. Currently, the only well-established small animal HBV infection model available is the chimeric uPA/SCID mice with humanized livers; however, the HBV inhibition kinetics under pegylated IFN-α-2a (pegIFN) in this model system have not been determined in sufficient detail. In this study, viral kinetics in 39 humanized mice treated with pegIFN and/or lamivudine were monitored and analyzed using a mathematical modeling approach. We found that the main mode of action of IFN-α is blocking HBV DNA synthesis and that the majority of synthesized HBV DNA is secreted. Our study provides novel insights into HBV DNA dynamics within infected human hepatocytes.

Published

2021

3. Efficacy of a Cap-Dependent Endonuclease Inhibitor and Neuraminidase Inhibitors against H7N9 Highly Pathogenic Avian Influenza Virus Causing Severe Viral Pneumonia in Cynomolgus Macaques

Author

Yasushi Itoh, Hiroyuki Osaka, Yoshihiro Sakoda, Kazumasa Ogasawara, Hirohito Ishigaki, Akihiro Shibata, Ayako Ogata-Nakahara, Masatoshi Okamatsu, Cong Thanh Nguyen, Saori Suzuki, and Hiroshi Kida

Subjects

Oseltamivir, medicine.drug_class, Pneumonia, Viral, Neuraminidase, Alpha interferon, Influenza A Virus, H7N9 Subtype, Antiviral Agents, Macaque, Virus, 03 medical and health sciences, chemistry.chemical_compound, Zanamivir, Orthomyxoviridae Infections, biology.animal, Influenza, Human, medicine, Animals, Humans, Pharmacology (medical), 030304 developmental biology, Pharmacology, 0303 health sciences, biology, Neuraminidase inhibitor, 030306 microbiology, Endonucleases, medicine.disease, Virology, Macaca fascicularis, Infectious Diseases, chemistry, Influenza in Birds, Viral pneumonia, biology.protein, Chickens, medicine.drug

Abstract

H7N9 highly pathogenic avian influenza virus (HPAIV) infection in a human was first reported in 2017. A/duck/Japan/AQ-HE29-22/2017 (H7N9) (Dk/HE29-22), found in imported duck meat at an airport in Japan, possesses a hemagglutinin with a multibasic cleavage site, indicating high pathogenicity in chickens, as in the case of other H7 HPAIVs. In the present study, we examined the pathogenicity of Dk/HE29-22 and the effectiveness of a cap-dependent endonuclease inhibitor (baloxavir) and neuraminidase inhibitors (oseltamivir and zanamivir) against infection with this strain in a macaque model (n = 3 for each group). All of the macaques infected with Dk/HE29-22 showed severe signs of disease and pneumonia even after the virus had disappeared from lung samples. Virus titers in macaques treated with baloxavir were significantly lower than those in the other treated groups. After infection, levels of interferon alpha and beta (IFN-α and IFN-β) in the blood of macaques in the baloxavir group were the highest among the groups, whereas levels of tumor necrosis factor alpha (TNF-α) and interleukin 13 (IL-13) were slightly increased in the untreated group. In addition, immune checkpoint proteins, including programmed death 1 (PD-1) and T cell immunoreceptor with Ig and ITIM domains (TIGIT), were expressed at high levels in the untreated group, especially in one macaque that showed severe signs of disease, indicating that negative feedback responses against vigorous inflammation may contribute to disease progression. In the group treated with baloxavir, the percentages of PD-1-, CTLA-4-, and TIGIT-positive T lymphocytes were lower than those in the untreated group, indicating that reduction in virus titers may prevent expression of immune checkpoint molecules from downregulation of T cell responses.

Published

2021

4. Comparative Study of Protection against Newcastle Disease in Young Broilers Administered Natural Chicken Alpha Interferon via Oral and Intramuscular Routes

Author

Sajjad Ur Rahman, Muhammad Aamir Aslam, Anas Sarwar Qureshi, and Faisal Rasheed Anjum

Subjects

0301 basic medicine, 040301 veterinary sciences, Newcastle disease virus, lcsh:QR1-502, Administration, Oral, Alpha interferon, chicken IFN-α, Spleen, Disease, Virus Replication, Injections, Intramuscular, Microbiology, Newcastle disease, lcsh:Microbiology, Virus, 0403 veterinary science, 03 medical and health sciences, Animals, Immunologic Factors, Medicine, innate immunity, Molecular Biology, Innate immune system, biology, business.industry, Broiler, Interferon-alpha, 04 agricultural and veterinary sciences, Therapeutics and Prevention, biology.organism_classification, Immunity, Innate, QR1-502, Immunity, Humoral, Virus Shedding, Vaccination, therapeutic, 030104 developmental biology, medicine.anatomical_structure, Immunology, business, Chickens, Research Article

Abstract

Newcastle disease (ND) is an economically important contagious disease of wild and domestic birds worldwide. The disease causes severe economic losses in terms of production due to high mortality and morbidity in nonvaccinated chickens. Despite extensive vaccination approaches, Newcastle disease (ND) remains a permanent threat to the poultry industry worldwide. In the current study, we used natural chicken IFN-α as an innate immune modulator to counteract ND in chickens. We report that chIFN-α is effective in protecting the chickens against ND and also prevents shedding of the virus, which can then prevent further spread of the disease. We propose that in addition to vaccination, chIFN-α therapy could be an effective option for controlling ND in areas of endemicity., Despite extensive vaccination approaches, Newcastle disease (ND) remains a permanent threat to the poultry industry worldwide. Besides vaccination, there is a burgeoning demand for new antivirals for use in interventions to control ND. One strategy is to strengthen the host innate immunity via host-derived innate immune proteins. Type I interferons define one of the first lines of innate immune defense against viral infections. Chicken interferon alpha (chIFN-α) is one of the potent cytokines that trigger antiviral responses. In the current study, we investigated the therapeutic effect of natural chIFN-α administered via oral and intramuscular (i.m.) routes against ND in broiler chickens. Our results showed that the level of protection against ND in response to chIFN-α therapy was dependent on the route and dose of IFN administration. A better therapeutic effect was observed in chickens treated with chIFN-α via the oral route than in those treated via the i.m. route. Regardless of the administration route, double-dose chIFN-α (2,000-U) treatments provided better protection than single-dose (1,000-U) treatments. However, complete protection against ND was achieved in birds treated with repeated doses of chIFN-α via the oral route. Histopathology of trachea, proventriculus, spleen, and liver showed a significant improvement in ND-induced degenerative changes in double-dose IFN-treatment groups compared to single-dose groups. Results of the hemagglutination test demonstrated a decrease in ND virus (NDV) titer in IFN-treated groups. Also, double doses of chIFN-α via oral route resulted in early recovery in weight gain. We propose that chIFN-α therapy via oral route could be an important therapeutic tool to control NDV infection in chicken. IMPORTANCE Newcastle disease (ND) is an economically important contagious disease of wild and domestic birds worldwide. The disease causes severe economic losses in terms of production due to high mortality and morbidity in nonvaccinated chickens. Despite extensive vaccination approaches, Newcastle disease (ND) remains a permanent threat to the poultry industry worldwide. In the current study, we used natural chicken IFN-α as an innate immune modulator to counteract ND in chickens. We report that chIFN-α is effective in protecting the chickens against ND and also prevents shedding of the virus, which can then prevent further spread of the disease. We propose that in addition to vaccination, chIFN-α therapy could be an effective option for controlling ND in areas of endemicity.

Published

2020

5. Interferon Alpha Induces Multiple Cellular Proteins That Coordinately Suppress Hepadnaviral Covalently Closed Circular DNA Transcription

Author

Muhammad Sheraz, Jinhong Chang, Ju-Tao Guo, Junjun Cheng, Qiong Zhao, Yan Zhou, and Liudi Tang

Subjects

Hepatitis B virus, Transcription, Genetic, Chromosomal Proteins, Non-Histone, Immunology, Alpha interferon, Promyelocytic Leukemia Protein, Biology, Hepadnaviridae, Virus Replication, Antiviral Agents, Microbiology, Cell Line, Epigenesis, Genetic, Hepatitis B Virus, Duck, Histones, 03 medical and health sciences, Hepatitis B, Chronic, 0302 clinical medicine, Transcription (biology), Virology, Gene expression, Animals, Humans, Gene silencing, STAT1, 030304 developmental biology, 0303 health sciences, Interferon-alpha, cccDNA, Hepadnaviridae Infections, Virus-Cell Interactions, Cell biology, Histone Code, STAT1 Transcription Factor, Histone, Insect Science, DNA, Viral, Hepatocytes, biology.protein, STAT protein, RNA, Viral, 030211 gastroenterology & hepatology, DNA, Circular, Chickens, Protein Processing, Post-Translational

Abstract

Covalently closed circular DNA (cccDNA) of hepadnaviruses exists as an episomal minichromosome in the nucleus of an infected hepatocyte and serves as the template for the transcription of viral mRNAs. It had been demonstrated by others and us that interferon alpha (IFN-α) treatment of hepatocytes induced a prolonged suppression of human and duck hepatitis B virus cccDNA transcription, which is associated with the reduction of cccDNA-associated histone modifications specifying active transcription (H3K9(ac) or H3K27(ac)), but not the histone modifications marking constitutive (H3K9(me3)) or facultative (H3K27(me3)) heterochromatin formation. In our efforts to identify IFN-induced cellular proteins that mediate the suppression of cccDNA transcription by the cytokine, we found that downregulating the expression of signal transducer and activator of transcription 1 (STAT1), structural maintenance of chromosomes flexible hinge domain containing 1 (SMCHD1), or promyelocytic leukemia (PML) protein increased basal level of cccDNA transcription activity and partially attenuated IFN-α suppression of cccDNA transcription. In contrast, ectopic expression of STAT1, SMCHD1, or PML significantly reduced cccDNA transcription activity. SMCHD1 is a noncanonical SMC family protein and implicated in epigenetic silencing of gene expression. PML is a component of nuclear domain 10 (ND10) and is involved in suppressing the replication of many DNA viruses. Mechanistic analyses demonstrated that STAT1, SMCHD1, and PML were recruited to cccDNA minichromosomes and phenocopied the IFN-α-induced posttranslational modifications of cccDNA-associated histones. We thus conclude that STAT1, SMCHD1, and PML may partly mediate the suppressive effect of IFN-α on hepadnaviral cccDNA transcription. IMPORTANCE Pegylated IFN-α is the only therapeutic regimen that can induce a functional cure of chronic hepatitis B in a small, but significant, fraction of treated patients. Understanding the mechanisms underlying the antiviral functions of IFN-α in hepadnaviral infection may reveal molecular targets for development of novel antiviral agents to improve the therapeutic efficacy of IFN-α. By a loss-of-function genetic screening of individual IFN-stimulated genes (ISGs) on hepadnaviral mRNAs transcribed from cccDNA, we found that downregulating the expression of STAT1, SMCHD1, or PML significantly increased the level of viral RNAs without altering the level of cccDNA. Mechanistic analyses indicated that those cellular proteins are recruited to cccDNA minichromosomes and induce the posttranslational modifications of cccDNA-associated histones similar to those induced by IFN-α treatment. We have thus identified three IFN-α-induced cellular proteins that suppress cccDNA transcription and may partly mediate IFN-α silencing of hepadnaviral cccDNA transcription.

Published

2020

6. Patterns of Herpes Simplex Virus 1 Infection in Neural Progenitor Cells

Author

David C. Bloom, Jennifer N. Naciri, Jason Yeung, Wenxiao Zheng, Jadranka Milosevic, Vishwajit L. Nimgaonkar, Matthew Demers, Leonardo D'Aiuto, Paul R. Kinchington, and Alissa M. Klammer

Subjects

cognition, viruses, neural progenitor cells (NPCs), Immunology, Central nervous system, Alpha interferon, Biology, medicine.disease_cause, Microbiology, 03 medical and health sciences, 0302 clinical medicine, Virology, Neurosphere, neurospheres, otorhinolaryngologic diseases, medicine, Gene silencing, 030304 developmental biology, 0303 health sciences, Neurogenesis, Neural stem cell, Virus-Cell Interactions, Cell biology, stomatognathic diseases, Herpes simplex virus, medicine.anatomical_structure, Lytic cycle, Insect Science, brivudin, acyclovir, herpes simplex virus 1 (HSV-1), 030217 neurology & neurosurgery

Abstract

This study employed human induced pluripotent stem cells (hiPSCs) to model the interaction of HSV-1 with NPCs, which reside in the neurogenic niches of the CNS and play a fundamental role in adult neurogenesis. Herein, we provide evidence that in NPCs infected at an MOI as low as 0.001, HSV-1 can establish a latent state, suggesting that (i) a variant of classical HSV-1 latency can be established during earlier stages of neuronal differentiation and (ii) neurogenic niches in the brain may constitute additional sites of viral reactivation. Lytic HSV-1 infections impaired NPC migration, which represents a critical step in neurogenesis. A difference in susceptibility to HSV-1 infection between two-dimensional (2D) and three-dimensional (3D) NPC cultures was observed, highlighting the potential value of 3D cultures for modeling host-pathogen interactions. Together, our results are relevant in light of observations relating HSV-1 infection to postencephalitic cognitive dysfunction., Herpes simplex virus 1 (HSV-1) can induce damage in brain regions that include the hippocampus and associated limbic structures. These neurogenic niches are important because they are associated with memory formation and are highly enriched with neural progenitor cells (NPCs). The susceptibility and fate of HSV-1-infected NPCs are largely unexplored. We differentiated human induced pluripotent stem cells (hiPSCs) into NPCs to generate two-dimensional (2D) and three-dimensional (3D) culture models to examine the interaction of HSV-1 with NPCs. Here, we show that (i) NPCs can be efficiently infected by HSV-1, but infection does not result in cell death of most NPCs, even at high multiplicities of infection (MOIs); (ii) limited HSV-1 replication and gene expression can be detected in the infected NPCs; (iii) a viral silencing mechanism is established in NPCs exposed to the antivirals (E)-5-(2-bromovinyl)-2′-deoxyuridine (5BVdU) and alpha interferon (IFN-α) and when the antivirals are removed, spontaneous reactivation can occur at low frequency; (iv) HSV-1 impairs the ability of NPCs to migrate in a dose-dependent fashion in the presence of 5BVdU plus IFN-α; and (v) 3D cultures of NPCs are less susceptible to HSV-1 infection than 2D cultures. These results suggest that NPC pools could be sites of HSV-1 reactivation in the central nervous system (CNS). Finally, our results highlight the potential value of hiPSC-derived 3D cultures to model HSV-1–NPC interaction. IMPORTANCE This study employed human induced pluripotent stem cells (hiPSCs) to model the interaction of HSV-1 with NPCs, which reside in the neurogenic niches of the CNS and play a fundamental role in adult neurogenesis. Herein, we provide evidence that in NPCs infected at an MOI as low as 0.001, HSV-1 can establish a latent state, suggesting that (i) a variant of classical HSV-1 latency can be established during earlier stages of neuronal differentiation and (ii) neurogenic niches in the brain may constitute additional sites of viral reactivation. Lytic HSV-1 infections impaired NPC migration, which represents a critical step in neurogenesis. A difference in susceptibility to HSV-1 infection between two-dimensional (2D) and three-dimensional (3D) NPC cultures was observed, highlighting the potential value of 3D cultures for modeling host-pathogen interactions. Together, our results are relevant in light of observations relating HSV-1 infection to postencephalitic cognitive dysfunction.

Published

2020

7. Can Unconventional Immunomodulatory Agents Help Alleviate COVID-19 Symptoms and Severity?

Author

Steven Krakowka, Kara Fitzgerald, Ryan G. Rhodes, Sunthorn Pond-Tor, John Mcmichael, Jeffrey L. Osborn, Albert E. Dahlberg, Sarah Beseme, Lloyd Saberski, Stephen W. Mamber, and Neal Wright

Subjects

0301 basic medicine, Chemokine, viruses, Phytochemicals, Pneumonia, Viral, lcsh:QR1-502, Alpha interferon, Disease, Microbiology, lcsh:Microbiology, Proinflammatory cytokine, Immunomodulation, Betacoronavirus, 03 medical and health sciences, 0302 clinical medicine, Immune system, Interferon, Humans, interferon alpha, Medicine, CXCL10, phytocannabinoids, thimerosal, Pandemics, Molecular Biology, biology, Cannabinoids, SARS-CoV-2, business.industry, virus diseases, Interferon-alpha, COVID-19, Respiratory infection, DNA, Opinion/Hypothesis, Therapeutics and Prevention, QR1-502, COVID-19 Drug Treatment, immunomodulatory agents, 030104 developmental biology, Immunology, biology.protein, Cytokines, Coronavirus Infections, business, 030215 immunology, medicine.drug

Abstract

Severe acute respiratory syndrome coronavirus 2 (SARS coronavirus 2, or SARS-CoV-2) is the cause of the respiratory infection known as COVID-19. From an immunopathological standpoint, coronaviruses such as SARS-CoV-2 induce increased levels of a variety of T-helper 1 (Th1) and inflammatory cytokines and chemokines, including interleukin-1 (IL-1), IL-6, CCL2 protein, and CXCL10 protein. In the absence of proven antiviral agents or an effective vaccine, substances with immunomodulatory activity may be able to inhibit inflammatory and Th1 cytokines and/or yield an anti-inflammatory and/or Th2 immune response to counteract COVID-19 symptoms and severity., Severe acute respiratory syndrome coronavirus 2 (SARS coronavirus 2, or SARS-CoV-2) is the cause of the respiratory infection known as COVID-19. From an immunopathological standpoint, coronaviruses such as SARS-CoV-2 induce increased levels of a variety of T-helper 1 (Th1) and inflammatory cytokines and chemokines, including interleukin-1 (IL-1), IL-6, CCL2 protein, and CXCL10 protein. In the absence of proven antiviral agents or an effective vaccine, substances with immunomodulatory activity may be able to inhibit inflammatory and Th1 cytokines and/or yield an anti-inflammatory and/or Th2 immune response to counteract COVID-19 symptoms and severity. This report briefly describes the following four unconventional but commercially accessible immunomodulatory agents that can be employed in clinical trials to evaluate their effectiveness at alleviating disease symptoms and severity: low-dose oral interferon alpha, microdose DNA, low-dose thimerosal, and phytocannabinoids.

Published

2020

8. Efficacy of Neuraminidase Inhibitors against H5N6 Highly Pathogenic Avian Influenza Virus in a Nonhuman Primate Model

Author

Cong Thanh Nguyen, Saori Suzuki, Misako Nakayama, Kazumasa Ogasawara, Yasushi Itoh, Masatoshi Okamatsu, Kaori Hayashi, Keita Matsuno, Yoshihiro Sakoda, Hirohito Ishigaki, and Hiroshi Kida

Subjects

Primates, Oseltamivir, medicine.drug_class, animal diseases, Neuraminidase, Alpha interferon, Lung injury, medicine.disease_cause, Antiviral Agents, Virus, 03 medical and health sciences, chemistry.chemical_compound, Influenza, Human, medicine, Influenza A virus, Animals, Pharmacology (medical), Phylogeny, 030304 developmental biology, Pharmacology, 0303 health sciences, biology, 030306 microbiology, business.industry, virus diseases, Virology, Infectious Diseases, chemistry, Influenza in Birds, biology.protein, Peramivir, Antiviral drug, business, medicine.drug

Abstract

Antimicrobial agents and chemotherapy. 2020 Jun 23;64(7):e02561-19., 令和2年度

Published

2020

9. Epstein-Barr Virus (EBV) Tegument Protein BGLF2 Suppresses Type I Interferon Signaling To Promote EBV Reactivation

Author

Tammy Krogmann, Tomohiko Sadaoka, Xueqiao Liu, and Jeffrey I. Cohen

Subjects

STAT3 Transcription Factor, Epstein-Barr Virus Infections, Herpesvirus 4, Human, viruses, Interferon Regulatory Factor-7, Immunology, Alpha interferon, medicine.disease_cause, Microbiology, 03 medical and health sciences, Interferon-gamma, 0302 clinical medicine, Interferon, Virology, medicine, Humans, STAT1, 030304 developmental biology, TYK2 Kinase, 0303 health sciences, biology, Epstein–Barr virus, BZLF1, Virus-Cell Interactions, IRF1, HEK293 Cells, STAT1 Transcription Factor, Type I interferon signaling pathway, 030220 oncology & carcinogenesis, Insect Science, Interferon Type I, biology.protein, IRF7, Virus Activation, Viral Fusion Proteins, medicine.drug, Interferon Regulatory Factor-1, Signal Transduction

Abstract

Interferon alpha (IFN-α) and IFN-β are type I IFNs that are induced by virus infection and are important in the host’s innate antiviral response. EBV infection activates multiple cell signaling pathways, resulting in the production of type I IFN which inhibits EBV infection and virus-induced B-cell transformation. We reported previously that EBV tegument protein BGLF2 activates p38 and enhances EBV reactivation. To further understand the role of BGLF2 in EBV infection, we used mass spectrometry to identify cellular proteins that interact with BGLF2. We found that BGLF2 binds to Tyk2 and confirmed this interaction by coimmunoprecipitation. BGLF2 blocked type I IFN-induced Tyk2, STAT1, and STAT3 phosphorylation and the expression of IFN-stimulated genes (ISGs) IRF1, IRF7, and MxA. In contrast, BGLF2 did not inhibit STAT1 phosphorylation induced by IFN-γ. Deletion of the carboxyl-terminal 66 amino acids of BGLF2 reduced the ability of the protein to repress type I IFN signaling. Treatment of gastric carcinoma and Raji cells with IFN-α blocked BZLF1 expression and EBV reactivation; however, expression of BGLF2 reduced the ability of IFN-α to inhibit BZLF1 expression and enhanced EBV reactivation. In summary, EBV BGLF2 interacts with Tyk2, inhibiting Tyk2, STAT1, and STAT3 phosphorylation and impairs type I IFN signaling; BGLF2 also counteracts the ability of IFN-α to suppress EBV reactivation. IMPORTANCE Type I interferons are important for controlling virus infection. We have found that the Epstein-Barr virus (EBV) BGLF2 tegument protein binds to a protein in the type I interferon signaling pathway Tyk2 and inhibits the expression of genes induced by type I interferons. Treatment of EBV-infected cells with type I interferon inhibits reactivation of the virus, while expression of EBV BGLF2 reduces the ability of type I interferon to inhibit virus reactivation. Thus, a tegument protein delivered to cells during virus infection inhibits the host’s antiviral response and promotes virus reactivation of latently infected cells. Therefore, EBV BGLF2 might protect virus-infected cells from the type I interferon response in cells undergoing lytic virus replication.

Published

2020

10. Macromolecular Synthesis Shutoff Resistance by Myeloid Cells Is Critical to IRF7-Dependent Systemic Interferon Alpha/Beta Induction after Alphavirus Infection

Author

Sierra N Downs, Matthew D. Dunn, William B. Klimstra, Nishank Bhalla, Chengqun Sun, and Christina L. Gardner

Subjects

Myeloid, Macromolecular Substances, Interferon Regulatory Factor-7, Immunology, Cell, Alpha interferon, Alphavirus, Biology, Virus Replication, Microbiology, Cell Line, Encephalitis Virus, Venezuelan Equine, Mice, Virology, medicine, Animals, Humans, Myeloid Cells, Mice, Knockout, Alphavirus Infections, Interferon-alpha, Interferon-beta, Fibroblasts, biology.organism_classification, Virus-Cell Interactions, Disease Models, Animal, RAW 264.7 Cells, medicine.anatomical_structure, Cell culture, Insect Science, IRF7, Interferon Regulatory Factor-3, IRF3, Interferon regulatory factors

Abstract

Alphavirus infection of fibroblastic cell types in vitro inhibits host cell translation and transcription, leading to suppression of interferon alpha/beta (IFN-α/β) production. However, the effect of infection upon myeloid cells, which are often the first cells encountered by alphaviruses in vivo, is unclear. Previous studies demonstrated an association of systemic IFN-α/β production with myeloid cell infection efficiency. Murine infection with wild-type Venezuelan equine encephalitis virus (VEEV), a highly myeloid-cell-tropic alphavirus, results in secretion of very high systemic levels of IFN-α/β, suggesting that stress responses in responding cells are active. Here, we infected myeloid cell cultures with VEEV to identify the cellular source of IFN-α/β, the timing and extent of translation and/or transcription inhibition in infected cells, and the transcription factors responsible for IFN-α/β induction. In contrast to fibroblast infection, myeloid cell cultures infected with VEEV secreted IFN-α/β that increased until cell death was observed. VEEV inhibited translation in most cells early after infection (6 h p.i.). Furthermore, the interferon regulatory factor 7 (IRF7), but not IRF3, transcription factor was critical for IFN-α/β induction in vitro and in sera of mice. We identified a subset of infected Raw 264.7 myeloid cells that resisted VEEV-induced translation inhibition and secreted IFN-α/β despite virus infection. However, in the absence of IFN receptor signaling, the size of this cell population was diminished. These results indicate that IFN-α/β induction in vivo is IRF7 dependent and arises in part from a subset of myeloid cells that are resistant, in an IFN-α/β-dependent manner, to VEEV-induced macromolecular synthesis inhibition. IMPORTANCE Most previous research exploring the interaction of alphaviruses with host cell antiviral responses has been conducted using fibroblast lineage cell lines. Previous studies have led to the discovery of virus-mediated activities that antagonize host cell antiviral defense pathways, such as host cell translation and transcription inhibition and suppression of STAT1 signaling. However, their relevance and impact upon myeloid lineage cell types, which are key responders during the initial stages of alphavirus infection in vivo, have not been well studied. Here, we demonstrate the different abilities of myeloid cells to resist VEEV infection compared to nonmyeloid cell types and begin to elucidate the mechanisms by which host antiviral responses are upregulated in myeloid cells despite the actions of virus-encoded antagonists.

Published

2019

11. Activation of RNase L in Egyptian Rousette Bat-Derived RoNi/7 Cells Is Dependent Primarily on OAS3 and Independent of MAVS Signaling

Author

Yize Li, Robert H. Silverman, Zuzhang Wei, Susan R. Weiss, and Beihua Dong

Subjects

oas-rnase, Sindbis virus, RNase P, Alpha interferon, Gene Expression, rousettus aegyptiacus, Biology, Microbiology, Catalysis, Host-Microbe Biology, Cell Line, 03 medical and health sciences, Mice, egyptian rousette, Interferon, Virology, Chiroptera, Endoribonucleases, medicine, 2',5'-Oligoadenylate Synthetase, Animals, Humans, Amino Acid Sequence, Promoter Regions, Genetic, 030304 developmental biology, Adaptor Proteins, Signal Transducing, oas-rnase l, 0303 health sciences, Binding Sites, bat innate immunity, 030302 biochemistry & molecular biology, RNA, biology.organism_classification, QR1-502, 3. Good health, RNA silencing, MRNA Sequencing, Viral replication, Egypt, Biomarkers, medicine.drug, Research Article, Protein Binding, Signal Transduction, dsrna-induced pathways

Abstract

Many RNA viruses that are highly pathogenic in humans are relatively apathogenic in their bat reservoirs, making it important to compare innate immune responses in bats to those well characterized in humans. One such antiviral response is the OAS-RNase L pathway. OASs, upon sensing dsRNA, produce 2-5A, leading to activation of RNase L which degrades viral and host RNA, limiting viral replication. Analysis of Egyptian Rousette bat sequences revealed three OAS genes expressing OAS1, OAS2, and OAS3 proteins. Interferon treatment or viral infection induces all three bat OAS mRNAs. In these bat cells as in human cells, RNase L activation and its antiviral activity are dependent primarily on OAS3 while MAVS signaling is not required. Importantly, our findings indicate the OAS-RNase L system is a primary response to virus rather than a secondary effect of interferon signaling and therefore can be activated early in infection or while interferon signaling is antagonized., Bats are reservoirs for many RNA viruses that are highly pathogenic in humans yet relatively apathogenic in the natural host. It has been suggested that differences in innate immunity are responsible. The antiviral OAS-RNase L pathway is well characterized in humans, but there is little known about its activation and antiviral activity in bats. During infection, OASs, upon sensing double-stranded RNA (dsRNA), produce 2′-5′ oligoadenylates (2-5A), leading to activation of RNase L which degrades viral and host RNA, limiting viral replication. Humans encode three active OASs (OAS1 to -3). Analysis of the Egyptian Rousette bat genome combined with mRNA sequencing from bat RoNi/7 cells revealed three homologous OAS proteins. Interferon alpha treatment or viral infection induced all three OAS mRNAs, but RNase L mRNA is constitutively expressed. Sindbis virus (SINV) or vaccinia virus (VACVΔE3L) infection of wild-type (WT) or OAS1-KO (knockout), OAS2-KO, or MAVS-KO RoNi/7 cells, but not RNase L-KO or OAS3-KO cells, induces robust RNase L activation. SINV replication is 100- to 200-fold higher in the absence of RNase L or OAS3 than in WT cells. However, MAVS-KO had no detectable effect on RNA degradation or replication. Thus, in RoNi/7 bat cells, as in human cells, activation of RNase L during infection and its antiviral activity are dependent primarily on OAS3 while MAVS signaling is not required for the activation of RNase L and restriction of infection. Our findings indicate that OAS proteins serve as pattern recognition receptors (PRRs) to recognize viral dsRNA and that this pathway is a primary response to virus rather than a secondary effect of interferon signaling.

Published

2019

12. Avian Flavivirus Infection of Monocytes/Macrophages by Extensive Subversion of Host Antiviral Innate Immune Responses

Author

Lu Cui, Shengwang Liu, Nana Wang, Hanguang Wu, Hai Li, Yumeng Liang, Zhijie Chen, Chenyang Zhu, Yong Ma, and Zhitao Wang

Subjects

China, viruses, Immunology, Alpha interferon, Virus Replication, Microbiology, Arbovirus, Host Specificity, Monocytes, Flavivirus Infections, Virology, medicine, Animals, Tropism, Poultry Diseases, Innate immune system, biology, Monocyte, Flavivirus, Macrophages, Pattern recognition receptor, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, medicine.disease, Immunity, Innate, medicine.anatomical_structure, Ducks, Viral replication, Insect Science, Host-Pathogen Interactions, Pathogenesis and Immunity, Female, Chickens

Abstract

Avian Tembusu virus (TMUV) is a newly emerging avian pathogenic flavivirus in China and Southeast Asia with features of rapid spread, an expanding host range, and cross-species transmission. The mechanisms of its infection and pathogenesis remain largely unclear. Here, we investigated the tropism of this arbovirus in peripheral blood mononuclear cells of specific-pathogen-free (SPF) ducks and SPF chickens and identified monocytes/macrophages as the key targets of TMUV infection. In vivo studies in SPF ducks and SPF chickens with monocyte/macrophage clearance demonstrated that the infection of monocytes/macrophages was crucial for viral replication, transmission, and pathogenesis. Further genome-wide transcriptome analyses of TMUV-infected chicken macrophages revealed that host antiviral innate immune barriers were the major targets of TMUV in macrophages. Despite the activation of major pattern recognition receptor signaling, the inductions of alpha interferon (IFN-α) and IFN-β were blocked by TMUV infection on transcription and translation levels, respectively. Meanwhile, TMUV inhibited host redox responses by repressing the transcription of genes encoding NADPH oxidase subunits and promoting Nrf2-mediated antioxidant responses. The recovery of either of the above-mentioned innate immune barriers was sufficient to suppress TMUV infection. Collectively, we identify an essential step of TMUV infection and reveal extensive subversion of host antiviral innate immune responses. IMPORTANCE Mosquito-borne flaviviruses include a group of pathogenic viruses that cause serious diseases in humans and animals, including dengue, West Nile, and Japanese encephalitis viruses. These flaviviruses are zoonotic and use animals, including birds, as amplifying and reservoir hosts. Avian Tembusu virus (TMUV) is an emerging mosquito-borne flavivirus that is pathogenic for many avian species and can infect cells derived from mammals and humans in vitro. Although not currently pathogenic for primates, the infection of duck industry workers and the potential risk of TMUV infection in immunocompromised individuals have been highlighted. Thus, the prevention of TMUV in flocks is important for both avian and mammalian health. Our study reveals the escape of TMUV from the first line of the host defense system in the arthropod-borne transmission route of arboviruses, possibly helping to extend our understanding of flavivirus infection in birds and refine the design of anti-TMUV therapeutics.

Published

2019

13. Reply to Hasenkrug et al., 'Different Biological Activities of Specific Interferon Alpha Subtypes'

Author

Stefan P. Kuster, Maarja Gruenbach, Roberto F. Speck, Erika Schlaepfer, Viviana Simon, Gideon Schreiber, Audrey Fahrny, University of Zurich, and Speck, Roberto F

Subjects

Author Reply, Biological Products, 2404 Microbiology, Human immunodeficiency virus (HIV), Interferon-alpha, Alpha interferon, 610 Medicine & health, HIV Infections, Biology, medicine.disease_cause, Antiviral Agents, Microbiology, Virology, QR1-502, Host-Microbe Biology, 10234 Clinic for Infectious Diseases, Interferon Type I, Replication (statistics), 1312 Molecular Biology, medicine, Humans, Molecular Biology

Abstract

We appreciate the reply by Hasenkrug et al. The basic issue we addressed in our paper was whether the differences between the different interferon alpha (IFN-α) subtypes are quantitative or qualitative. In our paper, we noted that all of the IFN-α subtypes are able to inhibit HIV replication in

Published

2019

14. Different Biological Activities of Specific Interferon Alpha Subtypes

Author

Ulf Dittmer, Kim J. Hasenkrug, Kathrin Sutter, Mario L. Santiago, and Kerry J. Lavender

Subjects

CD4-Positive T-Lymphocytes, Dose-Response Relationship, Drug, business.industry, Macrophages, Medizin, HIV, Interferon-alpha, Alpha interferon, HIV Infections, Computational biology, Biology, Virus Replication, Antiviral Agents, Microbiology, QR1-502, Host-Microbe Biology, HEK293 Cells, Text mining, Leukocytes, Mononuclear, Humans, business, Letter to the Editor, Molecular Biology, Gene, Signal Transduction

Abstract

Type I interferons (IFNs) are key players in the antiviral immune response. Interferon alpha (IFN-α) belongs to this class of IFNs and comprises 12 subtypes that differ from each other in their binding affinities for a common receptor and, thus, in their signaling potencies. Recent data suggest that IFN-α6 and -α14 are the most potent IFN-α subtypes in restricting HIV replication when applied exogenously. However, in the context of antiviral therapy, IFNs are administered at high doses, which may compensate for differences in potency seen between IFN-α subtypes. In this study, we reexamined whether IFN-α subtypes induce different biological activities, with a focus on how IFN-α treatment dose affects cellular responses to HIV in primary CD4

Published

2019

15. Hepatitis B Virus Precore Protein p22 Inhibits Alpha Interferon Signaling by Blocking STAT Nuclear Translocation

Author

Jinyu Wang, Jiming Zhang, Minhui Dong, Bidisha Mitra, Richeng Mao, Elena S. Kim, Haitao Guo, and Yuanjie Liu

Subjects

Male, viruses, medicine.disease_cause, 0302 clinical medicine, Hepatitis B e Antigens, 0303 health sciences, Viral Core Proteins, Liver Neoplasms, virus diseases, Hep G2 Cells, Middle Aged, Hepatitis B, Hepatitis B Core Antigens, Virus-Cell Interactions, Protein Transport, STAT1 Transcription Factor, Liver, HBeAg, Hepatocellular carcinoma, Female, 030211 gastroenterology & hepatology, Signal Transduction, Adult, Hepatitis B virus, Carcinoma, Hepatocellular, Adolescent, Immunology, Alpha interferon, Biology, Antiviral Agents, Microbiology, Virus, Young Adult, 03 medical and health sciences, Hepatitis B, Chronic, Immune system, Virology, medicine, Humans, 030304 developmental biology, Hepatitis, Interferon-alpha, medicine.disease, Immunity, Innate, digestive system diseases, Chronic infection, HEK293 Cells, Insect Science

Abstract

Antagonism of host immune defenses against hepatitis B virus (HBV) infection by the viral proteins is speculated to cause HBV persistence and the development of chronic hepatitis. The circulating hepatitis B e antigen (HBeAg, p17) is known to manipulate host immune responses to assist in the establishment of persistent viral infection, and HBeAg-positive (HBeAg(+)) patients respond less effectively to IFN-α therapy than do HBeAg-negative (HBeAg(−)) patients in clinical practice. However, the function(s) of the intracellular form of HBeAg, previously reported as the precore protein intermediate (p22) without the N-terminal signal peptide, remains elusive. Here, we report that the cytosolic p22 protein, but not the secreted HBeAg, significantly reduces interferon-stimulated response element (ISRE) activity and the expression of interferon-stimulated genes (ISGs) upon alpha interferon (IFN-α) stimulation in cell cultures. In line with this, HBeAg(+) patients exhibit weaker induction of ISGs in their livers than do HBeAg(−) patients upon IFN-α therapy. Mechanistically, while p22 does not alter the total STAT1 or pSTAT1 levels in cells treated with IFN-α, it blocks the nuclear translocation of pSTAT1 by interacting with the nuclear transport factor karyopherin α1 through its C-terminal arginine-rich domain. In summary, our study suggests that HBV precore protein, specifically the p22 form, impedes JAK-STAT signaling to help the virus evade the host innate immune response and, thus, causes resistance to IFN therapy. IMPORTANCE Chronic hepatitis B virus (HBV) infection continues to be a major global health concern, and patients who fail to mount an efficient immune response to clear the virus will develop a life-long chronic infection that can progress to chronic active hepatitis, cirrhosis, and primary hepatocellular carcinoma. There is no definite cure for chronic hepatitis B, and alpha interferon (IFN-α) is the only available immunomodulatory drug, to which only a minority of chronic patients are responsive, with hepatitis B e antigen (HBeAg)-negative patients responding better than HBeAg-positive patients. We herein report that the intracellular HBeAg, also known as precore or p22, inhibits the antiviral signaling of IFN-α, which sheds light on the enigmatic function of precore protein in shaping HBV chronicity and provides a perspective toward areas that need to be further studied to make the current therapy better until a cure is achieved.

Published

2019

16. Antiviral Candidates for Treating Hepatitis E Virus Infection

Author

Peter A. White, Daniel Enosi Tuipulotu, Jason M. Mackenzie, Subhash G. Vasudevan, and Natalie E. Netzler

Subjects

Adenosine, Sofosbuvir, viruses, Alpha interferon, medicine.disease_cause, Antiviral Agents, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Hepatitis E virus, Genes, Reporter, Cell Line, Tumor, Nitriles, medicine, Humans, Pharmacology (medical), Replicon, 030304 developmental biology, Pharmacology, 0303 health sciences, Dose-Response Relationship, Drug, business.industry, Ribavirin, virus diseases, Drug Synergism, Hepatitis E, medicine.disease, Nitro Compounds, Virology, Drug repositioning, Infectious Diseases, chemistry, RNA, Viral, 030211 gastroenterology & hepatology, business, Viral hepatitis, medicine.drug

Abstract

Globally, hepatitis E virus (HEV) causes significant morbidity and mortality each year. Despite this burden, there are no specific antivirals available to treat HEV patients, and the only licensed vaccine is not available outside China. Ribavirin and alpha interferon are used to treat chronic HEV infections; however, severe side effects and treatment failure are commonly reported. Therefore, this study aimed to identify potential antivirals for further development to combat HEV infection. We selected 16 compounds from the nucleoside and nonnucleoside antiviral classes that range in developmental status from late preclinical to FDA approved and evaluated them as potential antivirals for HEV infection, using genotype 1 replicon luminescence studies and replicon RNA quantification. Two potent inhibitors of HEV replication included NITD008 (half-maximal effective concentration [EC(50)], 0.03 μM; half-maximal cytotoxic concentration [CC(50)], >100 μM) and GPC-N114 (EC(50), 1.07 μM, CC(50), >100 μM), and both drugs reduced replicon RNA levels in cell culture (>50% reduction with either 10 μM GPC-N114 or 2.50 μM NITD008). Furthermore, GPC-N114 and NITD008 were synergistic in combinational treatment (combination index, 0.4) against HEV replication, allowing for dose reduction indices of 20.42 and 8.82 at 50% inhibition, respectively. Sofosbuvir has previously exhibited mixed results against HEV as an antiviral, both in vitro and in a few clinical applications; however, in this study it was effective against the HEV genotype 1 replicon (EC(50), 1.97 μM; CC(50), >100 μM) and reduced replicon RNA levels (47.2% reduction at 10 μM). Together these studies indicate drug repurposing may be a promising pathway for development of antivirals against HEV infection.

Published

2019

17. Interferon Alpha Enhances NK Cell Function and the Suppressive Capacity of HIV-Specific CD8 + T Cells

Author

Chloe A. G. Talana, Joel N. Blankson, and Abena K. Kwaa

Subjects

medicine.medical_treatment, T cell, Immunology, Alpha interferon, HIV Infections, CD8-Positive T-Lymphocytes, Biology, Lymphocyte Activation, Antiviral Agents, Microbiology, Cell Degranulation, 03 medical and health sciences, 0302 clinical medicine, Immune system, Virology, HIV Seropositivity, medicine, Humans, Cytotoxic T cell, Viremia, 030304 developmental biology, 0303 health sciences, Degranulation, Interferon-alpha, Virus Latency, Killer Cells, Natural, Cytokine, medicine.anatomical_structure, Case-Control Studies, Insect Science, HIV-1, Pathogenesis and Immunity, Cytokines, Cytokine secretion, CD8, 030215 immunology

Abstract

Current shock-and-kill strategies for the eradication of the HIV-1 reservoir have resulted in blips of viremia but not in a decrease in the size of the latent reservoir in patients on suppressive antiretroviral therapy (ART). This discrepancy could potentially be explained by an inability of the immune system to kill HIV-1-infected cells following the reversal of latency. Furthermore, some studies have suggested that certain latency-reversing agents (LRAs) may inhibit CD8(+) T cell and natural killer (NK) cell responses. In this study, we tested the hypothesis that alpha interferon (IFN-α) could improve the function of NK cells from chronic progressors (CP) on ART. We show here that IFN-α treatment enhanced cytokine secretion, polyfunctionality, degranulation, and the cytotoxic potential of NK cells from healthy donors (HD) and CP. We also show that this cytokine enhanced the viral suppressive capacity of NK cells from HD and elite controllers or suppressors. Furthermore, IFN-α enhanced global CP CD8(+) T cell cytokine responses and the suppressive capacity of ES CD8(+) T cells. Our data suggest that IFN-α treatment may potentially be used as an immunomodulatory agent in HIV-1 cure strategies. IMPORTANCE Data suggest that HIV(+) individuals unable to control infection fail to do so due to impaired cytokine production and/cytotoxic effector cell function. Consequently, the success of cure agendas such as the shock-and-kill strategy will probably depend on enhancing patient effector cell function. In this regard, NK cells are of particular interest since they complement the function of CD8(+) T cells. Here, we demonstrate the ability of short-course alpha interferon (IFN-α) treatments to effectively enhance such effector functions in chronic progressor NK cells without inhibiting their general CD8(+) T cell function. These results point to the possibility of exploring such short-course IFN-α treatments for the enhancement of effector cell function in HIV(+) patients in future cure strategies.

Published

2019

18. Dose-Dependent Differences in HIV Inhibition by Different Interferon Alpha Subtypes While Having Overall Similar Biologic Effects

Author

Erika Schlaepfer, Audrey Fahrny, Stefan P. Kuster, Maarja Gruenbach, Roberto F. Speck, Gideon Schreiber, Viviana Simon, University of Zurich, and Speck, Roberto F

Subjects

0301 basic medicine, Mutant, lcsh:QR1-502, Alpha interferon, 610 Medicine & health, Context (language use), Stimulation, therapeutic efficacy, Pharmacology, Biology, Peripheral blood mononuclear cell, Microbiology, lcsh:Microbiology, 10234 Clinic for Infectious Diseases, 03 medical and health sciences, 0302 clinical medicine, Immune system, antiviral therapy, 1312 Molecular Biology, Receptor, Molecular Biology, Gene, human immunodeficiency virus, 2404 Microbiology, Therapeutics and Prevention, QR1-502, 3. Good health, interferons, 030104 developmental biology, 030220 oncology & carcinogenesis, Research Article

Abstract

Elucidating the functional role of the IFN-α subtypes is of particular importance for the development of efficacious therapies using exogenous IFN-α. Specifically, this will help define whether IFN therapy should be based on the use of pathogen-dependent IFN subtypes or, rather, IFN mutants with optimized IFNAR binding properties., Type I interferons (IFNs) are key players in the antiviral immune response. Interferon alpha (IFN-α) belongs to this class of IFNs and comprises 12 subtypes that differ from each other in their binding affinities for a common receptor and, thus, in their signaling potencies. Recent data suggest that IFN-α6 and -α14 are the most potent IFN-α subtypes in restricting HIV replication when applied exogenously. However, in the context of antiviral therapy, IFNs are administered at high doses, which may compensate for differences in potency seen between IFN-α subtypes. In this study, we reexamined whether IFN-α subtypes induce different biological activities, with a focus on how IFN-α treatment dose affects cellular responses to HIV in primary CD4+ T cells, peripheral blood mononuclear cells (PBMCs), and macrophages. We found that the subtypes’ antiviral activities were dose dependent, with >90% inhibition of HIV replication at a high dose of all IFN-αs except the weak IFN-α/β receptor (IFNAR) binder, IFN-α1. The quality of the responses engendered by IFN-α1, -α2, -α6, and -α14 was highly comparable, with essentially the same set of genes induced by all four subtypes. Hierarchal cluster analysis revealed that the individual donors were stronger determinants for the IFN-stimulated-gene (ISG) responses than the specific IFN-α subtype used for stimulation. Notably, IFN-α2-derived mutants with substantially reduced IFNAR2 binding still inhibited HIV replication efficiently, whereas mutants with increased IFNAR1 binding potentiated antiviral activity. Overall, our results support the idea that IFN-α subtypes do not induce different biological responses, given that each subtype is exogenously applied at bioequivalent doses. IMPORTANCE Elucidating the functional role of the IFN-α subtypes is of particular importance for the development of efficacious therapies using exogenous IFN-α. Specifically, this will help define whether IFN therapy should be based on the use of pathogen-dependent IFN subtypes or, rather, IFN mutants with optimized IFNAR binding properties.

Published

2019

19. Complementary Effects of Interleukin-15 and Alpha Interferon Induce Immunity in Hepatitis B Virus Transgenic Mice

Author

Gloria González-Aseguinolaza, Miguel Galarraga, Itziar Otano, Cristina Olagüe, Lucia Vanrell, Laura Guembe, Africa Vales, Mirja Hommel, Irene Gil-Farina, Marianna Di Scala, Jesús Prieto, Carlos Ortiz de Solorzano, Indrajit Ghosh, and Mala K. Maini

Subjects

0301 basic medicine, Hepatitis B virus, T cell, Immunology, Alpha interferon, Mice, Transgenic, CD8-Positive T-Lymphocytes, Biology, medicine.disease_cause, Microbiology, Virus, Adenoviridae, Gene Delivery, 03 medical and health sciences, Hepatitis B, Chronic, 0302 clinical medicine, Immune system, Virology, medicine, Animals, Hepatitis B Antibodies, Interleukin-15, Drug Carriers, Interferon-alpha, Genetic Therapy, Viral Load, Hepatitis B, medicine.disease, 3. Good health, Disease Models, Animal, Treatment Outcome, 030104 developmental biology, medicine.anatomical_structure, Liver, Insect Science, Viral load, CD8, 030215 immunology

Abstract

In chronic hepatitis B (CHB), failure to control hepatitis B virus (HBV) is associated with T cell dysfunction. HBV transgenic mice mirror many features of the human disease, including T cell unresponsiveness, and thus represent an appropriate model in which to test novel therapeutic strategies. To date, the tolerant state of CD8 + T cells in these animals could be altered only by strong immunogens or by immunization with HBV antigen-pulsed dendritic cells; however, the effectors induced were unable to suppress viral gene expression or replication. Because of the known stimulatory properties of alpha interferon (IFN-α) and interleukin-15 (IL-15), this study explored the therapeutic potential of liver-directed gene transfer of these cytokines in a murine model of CHB using adeno-associated virus (AAV) delivery. This combination not only resulted in a reduction in the viral load in the liver and the induction of an antibody response but also gave rise to functional and specific CD8 + immunity. Furthermore, when splenic and intrahepatic lymphocytes from IFN-α- and IL-15-treated animals were transferred to new HBV carriers, partial antiviral immunity was achieved. In contrast to previous observations made using either cytokine alone, markedly attenuated PD-L1 induction in hepatic tissue was observed upon coadministration. An initial study with CHB patient samples also gave promising results. Hence, we demonstrated synergy between two stimulating cytokines, IL-15 and IFN-α, which, given together, constitute a potent approach to significantly enhance the CD8 + T cell response in a state of immune hyporesponsiveness. Such an approach may be useful for treating chronic viral infections and neoplastic conditions. IMPORTANCE With 350 million people affected worldwide and 600,000 annual deaths due to HBV-induced liver cirrhosis and/or hepatocellular carcinoma, chronic hepatitis B (CHB) is a major health problem. However, current treatment options are costly and not very effective and/or need to be administered for life. The unprecedented efficacy of the strategy described in our paper may offer an alternative and is relevant for a broad spectrum of readers because of its clear translational importance to other chronic viral infections in which a hyporesponsive antigen-specific T cell repertoire prevents clearance of the pathogen.

Published

2016

20. Interferon Alpha Subtype-Specific Suppression of HIV-1 Infection In Vivo

Author

Ali Gawanbacht, Eric J. Lee, Jacob Piehler, Jens Verheyen, Janis A. Müller, Brent Race, Mario L. Santiago, Sandra Francois, Cara C. Wilson, Kim J. Hasenkrug, Ronald J. Messer, Karin E. Peterson, Michael S. Harper, Kejun Guo, Katie Phillips, Jan Münch, Hartmut Hengel, Ulf Dittmer, Kathrin Gibbert, Erik Van Dis, Tyson A. Woods, Mirko Trilling, and Kerry J. Lavender

Subjects

Myxovirus Resistance Proteins, 0301 basic medicine, Combination therapy, Immunology, Medizin, Antiviral protein, Alpha interferon, HIV Infections, Mice, Transgenic, Viremia, APOBEC-3G Deaminase, CD8-Positive T-Lymphocytes, Biology, GPI-Linked Proteins, Lymphocyte Activation, Virus Replication, Antiviral Agents, Microbiology, Virus, Mice, 03 medical and health sciences, Immune system, Antigens, CD, Virology, Vaccines and Antiviral Agents, medicine, Animals, Humans, Interferon-alpha, virus diseases, Viral Load, medicine.disease, Immunity, Innate, Killer Cells, Natural, 030104 developmental biology, Viral replication, Insect Science, Disease Progression, HIV-1, Viral load

Abstract

Although all 12 subtypes of human interferon alpha (IFN-α) bind the same receptor, recent results have demonstrated that they elicit unique host responses and display distinct efficacies in the control of different viral infections. The IFN-α2 subtype is currently in HIV-1 clinical trials, but it has not consistently reduced viral loads in HIV-1 patients and is not the most effective subtype against HIV-1 in vitro . We now demonstrate in humanized mice that, when delivered at the same high clinical dose, the human IFN-α14 subtype has very potent anti-HIV-1 activity whereas IFN-α2 does not. In both postexposure prophylaxis and treatment of acute infections, IFN-α14, but not IFN-α2, significantly suppressed HIV-1 replication and proviral loads. Furthermore, HIV-1-induced immune hyperactivation, which is a prognosticator of disease progression, was reduced by IFN-α14 but not IFN-α2. Whereas ineffective IFN-α2 therapy was associated with CD8 + T cell activation, successful IFN-α14 therapy was associated with increased intrinsic and innate immunity, including significantly higher induction of tetherin and MX2, increased APOBEC3G signature mutations in HIV-1 proviral DNA, and higher frequencies of TRAIL + NK cells. These results identify IFN-α14 as a potent new therapeutic that operates via mechanisms distinct from those of antiretroviral drugs. The ability of IFN-α14 to reduce both viremia and proviral loads in vivo suggests that it has strong potential as a component of a cure strategy for HIV-1 infections. The broad implication of these results is that the antiviral efficacy of each individual IFN-α subtype should be evaluated against the specific virus being treated. IMPORTANCE The naturally occurring antiviral protein IFN-α2 is used to treat hepatitis viruses but has proven rather ineffective against HIV in comparison to triple therapy with the antiretroviral (ARV) drugs. Although ARVs suppress the replication of HIV, they fail to completely clear infections. Since IFN-α acts by different mechanism than ARVs and has been shown to reduce HIV proviral loads, clinical trials are under way to test whether IFN-α2 combined with ARVs might eradicate HIV-1 infections. IFN-α is actually a family of 12 distinct proteins, and each IFN-α subtype has different efficacies toward different viruses. Here, we use mice that contain a human immune system, so they can be infected with HIV. With this model, we demonstrate that while IFN-α2 is only weakly effective against HIV, IFN-α14 is extremely potent. This discovery identifies IFN-α14 as a more powerful IFN-α subtype for use in combination therapy trials aimed toward an HIV cure.

Published

2016

21. Antiviral Activities of Different Interferon Types and Subtypes against Hepatitis E Virus Replication

Author

Catherine François, Daniel Todt, Anggakusuma, Eike Steinmann, Patrick Behrendt, Michael Engelmann, Rune Hartmann, Gabrielle Vieyres, Heiner Wedemeyer, Gilles Duverlie, Leonard Knegendorf, and Thomas Pietschmann

Subjects

0301 basic medicine, Genotype, viruses, Hepatitis C virus, Alpha interferon, Interferon alpha-2, Biology, Virus Replication, medicine.disease_cause, Antiviral Agents, Interferon-gamma, 03 medical and health sciences, chemistry.chemical_compound, Hepatitis E virus, Interferon, Cell Line, Tumor, Ribavirin, medicine, Humans, Pharmacology (medical), Adaptor Proteins, Signal Transducing, Subgenomic mRNA, Pharmacology, Interleukins, Intracellular Signaling Peptides and Proteins, Interferon-alpha, RNA-Binding Proteins, virus diseases, Hep G2 Cells, Hepatitis E, medicine.disease, Virology, Recombinant Proteins, digestive system diseases, Chemokine CXCL10, 030104 developmental biology, Infectious Diseases, Gene Expression Regulation, Viral replication, chemistry, Host-Pathogen Interactions, Immunology, Replicon, Interferons, Carrier Proteins, medicine.drug

Abstract

Hepatitis E virus (HEV) is the causative agent of hepatitis E in humans and a member of the genus Orthohepevirus in the family Hepeviridae . HEV infections are the common cause of acute hepatitis but can also take chronic courses. Ribavirin is the treatment of choice for most patients, and type I interferon (IFN) has been evaluated in a few infected transplant patients in vivo . In this study, the antiviral effects of different exogenously administered interferons were investigated by using state-of-the-art subgenomic replicon and full-length HEV genome cell culture models. Hepatitis C virus (HCV) subgenomic replicons based on the genotype 2a JFH1 isolate served as the reference. The experiments revealed that HEV RNA replication was inhibited by the application of all types of IFN, including IFN-α (type I), IFN-γ (type II), and IFN-λ3 (type III), but to a far lesser extent than HCV replication. Simultaneous determination of interferon-stimulated gene (ISG) expression levels for all IFN types demonstrated efficient downregulation by HEV. Furthermore, different IFN-α subtypes were also able to block viral replication in combination with ribavirin. The IFN-α subtypes 2a and 2b exerted the strongest antiviral activity against HEV. In conclusion, these data demonstrate for the first time moderate anti-HEV activities of types II and III IFNs and different IFN-α subtypes. As HEV employed a potent anti-interferon mechanism by restricting ISG expression, exogenous application of IFNs as immunotherapy should be carefully assessed.

Published

2016

22. Exosomes Exploit the Virus Entry Machinery and Pathway To Transmit Alpha Interferon-Induced Antiviral Activity

Author

Jieliang Chen, Yunsheng Qiao, Zhenghong Yuan, Jiahui Ding, Lu Peng, Jia Liu, Lu Bai, Bisheng Shi, Zhenlan Yao, Fang Shen, Xiaofang Li, and Jianhua Li

Subjects

0301 basic medicine, Hepatitis B virus, Endosome, THP-1 Cells, Immunology, Endocytic cycle, Alpha interferon, Biology, Endocytosis, Exosomes, Virus Replication, Microbiology, Exosome, Virus, 03 medical and health sciences, Viral entry, Virology, Humans, Hepatitis A Virus Cellular Receptor 1, 030102 biochemistry & molecular biology, Macrophages, Interferon-alpha, Hep G2 Cells, Virus Internalization, Microvesicles, Clathrin, Cell biology, Virus-Cell Interactions, 030104 developmental biology, HEK293 Cells, Insect Science, Hepatocytes, Monoglycerides, Pinocytosis, Lysophospholipids

Abstract

Alpha interferon (IFN-α) induces the transfer of resistance to hepatitis B virus (HBV) from liver nonparenchymal cells (LNPCs) to hepatocytes via exosomes. However, little is known about the entry machinery and pathway involved in the transmission of IFN-α-induced antiviral activity. In this study, we found that macrophage exosomes uniquely depend on T cell immunoglobulin and mucin receptor 1 (TIM-1), a hepatitis A virus (HAV) receptor, to enter hepatocytes for delivering IFN-α-induced anti-HBV activity. Moreover, two primary endocytic routes for virus infection, clathrin-mediated endocytosis (CME) and macropinocytosis, collaborate to permit exosome entry and anti-HBV activity transfer. Subsequently, lysobisphosphatidic acid (LBPA), an anionic lipid closely related to endosome penetration of virus, facilitates membrane fusion of exosomes in late endosomes/multivesicular bodies (LEs/MVBs) and the accompanying exosomal cargo uncoating. Together, our findings provide comprehensive insights into the transmission route of macrophage exosomes to efficiently deliver IFN-α-induced antiviral substances and highlight the similarities between the entry mechanisms of exosomes and virus. IMPORTANCE Our previous study showed that LNPC-derived exosomes could transmit IFN-α-induced antiviral activity to HBV replicating hepatocytes, but the concrete transmission mechanisms, which include exosome entry and exosomal cargo release, remain unclear. In this study, we found that virus entry machinery and pathway were also applied to exosome-mediated cell-to-cell antiviral activity transfer. Macrophage-derived exosomes distinctively exploit hepatitis A virus receptor for access to hepatocytes. Later, CME and macropinocytosis are utilized by exosomes, followed by exosome-endosome fusion for efficient transfer of IFN-α-induced anti-HBV activity. We believe that understanding the cellular entry pathway of exosomes will be beneficial to designing exosomes as efficient vehicles for antiviral therapy.

Published

2018

23. Characterization of the Plasmacytoid Dendritic Cell Response to Transmitted/Founder and Nontransmitted Variants of HIV-1

Author

Joel Singer, Terry Lee, Zachary Ende, Hongliang Zhang, Jordan A. Schwartz, Mario A. Ostrowski, Tony Mazzulli, Martin J. Deymier, and Eric Hunter

Subjects

Adult, Male, 0301 basic medicine, Primary Cell Culture, 030106 microbiology, Immunology, Alpha interferon, HIV Infections, Plasmacytoid dendritic cell, Viral quasispecies, Biology, Microbiology, Virus, 03 medical and health sciences, Neutralization Tests, Virology, Humans, Secretion, Tumor Necrosis Factor-alpha, Virion, Interferon-alpha, hemic and immune systems, Dendritic Cells, 3. Good health, 030104 developmental biology, Insect Science, Viral evolution, Host-Pathogen Interactions, HIV-1, Pathogenesis and Immunity, Female, Cytokine secretion, Tumor necrosis factor alpha

Abstract

Human immunodeficiency virus type 1 (HIV-1) infection often arises from a single transmitted/founder (TF) viral variant among a large pool of viruses in the quasispecies in the transmitting partner. TF variants are typically nondominant in blood and genital secretions, indicating that they have unique traits. The plasmacytoid dendritic cell (pDC) is the primary alpha interferon (IFN-α)-producing cell in response to viral infections and is rapidly recruited to the female genital tract upon exposure to HIV-1. The impact of pDCs on transmission is unknown. We investigated whether evasion of pDC responses is a trait of TF viruses. pDCs from healthy donors were stimulated in vitro with a panel of 20 HIV-1 variants, consisting of one TF variant and three nontransmitted (NT) variants each from five transmission-linked donor pairs, and secretion of IFN-α and tumor necrosis factor alpha (TNF-α) was measured by enzyme-linked immunosorbent assay (ELISA). No significant differences in cytokine secretion in response to TF and NT viruses were observed, despite a trend toward enhanced IFN-α and TNF-α production in response to TF viruses. NT viruses demonstrated polarization toward production of either IFN-α or TNF-α, indicating possible dysregulation. Also, for NT viruses, IFN-α secretion was associated with increased resistance of the virus to inactivation by IFN-α in vitro, suggesting in vivo evolution. Thus, TF viruses do not appear to preferentially subvert pDC activation compared to that with nontransmitted HIV-1 variants. pDCs may, however, contribute to the in vivo evolution of HIV-1. IMPORTANCE The plasmacytoid dendritic cell (pDC) is the first cell type recruited to the site of HIV-1 exposure; however, its contribution to the viral bottleneck in HIV-1 transmission has not been explored previously. We hypothesized that transmitted/founder viruses are able to avoid the pDC response. In this study, we used previously established donor pair-linked transmitted/founder and nontransmitted (or chronic) variants of HIV-1 to stimulate pDCs. Transmitted/founder HIV-1, instead of suppressing pDC responses, induced IFN-α and TNF-α secretion to levels comparable to those induced by viruses from the transmitting partner. We noted several unique traits of chronic viruses, including polarization between IFN-α and TNF-α production as well as a strong relationship between IFN-α secretion and the resistance of the virus to neutralization. These data rule out the possibility that TF viruses preferentially suppress pDCs in comparison to the pDC response to nontransmitted HIV variants. pDCs may, however, be important drivers of viral evolution in vivo.

Published

2018

24. Role of MxB in Alpha Interferon-Mediated Inhibition of HIV-1 Infection

Author

Qinghua Pan, Chen Liang, and Bin Xu

Subjects

0301 basic medicine, Myxovirus Resistance Proteins, G protein, Immunology, Alpha interferon, Alpha (ethology), HIV Infections, Microbiology, Antiviral Agents, Models, Biological, Virus, Cell Line, 03 medical and health sciences, Gene Knockout Techniques, Interferon, Virology, medicine, Humans, Immunologic Factors, Gene, biology, virus diseases, Interferon-alpha, biology.organism_classification, 3. Good health, Virus-Cell Interactions, 030104 developmental biology, Cell culture, Vesicular stomatitis virus, Insect Science, HIV-1, medicine.drug

Abstract

Type I interferon inhibits viruses through inducing the expression of antiviral proteins, including the myxovirus resistance (Mx) proteins. Compared to the human MxA protein, which inhibits a wide range of viruses, the MxB protein has been reported to specifically inhibit primate lentiviruses, including HIV-1, and herpesviruses. Further, the role of endogenous MxB in alpha interferon-mediated inhibition of HIV-1 infection was questioned by a recent study showing that MxB knockout did not increase the level of infection by HIV-1 which carried the G protein of vesicular stomatitis virus (VSV), allowing infection of CD4-negative HT1080 cells. In order to further examine the anti-HIV-1 activity of endogenous MxB, we have used CRISPR/Cas9 to deplete MxB in different cell lines and observed a substantial restoration of HIV-1 infection in the presence of alpha interferon treatment. However, this rescue effect of MxB knockout became much less pronounced when infection was performed with HIV-1 carrying the VSV G protein. Interestingly, a CRISPR/Cas9 knockout screen of alpha interferon-stimulated genes in U87-MG cells revealed that the genes for interferon-induced transmembrane protein 2 (IFITM2) and IFITM3 inhibited VSV G-pseudotyped HIV-1 much more strongly than the rest of the genes tested, including the gene for MxB. Therefore, our results demonstrate the importance of MxB in alpha interferon-mediated inhibition of HIV-1 infection, which, however, can be underestimated if infection is performed with VSV G protein-pseudotyped HIV-1, due to the high sensitivity of VSV G-mediated infection to inhibition by IFITM proteins.IMPORTANCE The results of this study reconcile the controversial reports regarding the anti-HIV-1 function of alpha interferon-induced MxB protein. In addition to the different cell types that may have contributed to the different observations, our data also suggest that VSV G protein-pseudotyped HIV-1 is much less inhibited by alpha interferon-induced MxB than HIV-1 itself is. Our results clearly demonstrate an important contribution of MxB to alpha interferon-mediated inhibition of HIV-1 in CD4+ T cells, which calls for using HIV-1 target cells and wild-type virus to test the relevance of the anti-HIV-1 activity of endogenous MxB and other restriction factors.

Published

2018

25. Preclinical Profile of AB-423, an Inhibitor of Hepatitis B Virus Pregenomic RNA Encapsidation

Author

Richeng Mao, Bruce D. Dorsey, Andrew G. Cole, Quanxin Long, Alice H. L. Li, Sunny Tang, Rene Rijnbrand, Troy Harasym, Ellen Evangelista, Xiaohe Wang, Nicholas M. Snead, Kevin McClintock, Sara A. Majeski, Haitao Guo, Nagraj Mani, Kyle D. Cobarrubias, Stephen P. Reid, Fang Guo, Holly M. Micolochick Steuer, Janet R. Phelps, Steven G. Kultgen, Andrea Cuconati, Ju-Tao Guo, Qiong Zhao, Amy C.H. Lee, Salam Kadhim, Kim Stever, Kristi Fan, Andrzej Ardzinski, and Michael J. Sofia

Subjects

0301 basic medicine, Hepatitis B virus, Guanine, Alpha interferon, medicine.disease_cause, Antiviral Agents, Mice, 03 medical and health sciences, Capsid, RNA interference, Cell Line, Tumor, medicine, Animals, Humans, Cytotoxic T cell, Pharmacology (medical), Cytotoxicity, Pharmacology, Binding Sites, Chemistry, Virus Assembly, Entecavir, Hepatitis B, Molecular biology, In vitro, Molecular Docking Simulation, 030104 developmental biology, Infectious Diseases, DNA, Viral, RNA, Viral, Female, DNA, Circular, Protein Binding, medicine.drug

Abstract

AB-423 is a member of the sulfamoylbenzamide (SBA) class of hepatitis B virus (HBV) capsid inhibitors in phase 1 clinical trials. In cell culture models, AB-423 showed potent inhibition of HBV replication (50% effective concentration [EC 50 ] = 0.08 to 0.27 μM; EC 90 = 0.33 to 1.32 μM) with no significant cytotoxicity (50% cytotoxic concentration > 10 μM). Addition of 40% human serum resulted in a 5-fold increase in the EC 50 s. AB-423 inhibited HBV genotypes A through D and nucleos(t)ide-resistant variants in vitro . Treatment of HepDES19 cells with AB-423 resulted in capsid particles devoid of encapsidated pregenomic RNA and relaxed circular DNA (rcDNA), indicating that it is a class II capsid inhibitor. In a de novo infection model, AB-423 prevented the conversion of encapsidated rcDNA to covalently closed circular DNA, presumably by interfering with the capsid uncoating process. Molecular docking of AB-423 into crystal structures of heteroaryldihydropyrimidines and an SBA and biochemical studies suggest that AB-423 likely also binds to the dimer-dimer interface of core protein. In vitro dual combination studies with AB-423 and anti-HBV agents, such as nucleos(t)ide analogs, RNA interference agents, or interferon alpha, resulted in additive to synergistic antiviral activity. Pharmacokinetic studies with AB-423 in CD-1 mice showed significant systemic exposures and higher levels of accumulation in the liver. A 7-day twice-daily administration of AB-423 in a hydrodynamic injection mouse model of HBV infection resulted in a dose-dependent reduction in serum HBV DNA levels, and combination with entecavir or ARB-1467 resulted in a trend toward antiviral activity greater than that of either agent alone, consistent with the results of the in vitro combination studies. The overall preclinical profile of AB-423 supports its further evaluation for safety, pharmacokinetics, and antiviral activity in patients with chronic hepatitis B.

Published

2018

26. Exacerbated Apoptosis of Cells Infected with Infectious Bursal Disease Virus upon Exposure to Interferon Alpha

Author

Elisabet Diaz-Beneitez, Marina Ciscar, Dolores Rodríguez, Liliana L. Cubas-Gaona, and José F. Rodríguez

Subjects

0301 basic medicine, animal structures, Birnaviridae, Secondary infection, Immunology, Alpha interferon, Apoptosis, Chick Embryo, Antiviral Agents, Infectious bursal disease virus, Microbiology, Infectious bursal disease, 03 medical and health sciences, Bursa of Fabricius, Immune system, Interferon, Cell Line, Tumor, Virology, Chlorocebus aethiops, medicine, Animals, Humans, Vero Cells, Poultry Diseases, B-Lymphocytes, Innate immune system, biology, Tumor Necrosis Factor-alpha, NF-kappa B, Interferon-alpha, Birnaviridae Infections, medicine.disease, biology.organism_classification, Protein kinase R, 030104 developmental biology, Insect Science, Pathogenesis and Immunity, Chickens, Protein Kinases, HeLa Cells, medicine.drug

Abstract

Infectious bursal disease virus (IBDV) belongs to the Birnaviridae family and is the etiological agent of a highly contagious and immunosuppressive disease (IBD) that affects domestic chickens ( Gallus gallus ). IBD or Gumboro disease leads to high rates of morbidity and mortality of infected animals and is responsible for major economic losses to the poultry industry worldwide. IBD is characterized by a massive loss of IgM-bearing B lymphocytes and the destruction of the bursa of Fabricius. The molecular bases of IBDV pathogenicity are still poorly understood; nonetheless, an exacerbated cytokine immune response and B cell depletion due to apoptosis are considered main factors that contribute to the severity of the disease. Here we have studied the role of type I interferon (IFN) in IBDV infection. While IFN pretreatment confers protection against subsequent IBDV infection, the addition of IFN to infected cell cultures early after infection drives massive apoptotic cell death. Downregulation of double-stranded RNA (dsRNA)-dependent protein kinase (PKR), tumor necrosis factor alpha (TNF-α), or nuclear factor κB (NF-κB) expression drastically reduces the extent of apoptosis, indicating that they are critical proteins in the apoptotic response induced by IBDV upon treatment with IFN-α. Our results indicate that IBDV genomic dsRNA is a major viral factor that contributes to the triggering of apoptosis. These findings provide novel insights into the potential mechanisms of IBDV-induced immunosuppression and pathogenesis in chickens. IMPORTANCE IBDV infection represents an important threat to the poultry industry worldwide. IBDV-infected chickens develop severe immunosuppression, which renders them highly susceptible to secondary infections and unresponsive to vaccination against other pathogens. The early dysregulation of the innate immune response led by IBDV infection and the exacerbated apoptosis of B cells have been proposed as the main factors that contribute to virus-induced immunopathogenesis. Our work contributes for the first time to elucidating a potential mechanism driving the apoptotic death of IBDV-infected cells upon exposure to type I IFN. We provide solid evidence about the critical importance of PKR, TNF-α, and NF-κB in this phenomenon. The described mechanism could facilitate the early clearance of infected cells, thereby aiding in the amelioration of IBDV-induced pathogenesis, but it could also contribute to B cell depletion and immunosuppression. The balance between these two opposing effects might be dramatically affected by the genetic backgrounds of both the host and the infecting virus strain.

Published

2018

27. Reduced Chronic Lymphocyte Activation following Interferon Alpha Blockade during the Acute Phase of Simian Immunodeficiency Virus Infection in Rhesus Macaques

Author

Rafick-Pierre Sekaly, Kalpana Patel, Mark J. Cameron, Thomas H. Vanderford, Diane G. Carnathan, Reem A. Dawoud, Joana Yu, Olivia M. Delmas, Gregory K. Tharp, Peter Wilkinson, Benton Lawson, Steven E. Bosinger, Charles A. Nicolette, Guido Silvestri, and James M. Billingsley

Subjects

CD4-Positive T-Lymphocytes, 0301 basic medicine, T cell, Programmed Cell Death 1 Receptor, Immunology, Simian Acquired Immunodeficiency Syndrome, Alpha interferon, CD8-Positive T-Lymphocytes, Biology, Lymphocyte Activation, Virus Replication, medicine.disease_cause, Microbiology, Virus, 03 medical and health sciences, 0302 clinical medicine, Immune system, Interferon, Virology, medicine, Animals, B-Lymphocytes, Antibodies, Monoclonal, Interferon-alpha, Viral Load, Simian immunodeficiency virus, Macaca mulatta, CD4 Lymphocyte Count, Blockade, Killer Cells, Natural, Ki-67 Antigen, 030104 developmental biology, medicine.anatomical_structure, Insect Science, Pathogenesis and Immunity, Simian Immunodeficiency Virus, Viral load, 030215 immunology, medicine.drug

Abstract

Pathogenic human immunodeficiency virus (HIV)/simian immunodeficiency virus (SIV) infection of humans and rhesus macaques (RMs) induces persistently high production of type I interferon (IFN-I), which is thought to contribute to disease progression. To elucidate the specific role of interferon alpha (IFN-α) in SIV pathogenesis, 12 RMs were treated prior to intravenous (i.v.) SIV mac239 infection with a high or a low dose of an antibody (AGS-009) that neutralizes most IFN-α subtypes and were compared with six mock-infused, SIV-infected controls. Plasma viremia was measured postinfection to assess the effect of IFN-α blockade on virus replication, and peripheral blood and lymphoid tissue samples were analyzed by immunophenotypic staining. Consistent with the known antiviral effect of IFN-I, high-dose AGS-009 treatment induced a modest increase in acute-phase viral loads versus controls. Four out of 6 RMs receiving a high dose of AGS-009 also experienced an early decline in CD4 + T cell counts that was associated with progression to AIDS. Interestingly, 50% of the animals treated with AGS-009 (6/12) developed AIDS within 1 year of infection compared with 17% (1/6) of untreated controls. Finally, blockade of IFN-α decreased the levels of activated CD4 + and CD8 + T cells, as well as B cells, as measured by PD-1 and/or Ki67 expression. The lower levels of activated lymphocytes in IFN-α-blockaded animals supports the hypothesis that IFN-α signaling contributes to lymphocyte activation during SIV infection and suggests that this signaling pathway is involved in controlling virus replication during acute infection. The potential anti-inflammatory effect of IFN-α blockade should be explored as a strategy to reduce immune activation in HIV-infected individuals. IMPORTANCE Interferon alpha (IFN-α) is a member of a family of molecules (type I interferons) that prevent or limit virus infections in mammals. However, IFN-α production may contribute to the chronic immune activation that is thought to be the primary cause of immune decline and AIDS in HIV-infected patients. The study presented here attempts to understand the contribution of IFN-α to the natural history and progression of SIV infection of rhesus macaques, the primary nonhuman primate model system for testing hypotheses about HIV infection in humans. Here, we show that blockade of IFN-α action promotes lower chronic immune activation but higher early viral loads, with a trend toward faster disease progression. This study has significant implications for new treatments designed to impact the type I interferon system.

Published

2018

28. Porcine Mx1 Protein Inhibits Classical Swine Fever Virus Replication by Targeting Nonstructural Protein NS5B

Author

Xiao-min Zhang, Bin Zhou, Jing Chen, Zhi-Can Gao, Lin Kan, Zhao-Yao Li, Yun-Na Zhang, Jin-Xiu Hou, Jing Zhou, Wen-Liang Li, and Chun-Chun Liu

Subjects

0301 basic medicine, Myxovirus Resistance Proteins, Small interfering RNA, Swine, viruses, Immunology, Mutation, Missense, Alpha interferon, Biology, Viral Nonstructural Proteins, Virus Replication, Microbiology, Virus, 03 medical and health sciences, chemistry.chemical_compound, Interferon, Virology, RNA polymerase, medicine, Animals, Humans, NS5B, RNA, Virus-Cell Interactions, 030104 developmental biology, HEK293 Cells, chemistry, Viral replication, Amino Acid Substitution, Classical Swine Fever Virus, Insect Science, medicine.drug

Abstract

Mx proteins are interferon (IFN)-induced GTPases that have broad antiviral activity against a wide range of RNA and DNA viruses; they belong to the dynamin superfamily of large GTPases. In this study, we confirmed the anti-classical swine fever virus (CSFV) activity of porcine Mx1 in vitro and showed that porcine Mx2 (poMx2), human MxA (huMxA), and mouse Mx1 (mmMx1) also have anti-CSFV activity in vitro . Small interfering RNA (siRNA) experiments revealed that depletion of endogenous poMx1 or poMx2 enhanced CSFV replication, suggesting that porcine Mx proteins are responsible for the antiviral activity of interferon alpha (IFN-α) against CSFV infection. Confocal microscopy, immunoprecipitation, glutathione S -transferase (GST) pulldown, and bimolecular fluorescence complementation (BiFC) demonstrated that poMx1 associated with NS5B, the RNA-dependent RNA polymerase (RdRp) of CSFV. We used mutations in the poMx1 protein to elucidate the mechanism of their anti-CSFV activity and found that mutants that disrupted the association with NS5B lost all anti-CSV activity. Moreover, an RdRp activity assay further revealed that poMx1 undermined the RdRp activities of NS5B. Together, these results indicate that porcine Mx proteins exert their antiviral activity against CSFV by interacting with NS5B. IMPORTANCE Our previous studies have shown that porcine Mx1 (poMx1) inhibits classical swine fever virus (CSFV) replication in vitro and in vivo , but the molecular mechanism of action remains largely unknown. In this study, we dissect the molecular mechanism of porcine Mx1 and Mx2 against CSFV in vitro . Our results show that poMx1 associates with NS5B, the RNA-dependent RNA polymerase of CSFV, resulting in the reduction of CSFV replication. Moreover, the mutants of poMx1 further elucidate the mechanism of their anti-CSFV activities.

Published

2018

29. Zika Virus Replication Is Substantially Inhibited by Novel Favipiravir and Interferon Alpha Combination Regimens

Author

Jaime L. Rodriquez, Tae Hwan Kim, Justin J. Pomeroy, Ashley N. Brown, Camilly P. Pires de Mello, Xun Tao, and Jürgen B. Bulitta

Subjects

DNA Replication, 0301 basic medicine, Combination therapy, 030106 microbiology, Alpha interferon, Favipiravir, Virus Replication, Antiviral Agents, Virus, Cell Line, 03 medical and health sciences, chemistry.chemical_compound, Chlorocebus aethiops, Ribavirin, Animals, Humans, Medicine, Pharmacology (medical), Vero Cells, Pharmacology, Virus quantification, Zika Virus Infection, business.industry, Interferon-alpha, Zika Virus, Viral Load, Amides, Virology, Infectious Diseases, chemistry, Pyrazines, Vero cell, business, Viral load

Abstract

Zika virus (ZIKV) is a major public health concern due to its overwhelming spread into the Americas. Currently, there are neither licensed vaccines nor antiviral therapies available for the treatment of ZIKV. We aimed to identify and rationally optimize effective therapeutic regimens for ZIKV by evaluating the antiviral potentials of the approved broad-spectrum antiviral agents favipiravir (FAV), interferon alpha (IFN), and ribavirin (RBV) as single agents and in combinations. For these studies, Vero cells were infected with ZIKV in the presence of increasing concentrations of FAV, IFN, or/and RBV for 4 days. Supernatants were harvested daily, and the viral burden was quantified by a plaque assay on Vero cells. The time course of the viral burden during treatment in vitro was characterized by a novel translational, mechanism-based model, which was subsequently used to rationally optimize combination dosage regimens. The combination regimen of FAV plus IFN provided the greatest extent of viral inhibition without cytotoxicity, reducing the viral burden by 4.4 log 10 PFU/ml at concentrations of 250 μM FAV and 100 IU/ml IFN. Importantly, these concentrations are achievable in humans. The translational, mechanism-based model yielded unbiased and reasonably precise curve fits. Simulations with the model predicted that clinically relevant regimens of FAV plus IFN would markedly reduce viral burdens in humans, resulting in at least a 10,000-fold reduction in the amount of the virus during the first 4 days of treatment. These findings highlight the substantial promise of rationally optimized combination dosage regimens of FAV plus IFN, which should be further investigated to combat ZIKV.

Published

2018

30. Structural Basis of the Inhibition of STAT1 Activity by Sendai Virus C Protein

Author

Masaya Fukushi, Kosuke Oda, Takashi Irie, Ryoko Kawabata, Takemasa Sakaguchi, Masanori Sugiyama, and Yasuyuki Matoba

Subjects

Models, Molecular, Immunology, Alpha interferon, Electrophoretic Mobility Shift Assay, Plasma protein binding, Crystallography, X-Ray, Sendai virus, Microbiology, Cell Line, Interferon-gamma, Viral Proteins, Protein structure, Virology, Humans, Electrophoretic mobility shift assay, Phosphorylation, Binding site, STAT2, Binding Sites, biology, Binding protein, Interferon-alpha, STAT2 Transcription Factor, Interferon-beta, biology.organism_classification, Protein Structure, Tertiary, Virus-Cell Interactions, HEK293 Cells, STAT1 Transcription Factor, Biochemistry, Insect Science, Biophysics, biology.protein, Protein Binding, Signal Transduction

Abstract

Sendai virus (SeV) C protein inhibits the signal transduction pathways of interferon alpha/beta (IFN-α/β) and IFN-γ by binding to the N-terminal domain of STAT1 (STAT1ND), thereby allowing SeV to escape from host innate immunity. Here we determined the crystal structure of STAT1ND associated with the C-terminal half of the C protein (Y3 [amino acids 99 to 204]) at a resolution of 2.0 Å. This showed that two molecules of Y3 symmetrically bind to each niche created between two molecules of the STAT1ND dimer. Molecular modeling suggested that an antiparallel form of the full-length STAT1 dimer can bind only one Y3 molecule and that a parallel form can bind two Y3 molecules. Affinity analysis demonstrated anticooperative binding of two Y3 molecules with the STAT1 dimer, which is consistent with the hypothetical model that the second Y3 molecule can only target the STAT1 dimer in a parallel form. STAT1 with excess amounts of Y3 was prone to inhibit the dephosphorylation at Tyr 701 by a phosphatase. In an electrophoretic mobility shift assay, tyrosine-phosphorylated STAT1 (pY-STAT1) with Y3 associated with the γ-activated sequence, probably as high-molecular-weight complexes (HMWCs), which may account for partial inhibition of a reporter assay from IFN-γ by Y3. Our study suggests that the full-length C protein interferes with the domain arrangement of the STAT1 dimer, leading to the accumulation of pY-STAT1 and the formation of HMWCs. In addition, we discuss the mechanism by which phosphorylation of STAT2 is inhibited in the presence of the C protein after stimulation by IFN-α/β. IMPORTANCE Sendai virus, a paramyxovirus that causes respiratory diseases in rodents, possesses the C protein, which inhibits the signal transduction pathways of interferon alpha/beta (IFN-α/β) and IFN-γ by binding to the transcription factor STAT1. In virus-infected cells, phosphorylation of STAT1 at the Tyr 701 residue is potently enhanced, although transcription by STAT1 is inert. Here, we determined the crystal structure of the N-terminal domain of STAT1 associated with the C-terminal half of the C protein. Molecular modeling and experiments suggested that the two C proteins bind to and stabilize the parallel form of the STAT1 dimer, which are likely to be phosphorylated at Tyr 701 , further inducing high-molecular-weight complex formation and inhibition of transcription by IFN-γ. We also discuss the possible mechanism of inhibition of the IFN-α/β pathways by the C protein. This is the first structural report of the C protein, suggesting a mechanism of evasion of the paramyxovirus from innate immunity.

Published

2015

31. The Interferon-Inducible Protein Tetherin Inhibits Hepatitis B Virus Virion Secretion

Author

Yuanjie Liu, Timothy M. Block, Ju-Tao Guo, Haitao Guo, Dawei Cai, Ran Yan, and Xuesen Zhao

Subjects

Hepatitis B virus, Glycosylphosphatidylinositols, viruses, Immunology, Alpha interferon, Biology, GPI-Linked Proteins, Virus Replication, medicine.disease_cause, Antiviral Agents, Microbiology, Virus, Cell Line, Capsid, Viral envelope, Antigens, CD, Interferon, Virology, medicine, Humans, Secretion, Virus Release, Interferon-alpha, virus diseases, digestive system diseases, Virus-Cell Interactions, Gene Expression Regulation, Viral replication, Insect Science, Hepatocytes, Tetherin, medicine.drug

Abstract

Interferon alpha (IFN-α) is an approved medication for chronic hepatitis B therapy. Besides acting as an immunomodulator, IFN-α elicits a pleiotropic antiviral state in hepatitis B virus (HBV)-infected hepatocytes, but whether or not IFN-α impedes the late steps of the HBV life cycle, such as HBV secretion, remains elusive. Here we report that IFN-α treatment of HepAD38 cells with established HBV replication selectively reduced HBV virion release without altering intracellular viral replication or the secretion of HBV subviral particles and nonenveloped capsids. In search of the interferon-stimulated gene(s) that is responsible for the reduction of HBV virion release, we found that tetherin, a broad-spectrum antiviral transmembrane protein that inhibits the egress of a variety of enveloped viruses, was highly induced by IFN-α in HepAD38 cells and in primary human hepatocytes. We further demonstrated that the expression of full-length tetherin, but not the C-terminal glycosylphosphatidylinositol (GPI) anchor-truncated form, inhibited HBV virion egress from HepAD38 cells. In addition, GPI anchor-truncated tetherin exhibited a dominant-negative effect and was incorporated into the liberated virions. We also found colocalization of tetherin and HBV L protein at the intracellular multivesicular body, where the budding of HBV virions takes place. In line with this, electron microscopy demonstrated that HBV virions were tethered in the lumen of the cisterna membrane under tetherin expression. Finally, knockdown of tetherin or overexpression of dominant negative tetherin attenuated the IFN-α-mediated reduction of HBV virion release. Taken together, our study suggests that IFN-α inhibits HBV virion egress from hepatocytes through the induction of tetherin. IMPORTANCE Tetherin is a host restriction factor that blocks the egress of a variety of enveloped viruses through tethering the budding virions on the cell surface with its membrane anchor domains. Here we report that interferon directly and selectively inhibits the secretion of HBV virions, but not subviral particles or nonenveloped capsids, through the induction of tetherin in hepatocyte-derived cells. The antiviral function of tetherin requires the carboxyl-terminal GPI anchor, while the GPI anchor deletion mutant exhibits dominant negative activity and attaches to liberated HBV virions. Consistent with the fact that HBV is an intracellular budding virus, microscopy analyses demonstrated that the tethering of HBV virions occurs in the intracellular cisterna and that tetherin colocalizes with HBV virions on the multivesicular body, which is the HBV virion budding site. Our study not only expands the antiviral spectrum of tetherin but also sheds light on the mechanisms of interferon-elicited anti-HBV responses.

Published

2015

32. Robust Protection against Highly Virulent Foot-and-Mouth Disease Virus in Swine by Combination Treatment with Recombinant Adenoviruses Expressing Porcine Alpha and Gamma Interferons and Multiple Small Interfering RNAs

Author

Su-Hwa You, Jong-Hyeon Park, Su-Mi Kim, Byounghan Kim, Min-Goo Seo, Kwang-Nyeong Lee, Dongseob Tark, Se-Kyung Kim, Taeseong Kim, and Hyang-Sim Lee

Subjects

Swine, Immunology, Alpha interferon, Biology, medicine.disease_cause, Microbiology, Virus, Adenoviridae, Interferon-gamma, Virology, Vaccines and Antiviral Agents, medicine, Animals, Interferon gamma, RNA, Small Interfering, Interferon alfa, Recombination, Genetic, Swine Diseases, Virulence, Viral Vaccine, Interferon-alpha, Viral Vaccines, biology.organism_classification, Vaccination, Foot-and-Mouth Disease Virus, Foot-and-Mouth Disease, Insect Science, Foot-and-mouth disease virus, medicine.drug

Abstract

Because the currently available vaccines against foot-and-mouth disease (FMD) provide no protection until 4 to 7 days postvaccination, the only alternative method to halt the spread of the FMD virus (FMDV) during outbreaks is the application of antiviral agents. Combination treatment strategies have been used to enhance the efficacy of antiviral agents, and such strategies may be advantageous in overcoming viral mechanisms of resistance to antiviral treatments. We have developed recombinant adenoviruses (Ads) for the simultaneous expression of porcine alpha and gamma interferons (Ad-porcine IFN-αγ) as well as 3 small interfering RNAs (Ad-3siRNA) targeting FMDV mRNAs encoding nonstructural proteins. The antiviral effects of Ad-porcine IFN-αγ and Ad-3siRNA expression were tested in combination in porcine cells, suckling mice, and swine. We observed enhanced antiviral effects in porcine cells and mice as well as robust protection against the highly pathogenic strain O/Andong/SKR/2010 and increased expression of cytokines in swine following combination treatment. In addition, we showed that combination treatment was effective against all serotypes of FMDV. Therefore, we suggest that the combined treatment with Ad-porcine IFN-αγ and Ad-3siRNA may offer fast-acting antiviral protection and be used with a vaccine during the period that the vaccine does not provide protection against FMD. IMPORTANCE The use of current foot-and-mouth disease (FMD) vaccines to induce rapid protection provides limited effectiveness because the protection does not become effective until a minimum of 4 days after vaccination. Therefore, during outbreaks antiviral agents remain the only available treatment to confer rapid protection and reduce the spread of foot-and-mouth disease virus (FMDV) in livestock until vaccine-induced protective immunity can become effective. Interferons (IFNs) and small interfering RNAs (siRNAs) have been reported to be effective antiviral agents against FMDV, although the virus has associated mechanisms of resistance to type I interferons and siRNAs. We have developed recombinant adenoviruses for the simultaneous expression of porcine alpha and gamma interferons (Ad-porcine IFN-αγ) as well as 3 small interfering RNAs (Ad-3siRNA) to enhance the inhibitory effects of these antiviral agents observed in previous studies. Here, we show enhanced antiviral effects against FMDV by combination treatment with Ad-porcine IFN-αγ and Ad-3siRNA to overcome the mechanisms of resistance of FMDV in swine.

Published

2015

33. Sequential Combination Therapy with Pegylated Interferon Leads to Loss of Hepatitis B Surface Antigen and Hepatitis B e Antigen (HBeAg) Seroconversion in HBeAg-Positive Chronic Hepatitis B Patients Receiving Long-Term Entecavir Treatment

Author

Lingyun Shao, Chang-Shui Li, Guojun Li, Bin Yi, Jiazhen Chen, Shu-Yuan Xie, Ping Fan, Xiao-Na Mao, Wenhong Zhang, Yiqi Yu, Wei-Cun Chen, Shaolong Chen, and He-Hui Zou

Subjects

Adult, Male, HBsAg, medicine.medical_specialty, Guanine, Endpoint Determination, Alpha interferon, Antiviral Agents, Gastroenterology, Polyethylene Glycols, Young Adult, Hepatitis B, Chronic, Predictive Value of Tests, Pegylated interferon, Internal medicine, medicine, Clinical endpoint, Humans, Pharmacology (medical), Hepatitis B e Antigens, Seroconversion, Retrospective Studies, Pharmacology, Hepatitis B Surface Antigens, business.industry, Interferon-alpha, virus diseases, Entecavir, Middle Aged, Hepatitis B, medicine.disease, Recombinant Proteins, digestive system diseases, Treatment Outcome, Infectious Diseases, HBeAg, Area Under Curve, Immunology, Female, business, medicine.drug

Abstract

Nucleos(t)ide analogues rarely result in a durable off-treatment response in chronic hepatitis B infection, whereas pegylated interferon (Peg-IFN) induces a long-lasting response only in a subset of patients. We assessed the effect of sequential combination therapy with Peg-IFN-α2a and entecavir in hepatitis B e antigen (HBeAg)-positive patients with prior long-term entecavir therapy and investigated the predictors of response to treatment. HBeAg-positive individuals who did not achieve HBeAg seroconversion during previous long-term entecavir therapy, receiving Peg-IFN-α2a added to ongoing entecavir therapy (sequential combination [S-C] therapy; n = 81) for 48 weeks or remaining on entecavir monotherapy ( n = 116), were retrospectively included. A matched pair was created at a 1:1 ratio from each treatment group. The primary endpoint was HBeAg seroconversion at week 48. Subgroup analysis of response prediction was conducted for 81 patients with S-C therapy. More patients in the S-C therapy group achieved HBeAg seroconversion than those in the entecavir group (44% versus 6%; P < 0.0001). An HBeAg level of P < 0.0001). Hepatitis B surface antigen (HBsAg) levels at baseline and the decrease in HBsAg levels predicted HBsAg loss in the S-C therapy group. The combination of baseline HBeAg of 10 IU/ml provided the highest rate of HBeAg seroconversion (92.31%) and HBsAg loss (83.3%) at week 48. Patients receiving sequential combination therapy have a higher rate of HBeAg seroconversion and are more likely to experience HBsAg clearance than do those continuing entecavir monotherapy. Sequential combination therapy can be guided by baseline HBsAg/HBeAg levels and on-treatment HBsAg dynamics.

Published

2015

34. Deep Sequencing and Phylogenetic Analysis of Variants Resistant to Interferon-Based Protease Inhibitor Therapy in Chronic Hepatitis Induced by Genotype 1b Hepatitis C Virus

Author

Tatsuya Yamaguchi, Mitsuaki Sato, Fumitake Amemiya, Yasuhiro Nakayama, Nobutoshi Komatsu, Taisuke Inoue, Shinichi Takano, Tadashi Sato, Yuichiro Suzuki, Masaru Muraoka, Minoru Sakamoto, Nobuyuki Enomoto, Shinya Maekawa, Akihisa Tatsumi, Kohji Moriishi, Tomoyoshi Uetake, Mitsuharu Fukasawa, Atsuya Yamashita, and Mika Miura

Subjects

Adult, Male, Genotype, Hepatitis C virus, Molecular Sequence Data, Immunology, Alpha interferon, Hepacivirus, Viral quasispecies, Viral Nonstructural Proteins, Biology, medicine.disease_cause, Antiviral Agents, Microbiology, Telaprevir, chemistry.chemical_compound, Interferon, Pegylated interferon, Virology, Drug Resistance, Viral, Ribavirin, medicine, Humans, Protease Inhibitors, Protease inhibitor (pharmacology), Phylogeny, Aged, Base Sequence, virus diseases, High-Throughput Nucleotide Sequencing, Interferon-alpha, Hepatitis C, Chronic, Middle Aged, digestive system diseases, Genetic Diversity and Evolution, chemistry, Insect Science, Female, Oligopeptides, Sequence Alignment, medicine.drug

Abstract

Because of recent advances in deep sequencing technology, detailed analysis of hepatitis C virus (HCV) quasispecies and their dynamic changes in response to direct antiviral agents (DAAs) became possible, although the role of quasispecies is not fully understood. In this study, to clarify the evolution of viral quasispecies and the origin of drug-resistant mutations induced by interferon (IFN)-based protease inhibitor therapy, the nonstructural-3 (NS3) region of genotype 1b HCV in 34 chronic hepatitis patients treated with telaprevir (TVR)/pegylated interferon (PEG-IFN)/ribavirin (RBV) was subjected to a deep sequencing study coupled with phylogenetic analysis. Twenty-six patients (76.5%) achieved a sustained viral response (SVR), while 8 patients did not (non-SVR; 23.5%). When the complexity of the quasispecies was expressed as the mutation frequency or Shannon entropy value, a significant decrease in the IFNL3 (rs8099917) TT group and a marginal decrease in the SVR group were found soon (12 h) after the introduction of treatment, whereas there was no decrease in the non-SVR group and no significant decrease in mutation frequency in the IFNL3 TG/GG group. In the analysis of viral quasispecies composition in non-SVR patients, major populations greatly changed, accompanied by the appearance of resistance, and the compositions were unlikely to return to the pretreatment composition even after the end of therapy. Clinically TVR-resistant variants were observed in 5 non-SVR patients (5/8, 62.5%), all of which were suspected to have acquired resistance by mutations through phylogenetic analysis. In conclusion, results of the study have important implications for treatment response and outcome in interferon-based protease inhibitor therapy. IMPORTANCE In the host, hepatitis C virus (HCV) consists of a variety of populations (quasispecies), and it is supposed that dynamic changes in quasispecies are closely related to pathogenesis, although this is poorly understood. In this study, recently developed deep sequencing technology was introduced, and changes in quasispecies associated with telaprevir (TVR)/pegylated interferon (PEG-IFN)/ribavirin (RBV) triple therapy and their clinical significance were investigated extensively by phylogenetic tree analysis. Through this study, the associations among treatment response, changes in viral quasispecies complexity in the early stage of treatment, changes in the quasispecies composition, and origin of TVR-resistant variant HCV were elucidated.

Published

2015

35. Expression of Human Decay-Accelerating Factor on Intestinal Epithelium of Transgenic Mice Does Not Facilitate Infection by the Enteral Route

Author

Le Shen, Matthew A. Odenwald, Jieyan Pan, Lili Zhang, Jerrold R. Turner, and Jeffrey M. Bergelson

Subjects

Genetically modified mouse, viruses, Transgene, Immunoblotting, Immunology, Fluorescent Antibody Technique, Alpha interferon, Mice, Transgenic, Biology, Real-Time Polymerase Chain Reaction, Microbiology, Mice, Intestinal mucosa, Virology, Enterovirus Infections, Animals, Humans, Intestinal Mucosa, Receptor, Decay-accelerating factor, DNA Primers, CD55 Antigens, Reverse Transcriptase Polymerase Chain Reaction, fungi, Immunohistochemistry, Intestinal epithelium, Enterovirus B, Human, Cell biology, Microscopy, Electron, Insect Science, Pathogenesis and Immunity, Disease Susceptibility, Ex vivo

Abstract

In vitro , infection of polarized human intestinal epithelial cells by coxsackievirus B3 (CVB3) depends on virus interaction with decay-accelerating factor (DAF), a receptor expressed on the apical cell surface. Although mice are highly susceptible to CVB3 infection when virus is delivered by intraperitoneal injection, infection by the enteral route is very inefficient. Murine DAF, unlike human DAF, does not bind virus, and we hypothesized that the absence of an accessible receptor on the intestinal surface is an important barrier to infection by the oral route. We generated transgenic mice that express human DAF specifically on intestinal epithelium and measured their susceptibility to infection by a DAF-binding CVB3 isolate. Human DAF permitted CVB3 to bind to the intestinal surface ex vivo and to infect polarized monolayers of small-intestinal epithelial cells derived from DAF transgenic mice. However, expression of human DAF did not facilitate infection by the enteral route either in immunocompetent animals or in animals deficient in the interferon alpha/beta receptor. These results indicate that the absence of an apical receptor on intestinal epithelium is not the major barrier to infection of mice by the oral route. IMPORTANCE CVB3 infection of human intestinal epithelial cells depends on DAF at the apical cell surface, and expression of human DAF on murine intestinal epithelial cells permits their infection in vitro . However, expression of human DAF on the intestinal surface of transgenic mice did not facilitate infection by the oral route. Although the role of intestinal DAF in human infection has not been directly examined, these results suggest that DAF is not the critical factor in mice.

Published

2015

36. An OPTIMIZE Study Retrospective Analysis for Management of Telaprevir-Treated Hepatitis C Virus (HCV)-Infected Patients by Use of the Abbott RealTi m e HCV RNA Assay

Author

Sandra De Meyer, Anne Ghys, James Witek, Maria Buti, Katrien Janssen, Donghan Luo, Christoph Sarrazin, I. Dierynck, Gaston Picchio, and Gavin Cloherty

Subjects

Microbiology (medical), Hepatitis C virus, Hepacivirus, Alpha interferon, medicine.disease_cause, Antiviral Agents, Telaprevir, chemistry.chemical_compound, Pegylated interferon, Virology, Ribavirin, TaqMan, Humans, Medicine, Retrospective Studies, biology, business.industry, Interferon-alpha, Hepatitis C, Chronic, Viral Load, biology.organism_classification, Treatment Outcome, Molecular Diagnostic Techniques, chemistry, RNA, Viral, Drug Therapy, Combination, Drug Monitoring, business, Oligopeptides, Viral load, medicine.drug

Abstract

Protease inhibitor (PI)-based response-guided triple therapies for hepatitis C virus (HCV) infection are still widely used. Noncirrhotic treatment-naive and prior relapser patients receiving telaprevir-based treatment are eligible for shorter, 24-week total therapy if HCV RNA is undetectable at both weeks 4 and 12. In this study, the concordance in HCV RNA assessments between the Roche High Pure System/Cobas TaqMan and Abbott RealTi m e HCV RNA assays and the impacts of different HCV RNA cutoffs on treatment outcome were evaluated. A total of 2,629 samples from 663 HCV genotype 1 patients receiving telaprevir/pegylated interferon/ribavirin in OPTIMIZE were analyzed using the High Pure System and reanalyzed using Abbott RealTi m e (limits of detection, 15.1 IU/ml versus 8.3 IU/ml; limits of quantification, 25 IU/ml versus 12 IU/ml, respectively). Overall, good concordance was observed between the assays. Using undetectable HCV RNA at week 4, 34% of the patients would be eligible for shorter treatment duration with Abbott RealTi m e versus 72% with the High Pure System. However, using m e, a similar proportion (74%) would be eligible. Of the patients receiving 24-week total therapy, 87% achieved a sustained virologic response with undetectable HCV RNA by the High Pure System or m e; however, 92% of the patients with undetectable HCV RNA by Abbott RealTi m e achieved a sustained virologic response. Using undetectable HCV RNA as the cutoff, the more sensitive Abbott RealTi m e assay would identify fewer patients eligible for shorter treatment than the High Pure System. Our data confirm the m e assay, to determine eligibility for shortened PI-based HCV treatment. (The study was registered with ClinicalTrials.gov under registration no. NCT01241760.)

Published

2015

37. Efficient Reverse Genetics Reveals Genetic Determinants of Budding and Fusogenic Differences between Nipah and Hendra Viruses and Enables Real-Time Monitoring of Viral Spread in Small Animal Models of Henipavirus Infection

Author

Terence E. Hill, Shannon M. Beaty, Tatyana Yun, Yao E. Wang, Benhur Lee, Frederic Vigant, Junling Gao, Lihong Zhang, Arnold Park, Terry L. Juelich, Alexander N. Freiberg, Olivier Pernet, Ping Wu, and Jennifer K. Smith

Subjects

Immunology, Alpha interferon, Biology, Microbiology, Hendra Virus, Viral entry, Virology, Animals, Humans, Paramyxovirinae, Virus Release, Henipavirus Infections, Mice, Knockout, Recombination, Genetic, Genetic Complementation Test, Nipah Virus, Virus Internalization, biology.organism_classification, Reverse Genetics, Reverse genetics, Disease Models, Animal, Viral Tropism, Viral replication, Insect Science, Tissue tropism, Pathogenesis and Immunity, Henipavirus

Abstract

Nipah virus (NiV) and Hendra virus (HeV) are closely related henipaviruses of the Paramyxovirinae . Spillover from their fruit bat reservoirs can cause severe disease in humans and livestock. Despite their high sequence similarity, NiV and HeV exhibit apparent differences in receptor and tissue tropism, envelope-mediated fusogenicity, replicative fitness, and other pathophysiologic manifestations. To investigate the molecular basis for these differences, we first established a highly efficient reverse genetics system that increased rescue titers by ≥3 log units, which offset the difficulty of generating multiple recombinants under constraining biosafety level 4 (BSL-4) conditions. We then replaced, singly and in combination, the matrix (M), fusion (F), and attachment glycoprotein (G) genes in mCherry-expressing recombinant NiV (rNiV) with their HeV counterparts. These chimeric but isogenic rNiVs replicated well in primary human endothelial and neuronal cells, indicating efficient heterotypic complementation. The determinants of budding efficiency, fusogenicity, and replicative fitness were dissociable: HeV-M budded more efficiently than NiV-M, accounting for the higher replicative titers of HeV-M-bearing chimeras at early times, while the enhanced fusogenicity of NiV-G-bearing chimeras did not correlate with increased replicative fitness. Furthermore, to facilitate spatiotemporal studies on henipavirus pathogenesis, we generated a firefly luciferase-expressing NiV and monitored virus replication and spread in infected interferon alpha/beta receptor knockout mice via bioluminescence imaging. While intraperitoneal inoculation resulted in neuroinvasion following systemic spread and replication in the respiratory tract, intranasal inoculation resulted in confined spread to regions corresponding to olfactory bulbs and salivary glands before subsequent neuroinvasion. This optimized henipavirus reverse genetics system will facilitate future investigations into the growing numbers of novel henipavirus-like viruses. IMPORTANCE Nipah virus (NiV) and Hendra virus (HeV) are recently emergent zoonotic and highly lethal pathogens with pandemic potential. Although differences have been observed between NiV and HeV replication and pathogenesis, the molecular basis for these differences has not been examined. In this study, we established a highly efficient system to reverse engineer changes into replication-competent NiV and HeV, which facilitated the generation of reporter-expressing viruses and recombinant NiV-HeV chimeras with substitutions in the genes responsible for viral exit (the M gene, critical for assembly and budding) and viral entry (the G [attachment] and F [fusion] genes). These chimeras revealed differences in the budding and fusogenic properties of the M and G proteins, respectively, which help explain previously observed differences between NiV and HeV. Finally, to facilitate future in vivo studies, we monitored the replication and spread of a bioluminescent reporter-expressing NiV in susceptible mice; this is the first time such in vivo imaging has been performed under BSL-4 conditions.

Published

2015

38. Interferon-Inducible CD169/Siglec1 Attenuates Anti-HIV-1 Effects of Alpha Interferon

Author

Zandrea Ambrose, Nora-Guadalupe P. Ramirez, Hisashi Akiyama, Gregory A. Gibson, Suryaram Gummuluru, Simon C. Watkins, and Christopher Kline

Subjects

CD4-Positive T-Lymphocytes, 0301 basic medicine, Cell type, Sialic Acid Binding Ig-like Lectin 1, Immunology, Simian Acquired Immunodeficiency Syndrome, Alpha interferon, HIV Infections, Biology, medicine.disease_cause, Antiviral Agents, Microbiology, Proinflammatory cytokine, 03 medical and health sciences, 0302 clinical medicine, In vivo, Viral entry, Interferon, Virology, medicine, Animals, Humans, Cells, Cultured, Macrophages, Interferon-alpha, Dendritic Cells, Dendritic cell, Simian immunodeficiency virus, Virus-Cell Interactions, 030104 developmental biology, 030220 oncology & carcinogenesis, Insect Science, HIV-1, Simian Immunodeficiency Virus, Macaca nemestrina, medicine.drug

Abstract

A hallmark of human immunodeficiency virus type 1 (HIV-1) infection in vivo is chronic immune activation concomitant with type I interferon (IFN) production. Although type I IFN induces an antiviral state in many cell types, HIV-1 can replicate in vivo via mechanisms that have remained unclear. We have recently identified a type I IFN-inducible protein, CD169, as the HIV-1 attachment factor on dendritic cells (DCs) that can mediate robust infection of CD4 + T cells in trans . Since CD169 expression on macrophages is also induced by type I IFN, we hypothesized that type I IFN-inducible CD169 could facilitate productive HIV-1 infection in myeloid cells in cis and CD4 + T cells in trans and thus offset antiviral effects of type I IFN. In support of this hypothesis, infection of HIV-1 or murine leukemia virus Env (MLV-Env)-pseudotyped HIV-1 particles was enhanced in IFN-α-treated THP-1 monocytoid cells, and this enhancement was primarily dependent on CD169-mediated enhancement at the virus entry step, a phenomenon phenocopied in HIV-1 infections of IFN-α-treated primary monocyte-derived macrophages (MDMs). Furthermore, expression of CD169, a marker of type I IFN-induced immune activation in vivo , was enhanced in lymph nodes from pigtailed macaques infected with simian immunodeficiency virus (SIV) carrying HIV-1 reverse transcriptase (RT-SHIV), compared to uninfected macaques, and interestingly, there was extensive colocalization of p27 gag and CD169, suggesting productive infection of CD169 + myeloid cells in vivo . While cell-free HIV-1 infection of IFN-α-treated CD4 + T cells was robustly decreased, initiation of infection in trans via coculture with CD169 + IFN-α-treated DCs restored infection, suggesting that HIV-1 exploits CD169 in cis and in trans to attenuate a type I IFN-induced antiviral state. IMPORTANCE HIV-1 infection in humans causes immune activation characterized by elevated levels of proinflammatory cytokines, including type I interferons (IFN). Although type I IFN induces an antiviral state in many cell types in vitro , HIV-1 can replicate in vivo via mechanisms that have remained unclear. In this study, we tested the hypothesis that CD169, a type I IFN-inducible HIV-1 attachment factor, offsets antiviral effects of type I IFN. Infection of HIV-1 was rescued in IFN-α-treated myeloid cells via upregulation of CD169 and a subsequent increase in CD169-dependent virus entry. Furthermore, extensive colocalization of viral Gag and CD169 was observed in lymph nodes of infected pigtailed macaques, suggesting productive infection of CD169 + cells in vivo . Treatment of dendritic cell (DC)-T cell cocultures with IFN-α upregulated CD169 expression on DCs and rescued HIV-1 infection of CD4 + T cells in trans , suggesting that HIV-1 exploits CD169 to attenuate type I IFN-induced restrictions.

Published

2017

39. Zika Virus Infects Human Sertoli Cells and Modulates the Integrity of the In Vitro Blood-Testis Barrier Model

Author

David N. Siemann, Pei Yong Shi, Payal N. Maharaj, Daniel P. Strange, and Saguna Verma

Subjects

0301 basic medicine, Male, Sexual transmission, 030106 microbiology, Immunology, Alpha interferon, Vascular Cell Adhesion Molecule-1, Receptors, Cell Surface, Dengue virus, Biology, medicine.disease_cause, Microbiology, Dengue, 03 medical and health sciences, Virology, medicine, Humans, Claudin, Blood-Testis Barrier, Cells, Cultured, Blood–testis barrier, Innate immune system, Sertoli Cells, Cell adhesion molecule, Zika Virus Infection, Macrophages, Interferon-alpha, Zika Virus, Dengue Virus, Sertoli cell, Cell biology, Virus-Cell Interactions, 030104 developmental biology, medicine.anatomical_structure, Insect Science, Claudins, Zonula Occludens-1 Protein, Cell Adhesion Molecules

Abstract

Confirmed reports of Zika virus (ZIKV) in human seminal fluid for months after the clearance of viremia suggest the ability of ZIKV to establish persistent infection in the seminiferous tubules, an immune-privileged site in the testis protected by the blood-testis barrier, also called the Sertoli cell (SC) barrier (SCB). However, cellular targets of ZIKV in human testis and mechanisms by which the virus enters seminiferous tubules remain unclear. We demonstrate that primary human SCs were highly susceptible to ZIKV compared to the closely related dengue virus and induced the expression of alpha interferon (IFN-α), key cytokines, and cell adhesion molecules (vascular cell adhesion molecule 1 [VCAM-1] and intracellular adhesion molecule 1 [ICAM-1]). Furthermore, using an in vitro SCB model, we show that ZIKV was released on the adluminal side of the SCB model with a higher efficiency than in the blood-brain barrier model. ZIKV-infected SCs exhibited enhanced adhesion of leukocytes that correlated with decreases in SCB integrity. ZIKV infection did not affect the expression of tight and adherens junction proteins such as ZO-1, claudin, and JAM-A; however, exposure of SCs to inflammatory mediators derived from ZIKV-infected macrophages led to the degradation of the ZO-1 protein, which correlated with increased SCB permeability. Taken together, our data suggest that infection of SCs may be one of the crucial steps by which ZIKV gains access to the site of spermatozoon development and identify SCs as a therapeutic target to clear testicular infections. The SCB model opens up opportunities to assess interactions of SCs with other testicular cells and to test the ability of anti-ZIKV drugs to cross the barrier. IMPORTANCE Recent outbreaks of ZIKV, a neglected mosquito-borne flavivirus, have identified sexual transmission as a new route of disease spread, which has not been reported for other flaviviruses. To be able to sexually transmit for months after the clearance of viremia, ZIKV must establish infection in the seminiferous tubules, the site of spermatozoon development. However, little is known about the cell types that support ZIKV infection in the human testis. Currently, there are no models to study mechanisms of virus persistence in the seminiferous tubules. We provide evidence that ZIKV infection of human Sertoli cells, which are an important component of the seminiferous tubules, is robust and induces a strong antiviral response. The use of an in vitro Sertoli cell barrier to describe how ZIKV or inflammatory mediators derived from ZIKV-infected macrophages compromise barrier integrity will enable studies to explore the interactions of other testicular cells with Sertoli cells and to test novel antivirals for clearing testicular ZIKV infection.

Published

2017

40. Transcriptomic Signatures of Tacaribe Virus-Infected Jamaican Fruit Bats

Author

Diana L. Gerrard, Ann Hawkinson, Tyler Sherman, Cassandra M. Modahl, Gretchen Hume, Corey L. Campbell, Tony Schountz, Seth Frietze, and Christina F. Spiropoulou

Subjects

0301 basic medicine, Immunoglobulin gene, Molecular Biology and Physiology, viruses, bats, lcsh:QR1-502, Alpha interferon, Microbiology, lcsh:Microbiology, Virus, 03 medical and health sciences, Immune system, arenavirus, Molecular Biology, Gene, Artibeus, virus-host interactions, Arenavirus, 030102 biochemistry & molecular biology, biology, Acquired immune system, biology.organism_classification, Virology, QR1-502, 3. Good health, 030104 developmental biology, transcriptome, Research Article

Abstract

As reservoir hosts of viruses associated with human disease, little is known about the interactions between bats and viruses. Using Jamaican fruit bats infected with Tacaribe virus (TCRV) as a model, we characterized the gene expression responses to infection in different tissues and identified pathways involved with the response to infection. This report is the most detailed gene discovery work in the species to date and the first to describe immune gene expression responses in bats during a pathogenic viral infection., Tacaribe virus (TCRV) is a mammalian arenavirus that was first isolated from artibeus bats in the 1950s. Subsequent experimental infection of Jamaican fruit bats (Artibeus jamaicensis) caused a disease similar to that of naturally infected bats. Although substantial attention has focused on bats as reservoir hosts of viruses that cause human disease, little is known about the interactions between bats and their pathogens. We performed a transcriptome-wide study to illuminate the response of Jamaican fruit bats experimentally infected with TCRV. Differential gene expression analysis of multiple tissues revealed global and organ-specific responses associated with innate antiviral responses, including interferon alpha/beta and Toll-like receptor signaling, activation of complement cascades, and cytokine signaling, among others. Genes encoding proteins involved in adaptive immune responses, such as gamma interferon signaling and costimulation of T cells by the CD28 family, were also altered in response to TCRV infection. Immunoglobulin gene expression was also elevated in the spleens of infected bats, including IgG, IgA, and IgE isotypes. These results indicate an active innate and adaptive immune response to TCRV infection occurred but did not prevent fatal disease. This de novo assembly provides a high-throughput data set of the Jamaican fruit bat and its host response to TCRV infection, which remains a valuable tool to understand the molecular signatures involved in antiviral responses in bats. IMPORTANCE As reservoir hosts of viruses associated with human disease, little is known about the interactions between bats and viruses. Using Jamaican fruit bats infected with Tacaribe virus (TCRV) as a model, we characterized the gene expression responses to infection in different tissues and identified pathways involved with the response to infection. This report is the most detailed gene discovery work in the species to date and the first to describe immune gene expression responses in bats during a pathogenic viral infection.

Published

2017

41. Genotype 2 Strains of Porcine Reproductive and Respiratory Syndrome Virus Dysregulate Alveolar Macrophage Cytokine Production via the Unfolded Protein Response

Author

Wei Yu Chen, Gabriela Calzada-Nova, Federico A. Zuckermann, and William M. Schniztlein

Subjects

0301 basic medicine, Lipopolysaccharides, Genotype, 040301 veterinary sciences, Swine, medicine.medical_treatment, Immunology, Eukaryotic Initiation Factor-2, Porcine Reproductive and Respiratory Syndrome, Alpha interferon, Cellular Response to Infection, Biology, Virus Replication, Microbiology, Proinflammatory cytokine, Cell Line, 0403 veterinary science, 03 medical and health sciences, eIF-2 Kinase, Virology, Macrophages, Alveolar, medicine, Animals, Porcine respiratory and reproductive syndrome virus, Tumor Necrosis Factor-alpha, Interferon-alpha, 04 agricultural and veterinary sciences, Porcine reproductive and respiratory syndrome virus, biology.organism_classification, Protein kinase R, 030104 developmental biology, Cytokine, Insect Science, Unfolded protein response, Unfolded Protein Response, Tumor necrosis factor alpha, Translational attenuation

Abstract

Porcine reproductive and respiratory syndrome virus (PRRSV) infects alveolar macrophages (AMϕ), causing dysregulated alpha interferon (IFN-α) and tumor necrosis factor alpha (TNF-α) production through a mechanism(s) yet to be resolved. Here, we show that AMϕ infected with PRRSV secreted a reduced quantity of IFN-α following exposure of the cell to synthetic double-stranded RNA (dsRNA). This reduction did not correlate with reduced IFNA1 gene transcription. Rather, it coincided with two events that occurred late during infection and that were indicative of translational attenuation, specifically, the activation of eukaryotic translation initiation factor 2α (eIF2α) and the appearance of stress granules. Notably, the typical rapid production of TNF-α by AMϕ exposed to lipopolysaccharide (LPS) was suppressed or enhanced by PRRSV, depending on when the LPS exposure occurred after virus infection. If exposure was delayed until 6 h postinfection (hpi) so that the development of the cytokine response coincided with the time in which phosphorylation of eIF2α by the stress sensor PERK (protein kinase RNA [PKR]-like ER kinase) occurred, inhibition of TNF-α production was observed. However, if LPS exposure occurred at 2 hpi, prior to a detectable onset of eIF2α phosphorylation, a synergistic response was observed due to the earlier NF-κB activation via the stress sensor IRE1α (inositol-requiring kinase 1α). These results suggest that the asynchronous actions of two branches of the unfolded protein response (UPR), namely, IRE1α, and PERK, activated by ER stress resulting from the virus infection, are associated with enhancement or suppression of TNF-α production, respectively. IMPORTANCE The activation of AMϕ is controlled by the microenvironment to deter excessive proinflammatory cytokine responses to microbes that could impair lung function. However, viral pneumonias frequently become complicated by secondary bacterial infections, triggering severe inflammation, lung dysfunction, and death. Although dysregulated cytokine production is considered an integral component of the exacerbated inflammatory response in viral-bacterial coinfections, the mechanism responsible for this event is unknown. Here, we show that PRRSV replication in porcine AMϕ triggers activation of the IRE1α branch of the UPR, which causes a synergistic TNF-α response to LPS exposure. Thus, the severe pneumonias typically observed in pigs afflicted with PRRSV-bacterial coinfections could result from dysregulated, overly robust TNF-α production in response to opportunistic pathogens that is not commensurate with the typical restrained reaction by uninfected AMϕ. This notion could help in the design of therapies to mitigate the severity of viral and bacterial coinfections.

Published

2017

42. Human Metapneumovirus M2-2 Protein Acts as a Negative Regulator of Alpha Interferon Production by Plasmacytoid Dendritic Cells

Author

Bin Gotoh, Madoka Sakai, Masae Itoh, Mariko Funayama, and Yoshinori Kitagawa

Subjects

Bioluminescence Resonance Energy Transfer Techniques, 0301 basic medicine, Interferon Regulatory Factor-7, Immunology, Alpha interferon, Plasmacytoid dendritic cell, Transfection, Microbiology, Open Reading Frames, Viral Proteins, 03 medical and health sciences, Pneumovirinae, 0302 clinical medicine, Human metapneumovirus, Interferon, Virology, medicine, Humans, Paramyxovirinae, Phosphorylation, Immune Evasion, TNF Receptor-Associated Factor 6, biology, Genetic Complementation Test, Intracellular Signaling Peptides and Proteins, Interferon-alpha, Dendritic Cells, biology.organism_classification, I-kappa B Kinase, Cell biology, HEK293 Cells, 030104 developmental biology, Toll-Like Receptor 7, Toll-Like Receptor 9, Insect Science, Myeloid Differentiation Factor 88, Pathogenesis and Immunity, IRF7, Metapneumovirus, Signal Transduction, 030215 immunology, medicine.drug

Abstract

Human metapneumovirus (HMPV) has the ability to inhibit Toll-like receptor 7 (TLR7)- and TLR9-dependent alpha interferon (IFN-α) production by plasmacytoid dendritic cells (pDCs). However, the inhibition mechanism remains largely unknown. To identify viral proteins responsible for this inhibition, we performed a screening of HMPV open reading frames (ORFs) for the ability to block TLR7/9-dependent signaling reconstituted in HEK293T cells by transfection with myeloid differentiation factor 88 (MyD88), tumor necrosis factor receptor-associated factor 6 (TRAF6), IKKα, and IFN regulatory factor 7 (IRF7). This screening demonstrated that the M2-2 protein was the most potent inhibitor of TLR7/9-dependent IFN-α induction. A recombinant HMPV in which the M2-2 ORF was silenced indeed induced greater IFN-α production by human pDCs than wild-type HMPV did. Immunoprecipitation experiments showed direct physical association of the M2-2 protein with the inhibitory domain (ID) of IRF7. As a natural consequence of this, transfection of IRF7 lacking the ID, a constitutively active mutant, resulted in activation of the IFN-α promoter even in the presence of M2-2. Bioluminescence resonance energy transfer assays and split Renilla luciferase complementation assays revealed that M2-2 inhibited MyD88/TRAF6/IKKα-induced homodimerization of IRF7. In contrast, expression of the M2-2 protein did not result in inhibition of IPS-1-induced homodimerization and resultant activation of IRF7. This indicates that inhibition of MyD88/TRAF6/IKKα-induced IRF7 homodimerization does not result from a steric effect of M2-2 binding. Instead, it was found that M2-2 inhibited MyD88/TRAF6/IKKα-induced phosphorylation of IRF7 on Ser477. These results suggest that M2-2 blocks TLR7/9-dependent IFN-α induction by preventing IRF7 homodimerization, possibly through its effects on the phosphorylation status of IRF7. IMPORTANCE The family Paramyxoviridae is divided into two subfamilies, the Paramyxovirinae and the Pneumovirinae . Members of the subfamily Paramyxovirinae have the ability to inhibit TLR7/9-dependent IFN-α production, and the underlying inhibition mechanism has been intensively studied. In contrast, little is known about how members of the subfamily Pneumovirinae regulate IFN-α production by pDCs. We identified the M2-2 protein of HMPV, a member of the subfamily Pneumovirinae , as a negative regulator of IFN-α production by pDCs and uncovered the underlying mechanism. This study explains in part why the M2-2 knockout recombinant HMPV is attenuated and further suggests that M2-2 is a potential target for HMPV therapy.

Published

2017

43. Zika Virus Persistently Infects and Is Basolaterally Released from Primary Human Brain Microvascular Endothelial Cells

Author

Megan C. Mladinich, John Schwedes, Erich R. Mackow, and Glen Nemerow

Subjects

0301 basic medicine, Chemokine, Transplacental transmission, chemokine CCL5, Interferon Regulatory Factor-7, human brain endothelial cells, Alpha interferon, Virus Replication, Antiviral Agents, cell survival, Microbiology, CCL5, innate immune regulation, Zika virus, 03 medical and health sciences, transcriptome analysis, basolateral release, Virology, Endopeptidases, Humans, Cells, Cultured, Virus Release, persistent infection, biology, ISG15 induction, Gene Expression Profiling, Intracellular Signaling Peptides and Proteins, Brain, Endothelial Cells, Interferon-alpha, Interferon-beta, Virus Internalization, biology.organism_classification, ISG15, Immunity, Innate, Interferon-Stimulated Gene Factor 3, gamma Subunit, IFN-β regulation, QR1-502, 3. Good health, Flavivirus, 030104 developmental biology, Microvessels, biology.protein, IRF7, Ubiquitin Thiolesterase, Research Article

Abstract

Zika virus (ZIKV) is a mosquito-borne Flavivirus that has emerged as the cause of encephalitis and fetal microencephaly in the Americas. ZIKV uniquely persists in human bodily fluids for up to 6 months, is sexually transmitted, and traverses the placenta and the blood-brain barrier (BBB) to damage neurons. Cells that support persistent ZIKV replication and mechanisms by which ZIKV establishes persistence remain enigmatic but central to ZIKV entry into protected neuronal compartments. The endothelial cell (EC) lining of capillaries normally constrains transplacental transmission and forms the BBB, which selectively restricts access of blood constituents to neurons. We found that ZIKV (strain PRVABC59) persistently infects and continuously replicates in primary human brain microvascular ECs (hBMECs), without cytopathology, for >9 days and following hBMEC passage. ZIKV did not permeabilize hBMECs but was released basolaterally from polarized hBMECs, suggesting a direct mechanism for ZIKV to cross the BBB. ZIKV-infected hBMECs were rapidly resistant to alpha interferon (IFN-α) and transiently induced, but failed to secrete, IFN-β and IFN-λ. Global transcriptome analysis determined that ZIKV constitutively induced IFN regulatory factor 7 (IRF7), IRF9, and IFN-stimulated genes (ISGs) 1 to 9 days postinfection, despite persistently replicating in hBMECs. ZIKV constitutively induced ISG15, HERC5, and USP18, which are linked to hepatitis C virus (HCV) persistence and IFN regulation, chemokine CCL5, which is associated with immunopathogenesis, as well as cell survival factors. Our results reveal that hBMECs act as a reservoir of persistent ZIKV replication, suggest routes for ZIKV to cross hBMECs into neuronal compartments, and define novel mechanisms of ZIKV persistence that can be targeted to restrict ZIKV spread., IMPORTANCE ZIKV persists in patients, crossing placental and neuronal barriers, damaging neurons, and causing fetal microencephaly. We found that ZIKV persistently infects brain endothelial cells that normally protect neurons from viral exposure. hBMECs are not damaged by ZIKV infection and, analogous to persistent HCV infection, ZIKV constitutively induces and evades antiviral ISG and IFN responses to continuously replicate in hBMECs. As a result, hBMECs provide a protective niche for systemic ZIKV spread and a viral reservoir localized in the normally protective blood-brain barrier. Consistent with the spread of ZIKV into neuronal compartments, ZIKV was released basolaterally from hBMECs. Our findings define hBMEC responses that contribute to persistent ZIKV infection and potential targets for clearing ZIKV infections from hBMECs. These results further suggest roles for additional ZIKV-infected ECs to facilitate viral spread and persistence in the protected placental, retinal, and testicular compartments.

Published

2017

44. BST-2 Expression Modulates Small CD4-Mimetic Sensitization of HIV-1-Infected Cells to Antibody-Dependent Cellular Cytotoxicity

Author

Amos B. Smith, Mathieu Coutu, Nathalie Brassard, Andrés Finzi, Shilei Ding, David T. Evans, Benjamin von Bredow, Stuart J. D. Neil, Halima Medjahed, Daniel Sauter, Jonathan Richard, Joseph Sodroski, Beatrice H. Hahn, Katrina Gee, Frank Kirchhoff, Frederic Bibollet-Ruche, Bruno Melillo, Jérémie Prévost, and Daniel Kaufmann

Subjects

0301 basic medicine, viruses, Human Immunodeficiency Virus Proteins, Immunology, Alpha interferon, GPI-Linked Proteins, medicine.disease_cause, Microbiology, Jurkat cells, Epitope, Epitopes, Jurkat Cells, 03 medical and health sciences, Immune system, Downregulation and upregulation, Antigens, CD, Virology, medicine, Humans, Viral Regulatory and Accessory Proteins, Immune Evasion, Antibody-dependent cell-mediated cytotoxicity, biology, Interleukins, Molecular Mimicry, Antibody-Dependent Cell Cytotoxicity, env Gene Products, Human Immunodeficiency Virus, virus diseases, Interferon-beta, Up-Regulation, Molecular mimicry, 030104 developmental biology, Insect Science, CD4 Antigens, HIV-1, biology.protein, Pathogenesis and Immunity, Antibody

Abstract

Antibodies recognizing conserved CD4-induced (CD4i) epitopes on human immunodeficiency virus type 1 (HIV-1) Env and able to mediate antibody-dependent cellular cytotoxicity (ADCC) have been shown to be present in sera from most HIV-1-infected individuals. These antibodies preferentially recognize Env in its CD4-bound conformation. CD4 downregulation by Nef and Vpu dramatically reduces exposure of CD4i HIV-1 Env epitopes and therefore reduce the susceptibility of HIV-1-infected cells to ADCC mediated by HIV-positive (HIV+) sera. Importantly, this mechanism of immune evasion can be circumvented with small-molecule CD4 mimetics (CD4mc) that are able to transition Env into the CD4-bound conformation and sensitize HIV-1-infected cells to ADCC mediated by HIV+ sera. However, HIV-1 developed additional mechanisms to avoid ADCC, including Vpu-mediated BST-2 antagonism, which decreases the overall amount of Env present at the cell surface. Accordingly, BST-2 upregulation in response to alpha interferon (IFN-α) was shown to increase the susceptibility of HIV-1-infected cells to ADCC despite the activity of Vpu. Here we show that BST-2 upregulation by IFN-β and interleukin-27 (IL-27) also increases the surface expression of Env and thus boosts the ability of CD4mc to sensitize HIV-1-infected cells to ADCC by sera from HIV-1-infected individuals. IMPORTANCE HIV-1 evolved sophisticated strategies to conceal Env epitopes from ADCC-mediating antibodies present in HIV+ sera. Vpu-mediated BST-2 downregulation was shown to decrease ADCC responses by limiting the amount of Env present at the cell surface. This effect of Vpu was shown to be attenuated by IFN-α treatment. Here we show that in addition to IFN-α, IFN-β and IL-27 also affect Vpu-mediated BST-2 downregulation and greatly enhance ADCC responses against HIV-1-infected cells in the presence of CD4mc. These findings may inform strategies aimed at HIV prevention and eradication.

Published

2017

45. Topoisomerase II Inhibitors Induce DNA Damage-Dependent Interferon Responses Circumventing Ebola Virus Immune Evasion

Author

Priya Luthra, Sebastian Aguirre, Benjamin C. Yen, Colette A. Pietzsch, Maria T. Sanchez-Aparicio, Bersabeh Tigabu, Lorraine K. Morlock, Adolfo García-Sastre, Daisy W. Leung, Noelle S. Williams, Ana Fernandez-Sesma, Alexander Bukreyev, Christopher F. Basler, and Terence S. Dermody

Subjects

0301 basic medicine, cGAS-STING pathway, viruses, Alpha interferon, medicine.disease_cause, Virus Replication, Antiviral Agents, Microbiology, Cell Line, 03 medical and health sciences, Ebola virus, 0302 clinical medicine, Interferon, ATM signaling, Virology, medicine, Humans, Topoisomerase II Inhibitors, Immune Evasion, biology, Topoisomerase, RNA, RNA virus, biology.organism_classification, Ebolavirus, QR1-502, 3. Good health, 030104 developmental biology, Viral replication, innate immune responses, 030220 oncology & carcinogenesis, biology.protein, DNA damage, Interferons, Topoisomerase-II Inhibitor, medicine.drug, Research Article

Abstract

Ebola virus (EBOV) protein VP35 inhibits production of interferon alpha/beta (IFN) by blocking RIG-I-like receptor signaling pathways, thereby promoting virus replication and pathogenesis. A high-throughput screening assay, developed to identify compounds that either inhibit or bypass VP35 IFN-antagonist function, identified five DNA intercalators as reproducible hits from a library of bioactive compounds. Four, including doxorubicin and daunorubicin, are anthracycline antibiotics that inhibit topoisomerase II and are used clinically as chemotherapeutic drugs. These compounds were demonstrated to induce IFN responses in an ATM kinase-dependent manner and to also trigger the DNA-sensing cGAS-STING pathway of IFN induction. These compounds also suppress EBOV replication in vitro and induce IFN in the presence of IFN-antagonist proteins from multiple negative-sense RNA viruses. These findings provide new insights into signaling pathways activated by important chemotherapy drugs and identify a novel therapeutic approach for IFN induction that may be exploited to inhibit RNA virus replication., IMPORTANCE Ebola virus and other emerging RNA viruses are significant but unpredictable public health threats. Therapeutic approaches with broad-spectrum activity could provide an attractive response to such infections. We describe a novel assay that can identify small molecules that overcome Ebola virus-encoded innate immune evasion mechanisms. This assay identified as hits cancer chemotherapeutic drugs, including doxorubicin. Follow-up studies provide new insight into how doxorubicin induces interferon (IFN) responses, revealing activation of both the DNA damage response kinase ATM and the DNA sensor cGAS and its partner signaling protein STING. The studies further demonstrate that the ATM and cGAS-STING pathways of IFN induction are a point of vulnerability not only for Ebola virus but for other RNA viruses as well, because viral innate immune antagonists consistently fail to block these signals. These studies thereby define a novel avenue for therapeutic intervention against emerging RNA viruses.

Published

2017

46. Interferon Regulatory Factor 1 and Type I Interferon Cooperate To Control Acute Gammaherpesvirus Infection

Author

Philip T. Lange, Wadzanai P. Mboko, Michaela M. Rekow, Sean Anderson, Mitchell P. Ledwith, Kaitlin E. Schmitz, and Vera L. Tarakanova

Subjects

0301 basic medicine, Interferon-Induced Helicase, IFIH1, Interferon Regulatory Factor-7, viruses, Primary Cell Culture, Immunology, Antigens, Differentiation, Myelomonocytic, Alpha interferon, Receptor, Interferon alpha-beta, Biology, Microbiology, Virus, Interferon-gamma, Mice, 03 medical and health sciences, Gammaherpesvirinae, Immune system, Interferon, Virology, medicine, Animals, Humans, Interferon gamma, Lung, Mice, Knockout, Macrophages, virus diseases, Interferon-alpha, Proteins, Antigens, Nuclear, Herpesviridae Infections, Interferon-beta, biochemical phenomena, metabolism, and nutrition, Survival Analysis, Mice, Inbred C57BL, Chronic infection, 030104 developmental biology, IRF1, Gene Expression Regulation, Viral replication, Insect Science, Host-Pathogen Interactions, Pathogenesis and Immunity, Interferon Regulatory Factor-3, Spleen, Interferon Regulatory Factor-1, Signal Transduction, medicine.drug

Abstract

Gammaherpesviruses are ubiquitous pathogens that establish lifelong infection in >95% of adults worldwide and are associated with a variety of malignancies. Coevolution of gammaherpesviruses with their hosts has resulted in an intricate relationship between the virus and the host immune system, and perturbation of the virus-host balance results in pathology. Interferon regulatory factor 1 (IRF-1) is a tumor suppressor that is also involved in the regulation of innate and adaptive immune responses. Here, we show that type I interferon (IFN) and IRF-1 cooperate to control acute gammaherpesvirus infection. Specifically, we demonstrate that a combination of IRF-1 and type I IFN signaling ensures host survival during acute gammaherpesvirus infection and supports IFN gamma-mediated suppression of viral replication. Thus, our studies reveal an intriguing cross talk between IRF-1 and type I and II IFNs in the induction of the antiviral state during acute gammaherpesvirus infection. IMPORTANCE Gammaherpesviruses establish chronic infection in a majority of adults, and this long-term infection is associated with virus-driven development of a range of malignancies. In contrast, a brief period of active gammaherpesvirus replication during acute infection of a naive host is subclinical in most individuals. Here, we discovered that a combination of type I interferon (IFN) signaling and interferon regulatory factor 1 (IRF-1) expression is required to ensure survival of a gammaherpesvirus-infected host past the first 8 days of infection. Specifically, both type I IFN receptor and IRF-1 expression potentiated antiviral effects of type II IFN to restrict gammaherpesvirus replication in vivo , in the lungs, and in vitro , in primary macrophage cultures.

Published

2017

47. TLR7 Agonist GS-9620 Is a Potent Inhibitor of Acute HIV-1 Infection in Human Peripheral Blood Mononuclear Cells

Author

Tomas Cihlar, Andrew Mulato, Derek Hansen, Joseph Hesselgesser, Rujuta A. Bam, Alivelu Irrinki, Stephen R. Yant, Gregg S. Jones, and Christian R. Frey

Subjects

CD4-Positive T-Lymphocytes, 0301 basic medicine, Alpha interferon, HIV Infections, CD8-Positive T-Lymphocytes, Virus Replication, Antiviral Agents, Peripheral blood mononuclear cell, Antibodies, GS-9620, 03 medical and health sciences, 0302 clinical medicine, Immune system, In vivo, Humans, Pharmacology (medical), TLR7, Pharmacology, human immunodeficiency virus, biology, Interleukin-6, Chemistry, Macrophages, Pteridines, virus diseases, Interferon-alpha, Virology, interferons, 030104 developmental biology, Infectious Diseases, Toll-Like Receptor 7, Viral replication, HIV-1, Leukocytes, Mononuclear, biology.protein, Antibody, Ex vivo, 030215 immunology

Abstract

GS-9620 is a potent and selective oral Toll-like receptor 7 (TLR7) agonist that directly activates plasmacytoid dendritic cells (pDCs). GS-9620 suppressed hepatitis B virus (HBV) in animal models of chronic infection and transiently activated HIV expression ex vivo in latently infected peripheral blood mononuclear cells (PBMCs) from virally suppressed patients. Currently, GS-9620 is under clinical evaluation for treating chronic HBV infection and for reducing latent reservoirs in virally suppressed HIV-infected patients. Here, we investigated the in vitro anti-HIV-1 activity of GS-9620. GS-9620 potently inhibited viral replication in PBMCs, particularly when it was added 24 to 48 h prior to HIV infection (50% effective concentration = 27 nM). Depletion of pDCs but not other immune cell subsets from PBMC cultures suppressed GS-9620 antiviral activity. Although GS-9620 was inactive against HIV in purified CD4 + T cells and macrophages, HIV replication was potently inhibited by conditioned medium derived from GS-9620-treated pDC cultures when added to CD4 + T cells prior to infection. This suggests that GS-9620-mediated stimulation of PBMCs induced the production of a soluble factor(s) inhibiting HIV replication in trans . GS-9620-treated PBMCs primarily showed increased production of interferon alpha (IFN-α), and cotreatment with IFN-α-blocking antibodies reversed the HIV-1-inhibitory effect of GS-9620. Additional studies demonstrated that GS-9620 inhibited a postentry event in HIV replication at a step coincident with or prior to reverse transcription. The simultaneous activation of HIV-1 expression and inhibition of HIV-1 replication are important considerations for the clinical evaluation of GS-9620 since these antiviral effects may help restrict potential local HIV spread upon in vivo latency reversal.

Published

2017

48. Transfer of the Amino-Terminal Nuclear Envelope Targeting Domain of Human MX2 Converts MX1 into an HIV-1 Resistance Factor

Author

Caroline Goujon, Tomas Doyle, Michael H. Malim, Wendy S. Barclay, Hélène Bauby, and Olivier Moncorgé

Subjects

Myxovirus Resistance Proteins, Nuclear Envelope, R Factors, Molecular Sequence Data, Immunology, Protein domain, Alpha interferon, Biology, Antiviral Agents, Microbiology, Virus, Cell Line, GTP Phosphohydrolases, Interferon, Cell Line, Tumor, Virology, medicine, Humans, Amino Acid Sequence, Peptide sequence, Effector, biology.organism_classification, Fusion protein, Recombinant Proteins, Virus-Cell Interactions, Cell biology, HEK293 Cells, Vesicular stomatitis virus, Insect Science, HIV-1, Interferons, Sequence Alignment, HeLa Cells, medicine.drug

Abstract

The myxovirus resistance 2 (MX2) protein of humans has been identified recently as an interferon (IFN)-inducible inhibitor of human immunodeficiency virus type 1 (HIV-1) that acts at a late postentry step of infection to prevent the nuclear accumulation of viral cDNA (C. Goujon et al., Nature 502:559–562, 2013, http://dx.doi.org/10.1038/nature12542 ; M. Kane et al., Nature 502:563–566, 2013, http://dx.doi.org/10.1038/nature12653 ; Z. Liu et al., Cell Host Microbe 14:398–410, 2013, http://dx.doi.org/10.1016/j.chom.2013.08.015 ). In contrast, the closely related human MX1 protein, which suppresses infection by a range of RNA and DNA viruses (such as influenza A virus [FluAV]), is ineffective against HIV-1. Using a panel of engineered chimeric MX1/2 proteins, we demonstrate that the amino-terminal 91-amino-acid domain of MX2 confers full anti-HIV-1 function when transferred to the amino terminus of MX1, and that this fusion protein retains full anti-FluAV activity. Confocal microscopy experiments further show that this MX1/2 fusion, similar to MX2 but not MX1, can localize to the nuclear envelope (NE), linking HIV-1 inhibition with MX accumulation at the NE. MX proteins are dynamin-like GTPases, and while MX1 antiviral function requires GTPase activity, neither MX2 nor MX1/2 chimeras require this attribute to inhibit HIV-1. This key discrepancy between the characteristics of MX1- and MX2-mediated viral resistance, together with previous observations showing that the L4 loop of the stalk domain of MX1 is a critical determinant of viral substrate specificity, presumably reflect fundamental differences in the mechanisms of antiviral suppression. Accordingly, we propose that further comparative studies of MX proteins will help illuminate the molecular basis and subcellular localization requirements for implementing the noted diversity of virus inhibition by MX proteins. IMPORTANCE Interferon (IFN) elicits an antiviral state in cells through the induction of hundreds of IFN-stimulated genes (ISGs). The human MX2 protein has been identified as a key effector in the suppression of HIV-1 infection by IFN. Here, we describe a molecular genetic approach, using a collection of chimeric MX proteins, to identify protein domains of MX2 that specify HIV-1 inhibition. The amino-terminal 91-amino-acid domain of human MX2 confers HIV-1 suppressor capabilities upon human and mouse MX proteins and also promotes protein accumulation at the nuclear envelope. Therefore, these studies correlate the cellular location of MX proteins with anti-HIV-1 function and help establish a framework for future mechanistic analyses of MX-mediated virus control.

Published

2014

49. Limited Type I Interferons and Plasmacytoid Dendritic Cells during Neonatal Respiratory Syncytial Virus Infection Permit Immunopathogenesis upon Reinfection

Author

John P. DeVincenzo, Young-In Kim, Greg I. Lee, Stephania A. Cormier, Li Shen, Dahui You, Bishwas Shrestha, and Jordy Saravia

Subjects

Adoptive cell transfer, Immunology, Alpha interferon, Receptors, Cell Surface, Respiratory Syncytial Virus Infections, Plasmacytoid dendritic cell, Biology, Microbiology, Virus, Mice, Th2 Cells, Immune system, Interferon, Virology, medicine, Animals, Humans, Lung, Vero Cells, Mice, Inbred BALB C, Innate immune system, Interferon-alpha, Dendritic Cells, Viral Load, Respiratory Syncytial Viruses, Insect Science, Pathogenesis and Immunity, Viral load, medicine.drug

Abstract

Respiratory syncytial virus (RSV) infection is the number one cause of bronchiolitis in infants, yet no vaccines are available because of a lack of knowledge of the infant immune system. Using a neonatal mouse model, we previously revealed that mice initially infected with RSV as neonates develop Th2-biased immunopathophysiologies during reinfection, and we demonstrated a role for enhanced interleukin-4 receptor α (IL-4Rα) expression on T helper cells in these responses. Here we show that RSV infection in neonates induced limited type I interferon (IFN) and plasmacytoid dendritic cell (pDC) responses. IFN alpha (IFN-α) treatment or adoptive transfer of adult pDCs capable of inducing IFN-α prior to neonatal RSV infection decreased Th2-biased immunopathogenesis during reinfection. A reduced viral load and downregulation of IL-4Rα on Th2 cells were observed in IFN-α-treated neonatal mice, suggesting dual mechanisms of action. IMPORTANCE Respiratory syncytial virus (RSV) is the most significant cause of lower respiratory tract infection in infancy worldwide. Despite the dire need, we have failed to produce efficacious RSV vaccines or therapeutics. Part of the reason for this failure is our lack of understanding of how RSV interacts with the infant immune system to suppress the development of protective immunity. In the study described in the present paper, we used a neonatal mouse model, which more closely mimics human infants, to study the role of the innate immune system, particularly type I interferons (IFNs) and plasmacytoid dendritic cells (pDCs), in the pathogenesis of RSV infection. RSV infection in neonates induced limited type I IFN and pDC responses. IFN-α treatment or adoptive transfer of adult pDCs capable of producing IFN-α prior to neonatal RSV infection decreased Th2-biased immunopathogenesis during reinfection. These data suggest that IFN-α is a promising target for future RSV vaccine design.

Published

2014

50. Type I Interferon Mimetics Bypass Vaccinia Virus Decoy Receptor Virulence Factor for Protection of Mice against Lethal Infection

Author

Howard M. Johnson and Chulbul M. Ahmed

Subjects

Microbiology (medical), Virulence Factors, Clinical Biochemistry, Immunology, Alpha interferon, Vaccinia virus, Receptor, Interferon alpha-beta, Biology, Virus Replication, Antiviral Agents, Virus, Mice, Viral Proteins, chemistry.chemical_compound, Interferon, Vaccinia, medicine, Animals, Immunology and Allergy, Decoy receptors, Receptor, Smallpox virus, Interferon-alpha, Virology, Mice, Inbred C57BL, chemistry, Receptors, Virus, Clinical Immunology, Female, Decoy, medicine.drug

Abstract

The canonical model of interferon (IFN) signaling focuses solely on the activation of STAT transcription factors which, according to the model, are initiated by the singular event of cross-linkage of the receptor extracellular domain by the IFN. The IFN has no further function beyond this. The model thus provides no approach to circumventing poxviruses decoy receptors that compete with the IFN receptors for IFNs. This simple event has allowed smallpox virus to decimate human populations throughout the ages. We have developed a noncanonical model of IFN signaling that has resulted in the development of small peptide mimetics to both types I and II IFNs. In this report, we focus on a type I IFN mimetic at positions 152 to 189, IFN-α1(152–189), which corresponds to the C terminus of human IFN-α1. This mimetic functions intracellularly and is thus not recognized by the B18R vaccinia virus decoy receptor. Mimetic synthesized with an attached palmitate (lipo-) for cell penetration protects mice from a lethal dose of vaccinia virus, while the parent IFN-α1 is ineffective. Unlike IFN-α1, the mimetic does not bind to the B18R decoy receptor. It further differs from the parent IFN in that it lacks the toxicity of weight loss and bone marrow suppression in mice while at the same time possessing a strong adjuvant effect on the immune system. The mimetic is thus an innate and adaptive immune regulator that is evidence of the dynamic nature of the noncanonical model of IFN signaling, in stark contrast to the canonical or classical model of signaling.

Published

2014