Your search keyword '"Carles Martínez-Romero"' showing total 22 results

1. Proteomic Identification of Potential Target Proteins of Cathepsin W for Its Development as a Drug Target for Influenza

Author

Sira C, Günther, Carles, Martínez-Romero, Milagros, Sempere Borau, Christine T N, Pham, Adolfo, García-Sastre, and Silke, Stertz

Subjects

Proteomics, Mice, Cathepsin W, Influenza A virus, Host-Pathogen Interactions, Influenza, Human, Animals, Humans, Antiviral Agents

Abstract

Influenza A virus (IAV) coopts numerous host factors for efficient replication. The cysteine protease cathepsin W (CTSW) has been identified as one host factor required for IAV entry, specifically for the escape of IAVs from late endosomes. However, the substrate specificity of CTSW and the proviral mechanism are thus far unknown. Here, we show that intracellular but not secreted CTSW promotes viral entry. We reveal 79 potential direct and 31 potential indirect cellular target proteins of CTSW using the high-throughput proteomic approach terminal amine isotopic labeling of substrates (TAILS) and determine the cleavage motif shared by the substrates of CTSW. Subsequent integration with data from RNA interference (RNAi) screens for IAV host factors uncovers first insights into the proviral function of CTSW. Notably, CTSW-deficient mice display a 25% increase in survival and a delay in mortality compared to wild-type mice upon IAV infection. Altogether, these findings support the development of drugs targeting CTSW as novel host-directed antiviral therapies.

Published

2022

2. Characterization of SARS-CoV-2 Spike mutations important for infection of mice and escape from human immune sera

Author

Raveen, Rathnasinghe, Sonia, Jangra, Chengjin, Ye, Anastasija, Cupic, Gagandeep, Singh, Carles, Martínez-Romero, Lubbertus C F, Mulder, Thomas, Kehrer, Soner, Yildiz, Angela, Choi, Stephen T, Yeung, Ignacio, Mena, Virginia, Gillespie, Jana, De Vrieze, Sadaf, Aslam, Daniel, Stadlbauer, David A, Meekins, Chester D, McDowell, Velmurugan, Balaraman, Michael J, Corley, Juergen A, Richt, Bruno G, De Geest, Lisa, Miorin, Florian, Krammer, Luis, Martinez-Sobrido, Viviana, Simon, Adolfo, García-Sastre, and Amber S, Shin

Subjects

Multidisciplinary, SARS-CoV-2, Immune Sera, COVID-19, General Physics and Astronomy, General Chemistry, General Biochemistry, Genetics and Molecular Biology, Mice, Mutation, Spike Glycoprotein, Coronavirus, Animals, Humans, Aged, Immune Evasion

Abstract

Due to differences in human and murine angiotensin converting enzyme 2 (ACE-2) receptor, initially available SARS-CoV-2 isolates could not infect mice. Here we show that serial passaging of USA-WA1/2020 strain in mouse lungs results in “mouse-adapted” SARS-CoV-2 (MA-SARS-CoV-2) with mutations in S, M, and N genes, and a twelve-nucleotide insertion in the S gene. MA-SARS-CoV-2 infection causes mild disease, with more pronounced morbidity depending on genetic background and in aged and obese mice. Two mutations in the S gene associated with mouse adaptation (N501Y, H655Y) are present in SARS-CoV-2 variants of concern (VoCs). N501Y in the receptor binding domain of viruses of the B.1.1.7, B.1.351, P.1 and B.1.1.529 lineages (Alpha, Beta, Gamma and Omicron variants) is associated with high transmissibility and allows VoCs to infect wild type mice. We further show that S protein mutations of MA-SARS-CoV-2 do not affect neutralization efficiency by human convalescent and post vaccination sera.

Published

2022

3. Plitidepsin has potent preclinical efficacy against SARS-CoV-2 by targeting the host protein eEF1A

Author

Marion Dejosez, Carles Martínez-Romero, Melissa B. Uccellini, Ajda Rojc, Sonia Jangra, Lynda Coughlan, Michael Schotsaert, Raveen Rathnasinghe, Romel Rosales, Thomas P. Zwaka, Adolfo García-Sastre, Kevan M. Shokat, Kirsten Obernier, Mehdi Bouhaddou, Soner Yildiz, Kris M. White, Marco Vignuzzi, Lisa Miorin, Jyoti Batra, Nevan J. Krogan, Maria Jose Guillen, Jacqueline M. Fabius, Alejandro Losada, Pablo Aviles, Thomas Kehrer, and Elena Moreno

Subjects

viruses, Drug Evaluation, Preclinical, Pharmacology, Inbred C57BL, Virus Replication, Mice, 0302 clinical medicine, Peptide Elongation Factor 1, Depsipeptides, Viral, Lung, Research Articles, media_common, 0303 health sciences, Cyclic, Multidisciplinary, Alanine, Translation (biology), Preclinical, 3. Good health, Infectious Diseases, 5.1 Pharmaceuticals, 030220 oncology & carcinogenesis, Host-Pathogen Interactions, Pneumonia & Influenza, Medicine, RNA, Viral, Female, Development of treatments and therapeutic interventions, Infection, Research Article, Biotechnology, Drug, General Science & Technology, media_common.quotation_subject, Biology, Peptides, Cyclic, Antiviral Agents, Vaccine Related, 03 medical and health sciences, Eukaryotic translation, Rare Diseases, In vivo, Virology, Biodefense, Animals, Humans, Coronavirus Nucleocapsid Proteins, 030304 developmental biology, 5.2 Cellular and gene therapies, SARS-CoV-2, R-Articles, Prevention, HEK 293 cells, COVID-19, Pneumonia, Phosphoproteins, In vitro, Adenosine Monophosphate, COVID-19 Drug Treatment, Elongation factor, Mice, Inbred C57BL, HEK293 Cells, Orphan Drug, Emerging Infectious Diseases, Good Health and Well Being, Viral replication, Mutation, RNA, Drug Evaluation, Peptides

Abstract

Hurting the virus by targeting the host Many host proteins play a role in the life cycle of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), and some are required for viral replication and translation. There are efforts toward finding drugs that target viral proteins, but a complementary approach is to target these required host proteins. White et al. explored the antiviral activity of the cyclic depsipeptide drug plitidepsin, which targets the hosts cell's translational machinery (see the Perspective by Wong and Damania). The authors show that in cells, the drug is substantially more potent than remdesivir against SARS-CoV-2, with limited cellular toxicity. Prophylactic treatment protected mice against SARS-CoV-2 infection, so further investigation of plitidepsin as a therapeutic is warranted. Science, this issue p. 926; see also p. 884, Plitidepsin is a host-targeted antiviral against SARS-CoV-2, with potent efficacy both in vitro and in mouse models., Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) viral proteins interact with the eukaryotic translation machinery, and inhibitors of translation have potent antiviral effects. We found that the drug plitidepsin (aplidin), which has limited clinical approval, possesses antiviral activity (90% inhibitory concentration = 0.88 nM) that is more potent than remdesivir against SARS-CoV-2 in vitro by a factor of 27.5, with limited toxicity in cell culture. Through the use of a drug-resistant mutant, we show that the antiviral activity of plitidepsin against SARS-CoV-2 is mediated through inhibition of the known target eEF1A (eukaryotic translation elongation factor 1A). We demonstrate the in vivo efficacy of plitidepsin treatment in two mouse models of SARS-CoV-2 infection with a reduction of viral replication in the lungs by two orders of magnitude using prophylactic treatment. Our results indicate that plitidepsin is a promising therapeutic candidate for COVID-19.

Published

2021

4. The N501Y mutation in SARS-CoV-2 spike leads to morbidity in obese and aged mice and is neutralized by convalescent and post-vaccination human sera

Author

Viviana Simon, Florian Krammer, Lubbertus C. F. Mulder, Michael Schotsaert, Sadaf Aslam, Velmurugan Balaraman, Jana De Vrieze, Thomas Kehrer, Chester McDowell, Daniel Stadlbauer, Sonia Jangra, David A. Meekins, Bruno G. De Geest, Juergen A. Richt, Adolfo García-Sastre, Ignacio Mena, Carles Martínez-Romero, Angela Choi, Anastasija Cupic, Soner Yildiz, Lisa Miorin, and Raveen Rathnasinghe

Subjects

obesity, Mutation, mouse adaptation, diabetes, SARS-CoV-2, business.industry, Transmission (medicine), mouse model, viruses, Type 2 Diabetes Mellitus, Disease, medicine.disease_cause, medicine.disease, Virology, Article, Virus, B1.1.7 lineage, Diabetes mellitus, Angiotensin-converting enzyme 2, Medicine, aged mice, N501Y, business, Coronavirus

Abstract

The current COVID-19 (coronavirus disease 19) pandemic, caused by SARS-CoV-2, disproportionally affects the elderly and people with comorbidities like obesity and associated type 2 diabetes mellitus. Small animal models are crucial for the successful development and validation of antiviral vaccines, therapies and to study the role that comorbidities have on the outcome of viral infections. The initially available SARS-CoV-2 isolates require adaptation in order to use the mouse angiotensin converting enzyme 2 (mACE-2) entry receptor and to productively infect the cells of the murine respiratory tract. We have “mouse-adapted” SARS-CoV-2 by serial passaging a clinical virus isolate in the lungs of mice. We then used low doses of this virus in mouse models for advanced age, diabetes and obesity. Similar to SARS-CoV-2 infection in humans, the outcome of infection with mouse-adapted SARS-CoV-2 resulted in enhanced morbidity in aged and diabetic obese mice. Mutations associated with mouse adaptation occurred in the S, M, N and ORF8 genes. Interestingly, one mutation in the receptor binding domain of the S protein results in the change of an asparagine to tyrosine residue at position 501 (N501Y). This mutation is also present in the newly emerging SARS-CoV-2 variant viruses reported in the U.K. (20B/501Y.V1, B1.1.7 lineage) that is epidemiologically associated with high human to human transmission. We show that human convalescent and post vaccination sera can neutralize the newly emerging N501Y virus variant with similar efficiency as that of the reference USA-WA1/2020 virus, suggesting that current SARS-CoV-2 vaccines will protect against the 20B/501Y.V1 strain.

Published

2021

5. Virus-induced senescence is a driver and therapeutic target in COVID-19

Author

Markus Landthaler, Bernd Lamprecht, Riad Ghanem, Amjad Khan, Michael Mülleder, Maurice Reimann, Herta Steinkellner, Soyoung Lee, Emanuel Wyler, Mario Mairhofer, Wolfram Hoetzenecker, Paulina Richter-Pechanska, Séverine Kunz, Josef Tomasits, Rupert Langer, Kristina Dietert, Michael Schotsaert, Maria Pammer, Carles Martínez-Romero, Susanne Kimeswenger, Theresa C. Firsching, Jakob Trimpert, Melissa Uccellini, Achim D. Gruber, Bettina Purfürst, Adolfo García-Sastre, Clemens A. Schmitt, Reinhard Motz, Nikolaus Osterrieder, Anna Habringer, Markus Ralser, Julia Adler, Fahad Benthani, Martin Schönlein, Andrea Lau, Daniela Niemeyer, Christian Drosten, Dimitri Belenki, Dorothy N. Y. Fan, Roland Eils, Francesco Di Pierro, Lea Kausche, Gagandeep Singh, Christian Paar, Edward Georg Michaelis, Helmut J. F. Salzer, Yong Yu, and Sabine Kaltenbrunner

Subjects

Senescence, Male, medicine.medical_treatment, Dasatinib, Inflammation, Biology, Cell Line, Mice, Immune system, Cricetinae, medicine, Macrophage, Animals, Humans, Molecular Targeted Therapy, Senolytic, Cellular Senescence, Sulfonamides, Multidisciplinary, Aniline Compounds, SARS-CoV-2, fungi, COVID-19, Thrombosis, Neutrophil extracellular traps, COVID-19 Drug Treatment, Disease Models, Animal, Cytokine, Apoptosis, Cancer research, Female, Quercetin, medicine.symptom

Abstract

Derailed cytokine and immune cell networks account for the organ damage and the clinical severity of COVID-19 (refs. 1–4). Here we show that SARS-CoV-2, like other viruses, evokes cellular senescence as a primary stress response in infected cells. Virus-induced senescence (VIS) is indistinguishable from other forms of cellular senescence and is accompanied by a senescence-associated secretory phenotype (SASP), which comprises pro-inflammatory cytokines, extracellular-matrix-active factors and pro-coagulatory mediators5–7. Patients with COVID-19 displayed markers of senescence in their airway mucosa in situ and increased serum levels of SASP factors. In vitro assays demonstrated macrophage activation with SASP-reminiscent secretion, complement lysis and SASP-amplifying secondary senescence of endothelial cells, which mirrored hallmark features of COVID-19 such as macrophage and neutrophil infiltration, endothelial damage and widespread thrombosis in affected lung tissue1,8,9. Moreover, supernatant from VIS cells, including SARS-CoV-2-induced senescence, induced neutrophil extracellular trap formation and activation of platelets and the clotting cascade. Senolytics such as navitoclax and a combination of dasatinib plus quercetin selectively eliminated VIS cells, mitigated COVID-19-reminiscent lung disease and reduced inflammation in SARS-CoV-2-infected hamsters and mice. Our findings mark VIS as a pathogenic trigger of COVID-19-related cytokine escalation and organ damage, and suggest that senolytic targeting of virus-infected cells is a treatment option against SARS-CoV-2 and perhaps other viral infections. Virus-induced senescence is a central pathogenic feature in COVID-19, and senolytics, which promote apoptosis of senescent cells, can reduce disease severity in hamsters,mice, as well as humans infected with SARS-CoV-2.

Published

2021

6. Hybrid Gene Origination Creates Human-Virus Chimeric Proteins during Infection

Author

Jiajie Wei, Paul Digard, Robert J. Gifford, Nerea Irigoyen, Megan K. L. MacLeod, Alessandro Vannini, James P. Gibbs, Laura Campisi, Brad R. Rosenberg, Joshua D. Jones, Max W. Chang, Cheng Huang, Quan Gu, Edward C. Hutchinson, Veronica V. Rezelj, Christopher Benner, Helen M. Wise, Jessica Sook Yuin Ho, Jeffrey R. Johnson, Guojun Wang, Matthew Angel, Yesai Fstkchyan, Slobodan Paessler, Robyn M. Kaake, Nan Zhao, Maria João Amorim, Marta Alenquer, Elizabeth Sloan, Sara Clohisey, Ingeborg van Knippenberg, Harm van Bakel, Simin Zheng, Nevan J. Krogan, Liliane Chung, Adam M. Dinan, Bo Wang, Benjamin Greenbaum, Léa Meyer, Natasha Moshkina, Ian Brierley, Zeyu Zhu, Zuleyma Peralta, Adolfo García-Sastre, Andrew E. Firth, Marta Łuksza, Emily R. Miraldi, Vladimir Roudko, Ivan Marazzi, Rong Shen, Carles Martínez-Romero, Yixuan Ma, Jonathan W. Yewdell, J Kenneth Baillie, Justine Noel, Dinan, Adam [0000-0003-2812-1616], Irigoyen, Nerea [0000-0001-6346-3369], Brierley, Ian [0000-0003-3965-4370], Firth, Andrew [0000-0002-7986-9520], and Apollo - University of Cambridge Repository

Subjects

Transcription, Genetic, viruses, Mutant Chimeric Proteins, medicine.disease_cause, Virus Replication, gene origination, segmented negative-strand RNA viruses, viral evolution, Mice, 0302 clinical medicine, RNA Virus Infections, Cricetinae, RNA hybrid, Genetics, 0303 health sciences, 3. Good health, Influenza A virus, Viral evolution, RNA, Viral, influenza, RNA Caps, Recombinant Fusion Proteins, Biology, General Biochemistry, Genetics and Molecular Biology, Cap snatching, Cell Line, 03 medical and health sciences, Open Reading Frames, Viral Proteins, Dogs, chimeric proteins, Plant virus, upstream AUG, medicine, uORFs, Animals, Humans, RNA Viruses, RNA, Messenger, Gene, 030304 developmental biology, RNA, cap-snatching, RNA-Dependent RNA Polymerase, Fusion protein, viral RNA, Lassa virus, Cattle, Human Virus, 5' Untranslated Regions, 030217 neurology & neurosurgery

Abstract

RNA viruses are a major human health threat. The life cycles of many highly pathogenic RNA viruses like influenza A virus (IAV) and Lassa virus depends on host mRNA, as viral polymerases cleave 5’-m7G-capped host transcripts to primeviral mRNA synthesis (‘cap-snatching’). We hypothesized that start codons within cap-snatched host transcripts could generate chimeric human-viral mRNAs with coding potential. We report the existence of this mechanism of gene origination, that we named ‘start-snatching’. Depending on the reading frame, start-snatching allows the translation of host and viral “untranslated regions” (UTRs) to create Nterminallyextended viral proteins or entirely novel polypeptides by geneticoverprinting. We show that both types of chimeric proteins are made in IAVinfectedcells, generate T cell responses and contribute to virulence. Our resultsindicate that during infection with IAV, and likely a multitude of other human-,animal- and plant-viruses, a host-dependent mechanism allows the genesis ofhybrid genes.

Published

2020

7. Synergistic drug combination effectively blocks Ebola virus infection

Author

Paul Shinn, Wei Sun, Miao Xu, Xiangguo Qiu, Gregory J. Tawa, Carles Martínez-Romero, Shu Yang, Ethan G. Fisher, Philip E. Sanderson, Omid Motabar, Yan Long, Wei Zheng, Shihua He, Jennifer Kouznetsova, Peter R. Williamson, and Adolfo García-Sastre

Subjects

0301 basic medicine, Drug, media_common.quotation_subject, 030106 microbiology, Pharmacology, medicine.disease_cause, Antiviral Agents, Article, Cell Line, 03 medical and health sciences, Clarithromycin, Virology, Chlorocebus aethiops, medicine, Animals, Humans, Vero Cells, media_common, Ebolavirus, Ebola virus, Mefloquine, business.industry, Drug Synergism, Hemorrhagic Fever, Ebola, Triazoles, Virus Internalization, High-Throughput Screening Assays, Drug Combinations, Drug repositioning, Sphingomyelin Phosphodiesterase, 030104 developmental biology, Vero cell, Toremifene, Acid sphingomyelinase, NPC1, business, medicine.drug

Abstract

Although a group of FDA-approved drugs were previously identified with activity against Ebola virus (EBOV), most of them are not clinically useful because their human blood concentrations are not high enough to inhibit EBOV infection. We screened 795 unique three-drug combinations in an EBOV entry assay. Two sets of three-drug combinations, toremifene-mefloquine-posaconazole and toremifene-clarithromycin-posaconazole, were identified that effectively blocked EBOV entry and were further validated for inhibition of live EBOV infection. The individual drug concentrations in the combinations were reduced to clinically relevant levels. We identified mechanisms of action of these drugs: functional inhibitions of Niemann-Pick C1, acid sphingomyelinase, and lysosomal calcium release. Our findings identify the drug combinations with potential to treat EBOV infection.

Published

2017

8. Unanchored K48-Linked Polyubiquitin Synthesized by the E3-Ubiquitin Ligase TRIM6 Stimulates the Interferon-IKKε Kinase-Mediated Antiviral Response

Author

Sonja Schmid, Juliet Morrison, Giuseppe Pisanelli, David A. Stein, Ana M. Maestre, Gijs A. Versteeg, Ana Fernandez-Sesma, Maudry Laurent-Rolle, Hong M. Moulton, Ricardo Rajsbaum, Benjamin R. tenOever, Adolfo García-Sastre, Alan Belicha-Villanueva, Carles Martínez-Romero, Jenish R. Patel, Lisa Miorin, Ricardo, Rajsbaum, GIJS A., Versteeg, Sonja, Schmid, ANA M., Maestre, ALAN BELICHA, Villanueva, CARLES MARTÍNEZ, Romero, JENISH R., Patel, Juliet, Morrison, Pisanelli, Giuseppe, Lisa, Miorin, MAUDRY LAURENT, Rolle, HONG M., Moulton, DAVID A., Stein, ANA FERNANDEZ, Sesma, BENJAMIN R., Tenoever, and ADOLFO GARCÍA, S. A. S. T. R. E.

Subjects

IκB kinase, environment and public health, Tripartite Motif Proteins, Mice, Interferon, Immunology and Allergy, STAT1, Phosphorylation, RNA, Small Interfering, Polyubiquitin, Cells, Cultured, chemistry.chemical_classification, TRIM6 and the E2 conjugase UbE2K synthesize unanchored K48-linked ubiquitin chain, Cultured, Janus kinase 1, Kinase, I-kappa B Kinase, 3. Good health, Ubiquitin ligase, STAT1 Transcription Factor, Infectious Diseases, Interferon Type I, TRIM6 plays a critical role in innate immune activation, RNA Interference, Unanchored K48-linked ubiquitin chains activate the IKKε kinase, Signal Transduction, medicine.drug, Cells, 1.1 Normal biological development and functioning, Ubiquitin-Protein Ligases, Immunology, Biology, Small Interfering, Antiviral Agents, Article, Underpinning research, TRIM6 couples IFNαR engagement to activation of the IKKε kinase for ISG induction, Genetics, medicine, Animals, Humans, DNA ligase, Janus Kinase 1, Molecular biology, Enzyme Activation, enzymes and coenzymes (carbohydrates), chemistry, Ubiquitin-Conjugating Enzymes, biology.protein, RNA

Abstract

SummaryType I interferons (IFN-I) are essential antiviral cytokines produced upon microbial infection. IFN-I elicits this activity through the upregulation of hundreds of IFN-I-stimulated genes (ISGs). The full breadth of ISG induction demands activation of a number of cellular factors including the IκB kinase epsilon (IKKε). However, the mechanism of IKKε activation upon IFN receptor signaling has remained elusive. Here we show that TRIM6, a member of the E3-ubiquitin ligase tripartite motif (TRIM) family of proteins, interacted with IKKε and promoted induction of IKKε-dependent ISGs. TRIM6 and the E2-ubiquitin conjugase UbE2K cooperated in the synthesis of unanchored K48-linked polyubiquitin chains, which activated IKKε for subsequent STAT1 phosphorylation. Our work attributes a previously unrecognized activating role of K48-linked unanchored polyubiquitin chains in kinase activation and identifies the UbE2K-TRIM6-ubiquitin axis as critical for IFN signaling and antiviral response.

Published

2014

9. Induction and Evasion of Type-I Interferon Responses during Influenza A Virus Infection

Author

Raquel Muñoz-Moreno, Carles Martínez-Romero, and Adolfo García-Sastre

Subjects

0301 basic medicine, Innate immune system, Respiratory tract infections, 010405 organic chemistry, Biology, Evasion (ethics), medicine.disease_cause, 01 natural sciences, Virology, General Biochemistry, Genetics and Molecular Biology, 0104 chemical sciences, 03 medical and health sciences, 030104 developmental biology, Immune system, Viral replication, Influenza A virus, Interferon, Influenza, Human, Interferon Type I, medicine, Humans, Secretion, Immune Evasion, medicine.drug

Abstract

Influenza A viruses (IAVs) are contagious pathogens and one of the leading causes of respiratory tract infections in both humans and animals worldwide. Upon infection, the innate immune system provides the first line of defense to neutralize or limit the replication of invading pathogens, creating a fast and broad response that brings the cells into an alerted state through the secretion of cytokines and the induction of the interferon (IFN) pathway. At the same time, IAVs have developed a plethora of immune evasion mechanisms in order to avoid or circumvent the host antiviral response, promoting viral replication. Herein, we will review and summarize already known and recently described innate immune mechanisms that host cells use to fight IAV viral infections as well as the main strategies developed by IAVs to overcome such powerful defenses during this fascinating virus-host interplay.

Published

2020

10. Viral Fitness Landscapes in Diverse Host Species Reveal Multiple Evolutionary Lines for the NS1 Gene of Influenza A Viruses

Author

Raffael Nachbagauer, Daniel Blanco-Melo, Raquel Muñoz-Moreno, Florian Krammer, David H. Sachs, Benjamin R. tenOever, Ilseob Lee, Maryline Panis, Vinod Balasubramaniam, Ignacio Mena, Sadaf Aslam, Man Seong Park, Carles Martínez-Romero, Christian V. Forst, Asiel Arturo Benitez, Juan Ayllon, and Adolfo García-Sastre

Subjects

0301 basic medicine, Viral protein, viruses, Evolutionary landscape, Host tropism, Viral Nonstructural Proteins, Biology, Virus Replication, medicine.disease_cause, Host Specificity, Article, General Biochemistry, Genetics and Molecular Biology, Madin Darby Canine Kidney Cells, Mice, 03 medical and health sciences, Dogs, 0302 clinical medicine, Orthomyxoviridae Infections, Interferon, medicine, Animals, lcsh:QH301-705.5, Gene, Phylogeny, Tropism, 030304 developmental biology, Genetics, 0303 health sciences, Phylogenetic tree, 030306 microbiology, Host (biology), virus diseases, Phenotype, Immunity, Innate, 3. Good health, 030104 developmental biology, lcsh:Biology (General), Influenza A virus, Evolutionary biology, Host-Pathogen Interactions, Mutation, Female, 030217 neurology & neurosurgery, medicine.drug

Abstract

SUMMARY Influenza A viruses (IAVs) have a remarkable tropism in their ability to circulate in both mammalian and avian species. The IAV NS1 protein is a multifunctional virulence factor that inhibits the type I interferon host response through a myriad of mechanisms. How NS1 has evolved to enable this remarkable property across species and its specific impact in the overall replication, pathogenicity, and host preference remain unknown. Here we analyze the NS1 evolutionary landscape and host tropism using a barcoded library of recombinant IAVs. Results show a surprisingly great variety of NS1 phenotypes according to their ability to replicate in different hosts. The IAV NS1 genes appear to have taken diverse and random evolutionary pathways within their multiple phylogenetic lineages. In summary, the high evolutionary plasticity of this viral protein underscores the ability of IAVs to adapt to multiple hosts and aids in our understanding of its global prevalence., Graphical Abstract, In Brief Muñoz-Moreno et al. report that influenza A virus NS1 undergoes diverse and unpredictable evolutionary pathways based on its different phylogenetic lineages. A high-throughput approach using a barcoded library is used to test the interactions between NS1-recombinant viruses and to study their preference for specific or multiple hosts.

Published

2019

11. Emetine inhibits Zika and Ebola virus infections through two molecular mechanisms: inhibiting viral replication and decreasing viral entry

Author

Sergey A. Shiryaev, Hengli Tang, Dushyantha Jayaweera, Ruili Huang, Xiangguo Qiu, Yi Zhou, Yu-Shan Cheng, Zirui Zhang, Hongjun Song, Richard A. Preston, Wei Zheng, Emily M. Lee, Chun-Teng Huang, Adolfo García-Sastre, Anton Simeonov, Khalida Shamim, Shihua He, Xin Hu, Miao Xu, Menghang Xia, Shu Yang, Wenwei Huang, Alexey V. Terskikh, Yuying Wu, Guo Li Ming, Wenjun Zhu, Kirill Gorshkov, Carles Martínez-Romero, Wei Sun, Heng Zhu, Billy Lu, Guang Song, Antonella Pinto, Anil Mathew Tharappel, and Chen Farhy

Subjects

0301 basic medicine, Emetine, medicine.disease_cause, Biochemistry, Article, Zika virus, 03 medical and health sciences, chemistry.chemical_compound, Viral entry, Genetics, medicine, lcsh:QH573-671, Molecular Biology, IC50, Polymerase, Ebola virus, biology, lcsh:Cytology, business.industry, Cell Biology, biology.organism_classification, Virology, 3. Good health, 030104 developmental biology, chemistry, Viral replication, biology.protein, Cephaeline, business, medicine.drug

Abstract

The re-emergence of Zika virus (ZIKV) and Ebola virus (EBOV) poses serious and continued threats to the global public health. Effective therapeutics for these maladies is an unmet need. Here, we show that emetine, an anti-protozoal agent, potently inhibits ZIKV and EBOV infection with a low nanomolar half maximal inhibitory concentration (IC50) in vitro and potent activity in vivo. Two mechanisms of action for emetine are identified: the inhibition of ZIKV NS5 polymerase activity and disruption of lysosomal function. Emetine also inhibits EBOV entry. Cephaeline, a desmethyl analog of emetine, which may be better tolerated in patients than emetine, exhibits a similar efficacy against both ZIKV and EBOV infections. Hence, emetine and cephaeline offer pharmaceutical therapies against both ZIKV and EBOV infection.

Published

2018

12. Specific Mutations in the PB2 Protein of Influenza A Virus Compensate for the Lack of Efficient Interferon Antagonism of the NS1 Protein of Bat Influenza A-Like Viruses

Author

Amzie Pavlisin, Andres Moreira-Soto, Juan Ayllon, Shashank Tripathi, Martin Schwemmle, Eugenia Corrales-Aguilar, Carles Martínez-Romero, Ignacio Mena, Teresa Aydillo, Adolfo García-Sastre, and Amanda Vicente-Santos

Subjects

0301 basic medicine, viruses, Immunology, Virulence, Hemagglutinin (influenza), Viral Nonstructural Proteins, medicine.disease_cause, Microbiology, NS1 protein, Virus, law.invention, Viral Proteins, 03 medical and health sciences, Interferon, law, Virology, medicine, Influenza A virus, Influenza viruses, Humans, Gene, 599.472 867 Chiroptera (Quirópteros, Murciélagos), 030102 biochemistry & molecular biology, biology, Bat, virus diseases, HEK293 Cells, 030104 developmental biology, A549 Cells, Insect Science, Mutation, biology.protein, Recombinant DNA, Pathogenesis and Immunity, Interferons, Neuraminidase, medicine.drug

Abstract

Recently, two new influenza A-like viruses have been discovered in bats, A/little yellow-shouldered bat/Guatemala/060/2010 (HL17NL10) and A/flat-faced bat/Peru/033/2010 (HL18NL11). The hemagglutinin (HA)-like (HL) and neuraminidase (NA)-like (NL) proteins of these viruses lack hemagglutination and neuraminidase activities, despite their sequence and structural homologies with the HA and NA proteins of conventional influenza A viruses. We have now investigated whether the NS1 proteins of the HL17NL10 and HL18NL11 viruses can functionally replace the NS1 protein of a conventional influenza A virus. For this purpose, we generated recombinant influenza A/Puerto Rico/8/1934 (PR8) H1N1 viruses containing the NS1 protein of the PR8 wild-type, HL17NL10, and HL18NL11 viruses. These viruses (r/NS1PR8, r/NS1HL17, and r/NS1HL18, respectively) were tested for replication in bat and nonbat mammalian cells and in mice. Our results demonstrate that the r/NS1HL17 and r/NS1HL18 viruses are attenuated in vitro and in vivo . However, the bat NS1 recombinant viruses showed a phenotype similar to that of the r/NS1PR8 virus in STAT1 −/− human A549 cells and mice, both in vitro and in vivo systems being unable to respond to interferon (IFN). Interestingly, multiple mouse passages of the r/NS1HL17 and r/NS1HL18 viruses resulted in selection of mutant viruses containing single amino acid mutations in the viral PB2 protein. In contrast to the parental viruses, virulence and IFN antagonism were restored in the selected PB2 mutants. Our results indicate that the NS1 protein of bat influenza A-like viruses is less efficient than the NS1 protein of its conventional influenza A virus NS1 counterpart in antagonizing the IFN response and that this deficiency can be overcome by the influenza virus PB2 protein. IMPORTANCE Significant gaps in our understanding of the basic features of the recently discovered bat influenza A-like viruses HL17NL10 and HL18NL11 remain. The basic biology of these unique viruses displays both similarities to and differences from the basic biology of conventional influenza A viruses. Here, we show that recombinant influenza A viruses containing the NS1 protein from HL17NL10 and HL18NL11 are attenuated. This attenuation was mediated by their inability to antagonize the type I IFN response. However, this deficiency could be compensated for by single amino acid replacements in the PB2 gene. Our results unravel a functional divergence between the NS1 proteins of bat influenza A-like and conventional influenza A viruses and demonstrate an interplay between the viral PB2 and NS1 proteins to antagonize IFN.

Published

2018

13. Against the clock towards new Ebola virus therapies

Author

Carles Martínez-Romero and Adolfo García-Sastre

Subjects

Cancer Research, medicine.medical_specialty, Disease, Biology, medicine.disease_cause, Antiviral Agents, Disease Outbreaks, West africa, Virology, Drug Discovery, Health care, Disease Transmission, Infectious, medicine, Humans, Ebola Vaccines, Intensive care medicine, Ebolavirus, Clinical Trials as Topic, Ebola virus, Ebola vaccine, business.industry, Drug Repositioning, Outbreak, Hemorrhagic Fever, Ebola, Africa, Western, Infectious Diseases, business

Abstract

Since the end of 2013, West Africa has been suffering the largest Ebola virus (EBOV) outbreak in recorded history. The lack of health care infrastructure in the affected countries, as well as a concentration of infected cases in the most populated areas allowed the virus to spread with no control during the first months of the outbreak. With no specific treatment available to combat EBOV infection and its associated disease, an extraordinary worldwide effort was made to confront the severity of the situation and to establish new therapeutic strategies that would lead to better and faster control and eradicate the outbreak. In the last two years, several candidate therapies and potential vaccines against EBOV have arisen and human clinical trials are ongoing, in hopes of starting their deployment in the affected countries. This article reviews the current candidate therapies against EBOV, their stage of development and future prospects in battling EBOV outbreaks.

Published

2015

14. ISG15 Is Counteracted by Vaccinia Virus E3 Protein and Controls the Proinflammatory Response against Viral Infection

Author

Benedito Eduardo-Correia, Susana Guerra, Carles Martínez-Romero, Adolfo García-Sastre, and UAM. Departamento de Medicina Preventiva y Salud Pública y Microbiología

Subjects

Medicina, Protein, viruses, Immunology, Vaccinia Virus, Biology, Microbiology, Viral infection, ISG15, Virology, Virus, Proinflammatory cytokine, chemistry.chemical_compound, chemistry, Insect Science, Christian ministry, Vaccinia

Abstract

Conjugation of ISG15 inhibits replication of several viruses. Here, using an expression system for assaying human and mouse ISG15 conjugations (ISGylations), we have demonstrated that vaccinia virus E3 protein binds and antagonizes human and mouse ISG15 modification. To study ISGylation importance in poxvirus infection, we used a mouse model that expresses deconjugating proteases. Our results indicate that ISGylation restricts in vitro replication of the vaccinia virus VV E3L mutant but unconjugated ISG15 is crucial to counteract the inflammatory response produced after VV E3L infection, This work was supported by grants from the Spanish Ministry of Health, FIS2011-00127, and UAM-Banco de Santander to S.G. and was also partly supported by NIAID grant U19AI083025 to A.G.-S

Published

2014

15. The Polycomb group protein RING1B is overexpressed in ductal breast carcinoma and is required to sustain FAK steady state levels in breast cancer epithelial cells

Author

Saleta Morales, Carles Martínez-Romero, Eduardo F. Farias, Xavier Mayol, Juan Martín-Caballero, Ramon Gimeno, Tania Lobato, Josep M. Corominas, Almudena Bosch, Gema Moreno-Bueno, Konstantina Panoutsopoulou, Amparo Cano, Inmaculada Hernández-Muñoz, Ministerio de Ciencia e Innovación (España), European Commission, Instituto de Salud Carlos III, and Generalitat de Catalunya

Subjects

Chromatin Immunoprecipitation, Blotting, Western, Fluorescent Antibody Technique, Mice, Nude, Breast Neoplasms, ComputingMilieux_LEGALASPECTSOFCOMPUTING, Biology, Metastasis, Mice, Breast cancer, medicine, Carcinoma, ductal breast carcinoma, Animals, Humans, Neoplasm Invasiveness, Sensory disorders Radboud Institute for Molecular Life Sciences [Radboudumc 12], Cells, Cultured, Polycomb Repressive Complex 1, Regulation of gene expression, p63, Fak, Reverse Transcriptase Polymerase Chain Reaction, Carcinoma, Ductal, Breast, Membrane Proteins, Epithelial Cells, Cell migration, medicine.disease, Immunohistochemistry, Primary tumor, Molecular biology, Gene Expression Regulation, Neoplastic, Ductal Breast Carcinoma, Oncology, Tissue Array Analysis, Ring1B, Focal Adhesion Kinase 1, Cancer research, Heterografts, Female, mammary epithelial cell, Breast carcinoma, Research Paper

Abstract

This is an open-access article distributed under the terms of the Creative Commons Attribution License,.-- et al., In early stages of metastasis malignant cells must acquire phenotypic changes to enhance their migratory behavior and their ability to breach the matrix surrounding tumors and blood vessel walls. Epigenetic regulation of gene expression allows the acquisition of these features that, once tumoral cells have escape from the primary tumor, can be reverted. Here we report that the expression of the Polycomb epigenetic repressor Ring1B is enhanced in tumoral cells that invade the stroma in human ductal breast carcinoma and its expression is coincident with that of Fak in these tumors. Ring1B knockdown in breast cancer cell lines revealed that Ring1B is required to sustain Fak expression in basal conditions as well as in Tgfβ-treated cells. Functionally, endogenous Ring1B is required for cell migration and invasion in vitro and for in vivo invasion of the mammary fat pad by tumoral cells. Finally we identify p63 as a target of Ring1B to regulate Fak expression: Ring1B depletion results in enhanced p63 expression, which in turns represses Fak expression. Importantly, Fak downregulation upon Ring1B depletion is dependent on p63 expression. Our findings provide new insights in the biology of the breast carcinoma and open new avenues for breast cancer prognosis and therapy., This work was funded by grants from the Spanish Ministry of Science and Innovation/ Instituto de Salud Carlos III FEDER (PS09/00973) and from the AGAUR (2009 SGR 1409). IHM is an investigator at the Miguel Servet program (Instituto de Salud Carlos III).

Published

2014

16. Identification of 53 compounds that block Ebola virus-like particle entry via a repurposing screen of approved drugs

Author

Wei Sun, Jennifer Kouznetsova, Carles Martínez-Romero, Catherine Z. Chen, Philip E. Sanderson, Aaron D. Schimmer, John C. McKew, Adolfo García-Sastre, Wei Zheng, Paul Shinn, and Gregory J. Tawa

Subjects

Epidemiology, medicine.drug_class, drug repurposing screen, VP40, viruses, estrogen receptor modulator, Immunology, Antibiotics, virus entry, Pharmacology, medicine.disease_cause, Microbiology, Ebola virus, 03 medical and health sciences, Viral entry, Virology, Biosafety level, Drug Discovery, medicine, Antipsychotics, microtubule inhibitor, Repurposing, 030304 developmental biology, 0303 health sciences, 030306 microbiology, business.industry, virus diseases, General Medicine, 3. Good health, Drug repositioning, Infectious Diseases, Drug development, Ebola virus glycoprotein, Original Article, Parasitology, business

Abstract

In light of the current outbreak of Ebola virus disease, there is an urgent need to develop effective therapeutics to treat Ebola infection, and drug repurposing screening is a potentially rapid approach for identifying such therapeutics. We developed a biosafety level 2 (BSL-2) 1536-well plate assay to screen for entry inhibitors of Ebola virus-like particles (VLPs) containing the glycoprotein (GP) and the matrix VP40 protein fused to a beta-lactamase reporter protein and applied this assay for a rapid drug repurposing screen of Food and Drug Administration (FDA)-approved drugs. We report here the identification of 53 drugs with activity of blocking Ebola VLP entry into cells. These 53 active compounds can be divided into categories including microtubule inhibitors, estrogen receptor modulators, antihistamines, antipsychotics, pump/channel antagonists, and anticancer/antibiotics. Several of these compounds, including microtubule inhibitors and estrogen receptor modulators, had previously been reported to be active in BSL-4 infectious Ebola virus replication assays and in animal model studies. Our assay represents a robust, effective and rapid high-throughput screen for the identification of lead compounds in drug development for the treatment of Ebola virus infection.

Published

2014

17. Antiviral Role of IFITM Proteins in African Swine Fever Virus Infection

Author

Carles Martínez-Romero, Lucía Barrado-Gil, Raquel Muñoz-Moreno, Covadonga Alonso, Adolfo García-Sastre, Inmaculada Galindo, and Miguel Ángel Cuesta-Geijo

Subjects

0301 basic medicine, Cell Lines, viruses, Cell Membranes, lcsh:Medicine, Biochemistry, Membrane Fusion, Virions, Chlorocebus aethiops, Medicine and Health Sciences, lcsh:Science, Late endosome, Infectivity, Multidisciplinary, biology, African Swine Fever Virus, Lipids, Transmembrane protein, Endocytosis, 3. Good health, Cholesterol, Infectious Diseases, Biological Cultures, Cellular Structures and Organelles, Research Article, Infectious Disease Control, Endosome, Endosomes, Viral Structure, Research and Analysis Methods, African swine fever virus, Microbiology, Virus, 03 medical and health sciences, Viral entry, Virology, Animals, Humans, RNA Viruses, Vesicles, Vero Cells, RNA, Double-Stranded, 030102 biochemistry & molecular biology, Cell Membrane, lcsh:R, Membrane Proteins, Biology and Life Sciences, Proteins, Cell Biology, Virus Internalization, biology.organism_classification, Antigens, Differentiation, 030104 developmental biology, HEK293 Cells, Microscopy, Fluorescence, Vero cell, lcsh:Q, Interferons

Abstract

The interferon-induced transmembrane (IFITM) protein family is a group of antiviral restriction factors that impair flexibility and inhibit membrane fusion at the plasma or the endosomal membrane, restricting viral progression at entry. While IFITMs are widely known to inhibit several single-stranded RNA viruses, there are limited reports available regarding their effect in double-stranded DNA viruses. In this work, we have analyzed a possible antiviral function of IFITMs against a double stranded DNA virus, the African swine fever virus (ASFV). Infection with cell-adapted ASFV isolate Ba71V is IFN sensitive and it induces IFITMs expression. Interestingly, high levels of IFITMs caused a collapse of the endosomal pathway to the perinuclear area. Given that ASFV entry is strongly dependent on endocytosis, we investigated whether IFITM expression could impair viral infection. Expression of IFITM1, 2 and 3 reduced virus infectivity in Vero cells, with IFITM2 and IFITM3 having an impact on viral entry/uncoating. The role of IFITM2 in the inhibition of ASFV in Vero cells could be related to impaired endocytosis-mediated viral entry and alterations in the cholesterol efflux, suggesting that IFITM2 is acting at the late endosome, preventing the decapsidation stage of ASFV. Copyright © 2016 Muñoz-Moreno et al.

Published

2016

18. Characterization of HIV-1 entry inhibitors with broad activity against R5 and X4 viral strains

Author

Paolo Cozzi, Paolo Lusso, Mauro S. Malnati, Priscilla Biswas, Daniela Jabes, Francesca Sironi, Adolfo García-Sastre, Silvia Ghezzi, Christina Guzzo, Nicola Mongelli, and Carles Martínez-Romero

Subjects

Benzylamines, Receptors, CXCR4, Receptors, CCR5, medicine.drug_class, viruses, HIV Infections, HIV Envelope Protein gp120, Cyclams, Virus Replication, Bioinformatics, Monoclonal antibody, Antiviral Agents, Membrane Fusion, General Biochemistry, Genetics and Molecular Biology, Virus, Cell Line, Maraviroc, Mice, chemistry.chemical_compound, Viral envelope, Cyclohexanes, HIV Fusion Inhibitors, Heterocyclic Compounds, Viral entry, medicine, Animals, Humans, Medicine(all), Reporter gene, Cell Death, Biochemistry, Genetics and Molecular Biology(all), business.industry, Research, virus diseases, 3T3 Cells, General Medicine, Triazoles, Virus Internalization, Flow Cytometry, Virology, Mechanism of action, chemistry, Cell culture, HIV-1, medicine.symptom, business

Abstract

Background Combined antiretroviral therapy has drastically reduced mortality and morbidity of HIV-infected individuals. Nevertheless long-term toxicity and appearance of viral resistance hampers the prolonged effectiveness of combination therapy, requiring a continuous input of drugs to replace those utilized in combination regimens. We here investigated the anti-HIV activity of novel derivatives of the suradista chemical class. Methods Compounds were tested on acute HIV-1 infection of activated peripheral blood mononuclear cells. HIV production was monitored by enzyme-linked immunosorbent assay measuring the protein p24 released in culture supernatants. Fusion assays were carried out to study the mechanism of action of these compounds. A modified version of a previously established recombinant vaccinia virus-based assay was used measuring activation of a reporter gene upon fusion of two distinct cell populations. Flow cytometry was performed in competition assays for the binding of several antibodies targeting different sites of the viral envelope glycoprotein gp120, or the receptor CD4, or the coreceptors CXCR4 and CCR5. Results Four compounds inhibited replication of a prototypic R5 (BaL) and X4 (IIIB) laboratory-adapted HIV-1 strain at low micromolar concentrations, in the absence of cytotoxicity. Approximately a ten fold greater activity was achieved against the X4 as compared to the R5 strain. The compounds blocked X4 and R5 HIV-1 fusion, a step of viral entry. This activity appeared specific for HIV-1, as entry of human herpesvirus 6 (HHV-6) and influenza virus was not substantially affected. Further investigation of the inhibitory mechanism revealed that these new molecules target the viral envelope, rather than the coreceptors, as previously shown for a congener of the same class characterized by a long plasmatic half-life. Indeed ND-4043, the most active compound, specifically competed with binding of monoclonal antibodies against the CD4-binding site (CD4-BS) and coreceptor-binding site (CoR-BS) of gp120. These compounds displayed broad anti-HIV activity, as they inhibited various primary R5, X4 and, importantly, dualtropic R5X4 HIV-1 isolates. Of the four derivatives tested, the dimeric compounds were consistently more potent than the monomeric ones. Conclusions Given their unique features, these molecules represent promising candidates for further development and exploitation as anti-HIV therapeutics. Electronic supplementary material The online version of this article (doi:10.1186/s12967-015-0461-9) contains supplementary material, which is available to authorized users.

Published

2015

19. Mouse Dendritic Cell (DC) Influenza Virus Infectivity Is Much Lower than That for Human DCs and Is Hemagglutinin Subtype Dependent

Author

Thomas M. Moran, Sonali Patil, Jingjing Jia, Wenjing Li, Stuart C. Sealfon, Randy A. Albrecht, Carles Martínez-Romero, Nada Marjanovic, Boris M. Hartmann, James G. Wetmur, Fernand Hayot, and Adolfo García-Sastre

Subjects

viruses, Immunology, Hemagglutinin (influenza), chemical and pharmacologic phenomena, Hemagglutinin Glycoproteins, Influenza Virus, Microbiology, Virus, law.invention, Mice, Influenza A Virus, H1N1 Subtype, Viral entry, law, Virology, Animals, Humans, Cells, Cultured, Infectivity, biology, hemic and immune systems, Dendritic Cells, Virus Internalization, In vitro, Virus-Cell Interactions, Mouse Dendritic Cell, Insect Science, biology.protein, Recombinant DNA, Influenza A (H1N1) Virus Infection

Abstract

We show that influenza A H1N1 virus infection leads to very low infectivity in mouse dendritic cells (DCs) in vitro compared with that in human DCs. This holds when H3 or H5 replaces H1 in recombinant viruses. Viruslike particles confirm the difference between mouse and human, suggesting that reduced virus entry contributes to lower mouse DC infectivity. Low infectivity of mouse DCs should be considered when they are used to study responses of DCs that are actually infected.

Published

2013

20. The interferon signaling antagonist function of yellow fever virus NS5 protein is activated by type I interferon

Author

Carles Martínez-Romero, Alissa M. Pham, Adolfo García-Sastre, Benjamin R. tenOever, Giuseppe Pisanelli, Juliet Morrison, Juan Ayllon, Maudry Laurent-Rolle, Ricardo Rajsbaum, Lisa Miorin, Jesica M. Levingston Macleod, Laurent Rolle, Maudry, Morrison, Juliet, Rajsbaum, Ricardo, Macleod, Jesica M. Levingston, Pisanelli, Giuseppe, Pham, Alissa, Ayllon, Juan, Miorin, Lisa, Martínez Romero, Carle, Tenoever, Benjamin R, and García Sastre, Adolfo

Subjects

Cancer Research, viruses, Amino Acid Motifs, Viral Nonstructural Proteins, medicine.disease_cause, chemistry.chemical_compound, Interferon, STAT1, STAT2, Phosphorylation, virus diseases, Host-Pathogen Interaction, STAT1 Transcription Factor, Infectious Diseases, Medical Microbiology, Host-Pathogen Interactions, Amino Acid Motif, Signal transduction, Yellow fever virus, Infection, GTP-Binding Protein, Human, medicine.drug, Signal Transduction, Protein Binding, Viral protein, Immunology, Biology, Microbiology, Cell Line, Vaccine Related, GTP-Binding Proteins, Immunology and Microbiology(all), Virology, Biodefense, Yellow Fever, medicine, Animals, Humans, Molecular Biology, Transcription factor, Animal, Prevention, Viral Nonstructural Protein, Tyrosine phosphorylation, STAT2 Transcription Factor, Interferon-beta, Emerging Infectious Diseases, chemistry, biology.protein, Parasitology

Abstract

SummaryTo successfully establish infection, flaviviruses have to overcome the antiviral state induced by type I interferon (IFN-I). The nonstructural NS5 proteins of several flaviviruses antagonize IFN-I signaling. Here we show that yellow fever virus (YFV) inhibits IFN-I signaling through a unique mechanism that involves binding of YFV NS5 to the IFN-activated transcription factor STAT2 only in cells that have been stimulated with IFN-I. This NS5-STAT2 interaction requires IFN-I-induced tyrosine phosphorylation of STAT1 and the K63-linked polyubiquitination at a lysine in the N-terminal region of YFV NS5. We identified TRIM23 as the E3 ligase that interacts with and polyubiquitinates YFV NS5 to promote its binding to STAT2 and trigger IFN-I signaling inhibition. Our results demonstrate the importance of YFV NS5 in overcoming the antiviral action of IFN-I and offer a unique example of a viral protein that is activated by the same host pathway that it inhibits.

Published

2014

21. Correction for Eduardo-Correia et al., ISG15 Is Counteracted by Vaccinia Virus E3 Protein and Controls the Proinflammatory Response against Viral Infection

Author

Carles Martínez-Romero, Adolfo García-Sastre, Benedito Eduardo-Correia, and Susana Guerra

Subjects

viruses, Immunology, Cellular Response to Infection, Poxviridae Infections, Biology, Virus Replication, Microbiology, Viral infection, Virus, Proinflammatory cytokine, Mice, Viral Proteins, chemistry.chemical_compound, Virology, Animals, Humans, Ubiquitins, Mice, Knockout, Histological Techniques, Intracellular Signaling Peptides and Proteins, RNA-Binding Proteins, ISG15, Author Corrections, chemistry, Insect Science, Mutation, Cytokines, Vaccinia, Peptide Hydrolases

Abstract

Conjugation of ISG15 inhibits replication of several viruses. Here, using an expression system for assaying human and mouse ISG15 conjugations (ISGylations), we have demonstrated that vaccinia virus E3 protein binds and antagonizes human and mouse ISG15 modification. To study ISGylation importance in poxvirus infection, we used a mouse model that expresses deconjugating proteases. Our results indicate that ISGylation restricts in vitro replication of the vaccinia virus VVΔE3L mutant but unconjugated ISG15 is crucial to counteract the inflammatory response produced after VVΔE3L infection.

Published

2016

22. The role of unanchored polyubiquitin chains and the TRIM E3-ubiquitin ligase family of proteins in the innate immune response to influenza virus infection (INM3P.402)

Author

Ricardo Rajsbaum, Preeti Bharaj, Jane Ellis, Gijs Versteeg, Sonja Schmid, Ana Maestre, Alan Belicha-Villanueva, Jenish Patel, Juliet Morrison, Giuseppe Giuseppe Pisanelli, Lisa Miorin, Carles Martínez-Romero, Maudry Laurent-Rolle, Hong Moulton, David Stein, Ana Fernandez-Sesma, Benjamin tenOever, and Adolfo Garcia-Sastre

Subjects

Immunology, Immunology and Allergy

Abstract

Intracellular innate immune responses are essential to protect host cells against pathogens. Upon infection, pattern recognition receptors detect incoming microbes and trigger downstream signaling pathways leading to production of antiviral type-I interferons (IFNs).These signaling pathways are regulated by different posttranslational modifications including the ubiquitin (Ub) system. Proteins covalently attached to K48-linked polyUb are targeted for degradation by the proteasome, whereas protein modification with K63-linked polyUb may have non-proteolytic activating functions. Unanchored Ub chains that are not covalently attached to any protein are also important for kinase activation. Tripartite motif (TRIM) proteins, which function as E3-ubiquitin ligases, have been implicated in antiviral activity. We found that TRIM6 is important in the synthesis of unanchored K48-linked polyUb chains, which activate the IKKε kinase for STAT1 phosphorylation and induction of an antiviral response. These polyUb chains and IKKε interact in vivo in an IFN-I signaling dependent manner upon virus infection in mice. To better understand the physiological role of unanchored polyUb during virus infection, we developed a system to isolate ubiquitin-interacting proteins from the lungs of influenza-infected mice. Using a proteomics approach we identified new cellular factors that interact with unanchored polyUb chains in vivo and may be involved in the innate immune antiviral response.

Published

2015