Your search keyword '"Paul D. De Jesus"' showing total 25 results

1. MDA5 Governs the Innate Immune Response to SARS-CoV-2 in Lung Epithelial Cells

Author

Xin Yin, Laura Riva, Yuan Pu, Laura Martin-Sancho, Jun Kanamune, Yuki Yamamoto, Kouji Sakai, Shimpei Gotoh, Lisa Miorin, Paul D. De Jesus, Chih-Cheng Yang, Kristina M. Herbert, Sunnie Yoh, Judd F. Hultquist, Adolfo García-Sastre, and Sumit K. Chanda

Subjects

SARS-CoV-2, lung epithelial cells, interferon, MDA5, IRF3, IRF5, Biology (General), QH301-705.5

Abstract

Summary: Recent studies have profiled the innate immune signatures in patients infected with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) and suggest that cellular responses to viral challenge may affect disease severity. Yet the molecular events that underlie cellular recognition and response to SARS-CoV-2 infection remain to be elucidated. Here, we find that SARS-CoV-2 replication induces a delayed interferon (IFN) response in lung epithelial cells. By screening 16 putative sensors involved in sensing of RNA virus infection, we found that MDA5 and LGP2 primarily regulate IFN induction in response to SARS-CoV-2 infection. Further analyses revealed that viral intermediates specifically activate the IFN response through MDA5-mediated sensing. Additionally, we find that IRF3, IRF5, and NF-κB/p65 are the key transcription factors regulating the IFN response during SARS-CoV-2 infection. In summary, these findings provide critical insights into the molecular basis of the innate immune recognition and signaling response to SARS-CoV-2.

Published

2021

2. Large-Scale Arrayed Analysis of Protein Degradation Reveals Cellular Targets for HIV-1 Vpu

Author

Prashant Jain, Guney Boso, Simon Langer, Stephen Soonthornvacharin, Paul D. De Jesus, Quy Nguyen, Kevin C. Olivieri, Alex J. Portillo, Sunnie M. Yoh, Lars Pache, and Sumit K. Chanda

Subjects

Biology (General), QH301-705.5

Abstract

Summary: Accessory proteins of lentiviruses, such as HIV-1, target cellular restriction factors to enhance viral replication. Systematic analyses of proteins that are targeted for degradation by HIV-1 accessory proteins may provide a better understanding of viral immune evasion strategies. Here, we describe a high-throughput platform developed to study cellular protein stability in a highly parallelized matrix format. We used this approach to identify cellular targets of the HIV-1 accessory protein Vpu through arrayed coexpression with 433 interferon-stimulated genes, followed by differential fluorescent labeling and automated image analysis. Among the previously unreported Vpu targets identified by this approach, we find that the E2 ligase mediating ISG15 conjugation, UBE2L6, and the transmembrane protein PLP2 are targeted by Vpu during HIV-1 infection to facilitate late-stage replication. This study provides a framework for the systematic and high-throughput evaluation of protein stability and establishes a more comprehensive portrait of cellular Vpu targets. : Retroviruses use their accessory proteins to evade immune detection and enhance viral replication. Jain et al. developed a high-throughput–high-content imaging platform to study protein stability and degradation. This method was then applied to reveal cellular targets of the HIV-1 accessory factor Vpu. Keywords: Vpu, HIV-1, high-content imaging, protein degradation, interferon-stimulated genes, antiviral, ISGylation, immune evasion

Published

2018

3. A combined EM and proteomic analysis places HIV-1 Vpu at the crossroads of retromer and ESCRT complexes: PTPN23 is a Vpu-cofactor.

Author

Charlotte A Stoneham, Simon Langer, Paul D De Jesus, Jacob M Wozniak, John Lapek, Thomas Deerinck, Andrea Thor, Lars Pache, Sumit K Chanda, David J Gonzalez, Mark Ellisman, and John Guatelli

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

The HIV-1 accessory protein Vpu modulates membrane protein trafficking and degradation to provide evasion of immune surveillance. Targets of Vpu include CD4, HLAs, and BST-2. Several cellular pathways co-opted by Vpu have been identified, but the picture of Vpu's itinerary and activities within membrane systems remains incomplete. Here, we used fusion proteins of Vpu and the enzyme ascorbate peroxidase (APEX2) to compare the ultrastructural locations and the proximal proteomes of wild type Vpu and Vpu-mutants. The proximity-omes of the proteins correlated with their ultrastructural locations and placed wild type Vpu near both retromer and ESCRT-0 complexes. Hierarchical clustering of protein abundances across the mutants was essential to interpreting the data and identified Vpu degradation-targets including CD4, HLA-C, and SEC12 as well as Vpu-cofactors including HGS, STAM, clathrin, and PTPN23, an ALIX-like protein. The Vpu-directed degradation of BST-2 was supported by STAM and PTPN23 and to a much lesser extent by the retromer subunits Vps35 and SNX3. PTPN23 also supported the Vpu-directed decrease in CD4 at the cell surface. These data suggest that Vpu directs targets from sorting endosomes to degradation at multi-vesicular bodies via ESCRT-0 and PTPN23.

Published

2021

4. Restriction factor compendium for influenza A virus reveals a mechanism for evasion of autophagy

Author

Courtney Nguyen, Danielle L. Swaney, Lars Pache, Hong M. Moulton, David A. Stein, Shashank Tripathi, Dexter Pratt, Trey Ideker, Stephen Soonthornvacharin, David Jimenez-Morales, Maite Sanchez-Aparicio, Nish Beltran-Raygoza, Paul D. De Jesus, Randy A. Albrecht, Kelsey M. Haas, Adolfo García-Sastre, Judd F. Hultquist, João I. Mamede, Guojun Wang, Laura Martin-Sancho, Ariel Rodriguez-Frandsen, Christopher Churas, Max W. Chang, Sara Brin Rosenthal, Thong T. Nguyen, Nevan J. Krogan, Sumit K. Chanda, Michael J. McGregor, Laura Riva, and Christopher Benner

Subjects

Microbiology (medical), Immunology, Regulator, Biology, Virus Replication, medicine.disease_cause, Proteomics, Antiviral Agents, Applied Microbiology and Biotechnology, Microbiology, Article, Viral Matrix Proteins, Vaccine Related, Cell membrane, Transcriptome, Biodefense, Autophagy, Genetics, Influenza A virus, medicine, Humans, 2.2 Factors relating to the physical environment, 2.1 Biological and endogenous factors, Aetiology, Immune Evasion, Prevention, GTPase-Activating Proteins, rab7 GTP-Binding Proteins, Cell Biology, Influenza, In vitro, Cell biology, Infectious Diseases, Emerging Infectious Diseases, medicine.anatomical_structure, rab GTP-Binding Proteins, Medical Microbiology, Cytoplasm, Host-Pathogen Interactions, Pneumonia & Influenza, Lysosomes, Infection, Protein Binding

Abstract

The fate of influenza A virus (IAV) infection in the host cell depends on the balance between cellular defence mechanisms and viral evasion strategies. To illuminate the landscape of IAV cellular restriction, we generated and integrated global genetic loss-of-function screens with transcriptomics and proteomics data. Our multi-omics analysis revealed a subset of both IFN-dependent and independent cellular defence mechanisms that inhibit IAV replication. Amongst these, the autophagy regulator TBC1 domain family member 5 (TBC1D5), which binds Rab7 to enable fusion of autophagosomes and lysosomes, was found to control IAV replication in vitro and in vivo and to promote lysosomal targeting of IAV M2 protein. Notably, IAV M2 was observed to abrogate TBC1D5-Rab7 binding through a physical interaction with TBC1D5 via its cytoplasmic tail. Our results provide evidence for the molecular mechanism utilised by IAV M2 protein to escape lysosomal degradation and traffic to the cell membrane, where it supports IAV budding and growth.

Published

2021

5. Discovery of SARS-CoV-2 antiviral drugs through large-scale compound repurposing

Author

Laura Riva, Shuofeng Yuan, Xin Yin, Laura Martin-Sancho, Naoko Matsunaga, Lars Pache, Sebastian Burgstaller-Muehlbacher, Paul D. De Jesus, Peter Teriete, Mitchell V. Hull, Max W. Chang, Jasper Fuk-Woo Chan, Jianli Cao, Vincent Kwok-Man Poon, Kristina M. Herbert, Kuoyuan Cheng, Tu-Trinh H. Nguyen, Andrey Rubanov, Yuan Pu, Courtney Nguyen, Angela Choi, Raveen Rathnasinghe, Michael Schotsaert, Lisa Miorin, Marion Dejosez, Thomas P. Zwaka, Ko-Yung Sit, Luis Martinez-Sobrido, Wen-Chun Liu, Kris M. White, Mackenzie E. Chapman, Emma K. Lendy, Richard J. Glynne, Randy Albrecht, Eytan Ruppin, Andrew D. Mesecar, Jeffrey R. Johnson, Christopher Benner, Ren Sun, Peter G. Schultz, Andrew I. Su, Adolfo García-Sastre, Arnab K. Chatterjee, Kwok-Yung Yuen, and Sumit K. Chanda

Subjects

0301 basic medicine, medicine.medical_specialty, Coronavirus disease 2019 (COVID-19), Morpholines, Induced Pluripotent Stem Cells, Pneumonia, Viral, Drug Evaluation, Preclinical, Cysteine Proteinase Inhibitors, Virus Replication, Antiviral Agents, Models, Biological, Article, Cell Line, Unit (housing), Small Molecule Libraries, Betacoronavirus, 03 medical and health sciences, 0302 clinical medicine, Pandemic, medicine, Humans, Pandemics, Alanine, Multidisciplinary, Dose-Response Relationship, Drug, SARS-CoV-2, Triazines, business.industry, General surgery, Drug Repositioning, Hydrazones, COVID-19, Reproducibility of Results, Drug Synergism, Virus Internalization, Adenosine Monophosphate, COVID-19 Drug Treatment, Pyrimidines, 030104 developmental biology, Gene Expression Regulation, Cardiothoracic surgery, Alveolar Epithelial Cells, 030220 oncology & carcinogenesis, Quality standard, Coronavirus Infections, business

Abstract

Summary The emergence of the novel SARS coronavirus 2 (SARS-CoV-2) in 2019 has triggered an ongoing global pandemic of severe pneumonia-like disease designated as coronavirus disease 2019 (COVID-19)1. The development of a vaccine is likely to require at least 12-18 months, and the typical timeline for approval of a novel antiviral therapeutic can exceed 10 years. Thus, repurposing of known drugs could significantly accelerate the deployment of novel therapies for COVID-19. Towards this end, we profiled a library of known drugs encompassing approximately 12,000 clinical-stage or FDA-approved small molecules. We report the identification of 100 molecules that inhibit viral replication, including 21 known drugs that exhibit dose response relationships. Of these, thirteen were found to harbor effective concentrations likely commensurate with achievable therapeutic doses in patients, including the PIKfyve kinase inhibitor apilimod2–4, and the cysteine protease inhibitors MDL-28170, Z LVG CHN2, VBY-825, and ONO 5334. Notably, MDL-28170, ONO 5334, and apilimod were found to antagonize viral replication in human iPSC-derived pneumocyte-like cells, and the PIKfyve inhibitor also demonstrated antiviral efficacy in a primary human lung explant model. Since most of the molecules identified in this study have already advanced into the clinic, the known pharmacological and human safety profiles of these compounds will enable accelerated preclinical and clinical evaluation of these drugs for the treatment of COVID-19.

Published

2020

6. The Compound SBI-0090799 Inhibits Zika Virus Infection by Blocking De Novo Formation of the Membranous Replication Compartment

Author

Uta Haselmann, Chun-Teng Huang, Paul D. De Jesus, Anthony B. Pinkerton, Scott B. Biering, Alexey V. Terskikh, Andrey Rubanov, Sarah Goellner, Eva Harris, Colin M. Warnes, Sumit K. Chanda, Ralf Bartenschlager, Laura Riva, and Laura Martin-Sancho

Subjects

Daclatasvir, medicine.drug_class, Hepatitis C virus, Immunology, Primary Cell Culture, Drug Evaluation, Preclinical, Biology, medicine.disease_cause, Virus Replication, Microbiology, Antiviral Agents, Virus, Zika virus, Viral entry, Virology, Vaccines and Antiviral Agents, Chlorocebus aethiops, Drug Discovery, medicine, Animals, Humans, NS5A, Vero Cells, Zika Virus Infection, Dendritic Cells, Zika Virus, biology.organism_classification, HEK293 Cells, Viral replication, Insect Science, Astrocytes, Antiviral drug, Viral Replication Compartments, medicine.drug

Abstract

Zika virus (ZIKV) is a mosquito-borne pathogen classified by the World Health Organization (WHO) as a public health emergency of international concern in 2016, and it is still identified as a priority disease. Although most infected individuals are asymptomatic or show mild symptoms, a risk of neurologic complications is associated with infection in adults. Additionally, infection during pregnancy is directly linked to microcephaly and other congenital malformations. Since there are no currently available vaccines or approved therapeutics for this virus, there is a critical unmet need in developing treatments to prevent future ZIKV outbreaks. Towards this end, we performed a large-scale cell-based high-content screen of 51,520 chemical compounds to identify potential antiviral drug candidates. The compound (2E)-N-benzyl-3-(4-butoxyphenyl)prop-2-enamide (SBI-0090799) was found to inhibit replication of multiple ZIKV strains and in different cell systems. SBI-0090799 did not affect viral entry or RNA translation but suppressed RNA replication by preventing the formation of the membranous replication compartment. Selection of drug-resistant viruses identified single amino acid substitions in the N-terminal region of non-structural protein NS4A arguing this to be the likely drug target. These resistance mutations rescued viral RNA replication and restored the formation of the membranous replication compartment. This mechanism of action is similar to clinically-approved NS5A inhibitors for hepatitis C virus (HCV). Taken together, SBI-0090799 represents a promising lead candidate for the development of an antiviral treatment against ZIKV infection for the mitigation of severe complications and potential resurgent outbreaks of the virus. IMPORTANCE This study describes the elucidation of (2E)-N-benzyl-3-(4-butoxyphenyl)prop-2-enamide (SBI-0090799) as selective and potent inhibitor of Zika virus (ZIKV) replication using a high throughput screening approach. Mapping and resistance studies, supported by electron microscopy observations, indicate that the small molecule is functioning through inhibition of NS4A-mediated formation of ZIKV replication compartments in the endoplasmic reticulum (ER). Intriguingly, this defines a novel non-enzymatic target and chemical matter for the development of a new class of ZIKV antivirals. Moreover, chemical modulation affecting this non-structural protein mirrors the identification and development of hepatitis C virus (HCV) NS5A inhibitor daclatasvir and its derivatives, similarly interfering with the formation of the viral replication compartment and also targeting a protein with no enzymatic activity, which have been part of a curative strategy for HCV.

Published

2021

7. Positive regulation of TRAF6-dependent innate immune responses by protein phosphatase PP1-γ.

Author

Amanda M Opaluch, Monika Schneider, Chih-yuan Chiang, Quy T Nguyen, Ana M Maestre, Lubbertus C F Mulder, Ismael Secundino, Paul D De Jesus, Renate König, Viviana Simon, Victor Nizet, Graham MacLeod, Susannah Varmuza, Ana Fernandez-Sesma, and Sumit K Chanda

Subjects

Medicine, Science

Abstract

Innate immune sensors such as Toll-like receptors (TLRs) differentially utilize adaptor proteins and additional molecular mediators to ensure robust and precise immune responses to pathogen challenge. Through a gain-of-function genetic screen, we identified the gamma catalytic subunit of protein phosphatase 1 (PP1-γ) as a positive regulator of MyD88-dependent proinflammatory innate immune activation. PP1-γ physically interacts with the E3 ubiquitin ligase TRAF6, and enhances the activity of TRAF6 towards itself and substrates such as IKKγ, whereas enzymatically inactive PP1-γ represses these events. Importantly, these activities were found to be critical for cellular innate responses to pathogen challenge and microbial clearance in both mouse macrophages and human monocyte lines. These data indicate that PP1-γ phosphatase activity regulates overall TRAF6 E3 ubiquitin ligase function and promotes NF-κB-mediated innate signaling responses.

Published

2014

8. Functional Landscape of SARS-CoV-2 Cellular Restriction

Author

Christopher Churas, Lisa Miorin, Dexter Pratt, Anshu P. Gounder, Aaron L. Oom, Laura Martin-Sancho, Sumit K. Chanda, Judd F. Hultquist, Sophie Liu, Courtney Nguyen, Max W. Chang, Ariel Rodriguez-Frandsen, Trey Ideker, Alan M. O’Neill, Matthew Urbanowski, Yuan Pu, Megan L. Shaw, Sara Brin Rosenthal, John C. Guatelli, Paul D. De Jesus, Charlotte A. Stoneham, Christopher Benner, Mary K. Lewinski, Matthew B. Frieman, Lars Pache, Adolfo García-Sastre, and Xin Yin

Subjects

Innate immune system, business.industry, Center of excellence, viruses, Viral translation, virus diseases, Biology, Influenza research, Virology, Article, Immune system, Viral replication, Interferon, Viral entry, Biosafety level, Tetherin, medicine, business, Gene, medicine.drug

Abstract

A deficient interferon response to SARS-CoV-2 infection has been implicated as a determinant of severe COVID-19. To identify the molecular effectors that govern interferon control of SARS-CoV-2 infection, we conducted a large-scale gain-of-function analysis that evaluated the impact of human interferon stimulated genes (ISGs) on viral replication. A limited subset of ISGs were found to control viral infection, including endosomal factors that inhibited viral entry, nucleic acid binding proteins that suppressed viral RNA synthesis, and a highly enriched cluster of ER and Golgi-resident ISGs that inhibited viral translation and egress. These included the type II integral membrane protein BST2/tetherin, which was found to impede viral release, and is targeted for immune evasion by SARS-CoV-2 Orf7a protein. Overall, these data define the molecular basis of early innate immune control of viral infection, which will facilitate the understanding of host determinants that impact disease severity and offer potential therapeutic strategies for COVID-19. Funding: This work was supported by the following grants to the Sanford Burnham Prebys Medical Discovery Institute and the Icahn School of medicine at Mount Sinai: DoD: W81XWH-20-10270; DHIPC: U19 AI118610; Fluomics/NOSI: U19 AI135972. This work was also supported by generous philanthropic donations from Dinah Ruch and Susan & James Blair, from the JPB Foundation, the Open Philanthropy Project (research grant 2020-215611 (5384)) and anonymous donors. Additional support has been provided by DARPA grant HR0011-19-2-0020 and by CRIP (Center for research on Influenza Pathogenesis), a NIAID-funded Center of Excellence for Influenza Research and Surveillance (CEIRS, contract # HHSN272201400008C). This work was additionally supported by the following grants to Northwestern University Feinberg School of Medicine: a CTSA supplement to NCATS: UL1 TR002389; a CTSA supplement to NUCATS with the generous support of the Dixon family: UL1 TR001422; and a Cancer Center supplement: P30 CA060553, and the following grant to JG at UC San Diego: NIH grant R37AI081668. This work was also supported by a generous grant from the James B. Pendleton Charitable Trust. Conflict of Interest: The authors declare no competing interests. Ethical Approval: All experiments involving live SARS-CoV-2 followed the approved standard operating procedures of the Biosafety Level 3 facility at the Sanford Burnham Prebys Medical Discovery Institute.

Published

2020

9. A Large-scale Drug Repositioning Survey for SARS-CoV-2 Antivirals

Author

Sumit K. Chanda, Tu-Trinh Nguyen, Ren Sun, Adolfo García-Sastre, Andrew I. Su, Arnab K. Chatterjee, Andrey Rubanov, Kris M. White, Sebastian Burgstaller, Laura Riva, Luis Martinez-Sobrido, Xin Yin, Lars Pache, Jasper Fuk-Woo Chan, Kristina M. Herbert, Jeffrey R Johnson, Mitchell V. Hull, Max W. Chang, Shuofeng Yuan, Christopher Benner, Jianli Cao, Kwok-Yung Yuen, Peter G. Schultz, Naoko Matsunaga, Wen-Chun Lui, Laura Martin-Sancho, Paul D. De Jesus, Yuan Pu, Vincent Kwok-Man Poon, Lisa Miorin, and Courtney Nguyen

Subjects

Drug, business.industry, media_common.quotation_subject, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Disease, Bioinformatics, Article, Drug repositioning, PIKFYVE, Viral replication, Pandemic, Medicine, In patient, business, media_common

Abstract

The emergence of novel SARS coronavirus 2 (SARS-CoV-2) in 2019 has triggered an ongoing global pandemic of severe pneumonia-like disease designated as coronavirus disease 2019 (COVID-19). To date, more than 2.1 million confirmed cases and 139,500 deaths have been reported worldwide, and there are currently no medical countermeasures available to prevent or treat the disease. As the development of a vaccine could require at least 12-18 months, and the typical timeline from hit finding to drug registration of an antiviral is >10 years, repositioning of known drugs can significantly accelerate the development and deployment of therapies for COVID-19. To identify therapeutics that can be repurposed as SARS-CoV-2 antivirals, we profiled a library of known drugs encompassing approximately 12,000 clinical-stage or FDA-approved small molecules. Here, we report the identification of 30 known drugs that inhibit viral replication. Of these, six were characterized for cellular dose-activity relationships, and showed effective concentrations likely to be commensurate with therapeutic doses in patients. These include the PIKfyve kinase inhibitor Apilimod, cysteine protease inhibitors MDL-28170, Z LVG CHN2, VBY-825, and ONO 5334, and the CCR1 antagonist MLN-3897. Since many of these molecules have advanced into the clinic, the known pharmacological and human safety profiles of these compounds will accelerate their preclinical and clinical evaluation for COVID-19 treatment.

Published

2020

10. Large-Scale Arrayed Analysis of Protein Degradation Reveals Cellular Targets for HIV-1 Vpu

Author

Simon Langer, Lars Pache, Paul D. De Jesus, Sunnie M. Yoh, Kevin C. Olivieri, Alex J. Portillo, Prashant Jain, Quy T. Nguyen, Sumit K. Chanda, Guney Boso, and Stephen Soonthornvacharin

Subjects

0301 basic medicine, Proteasome Endopeptidase Complex, viruses, Human Immunodeficiency Virus Proteins, Human immunodeficiency virus (HIV), Down-Regulation, Computational biology, Biology, Protein degradation, medicine.disease_cause, Antiviral Agents, Article, General Biochemistry, Genetics and Molecular Biology, Cellular protein, 03 medical and health sciences, medicine, Humans, Viral Regulatory and Accessory Proteins, lcsh:QH301-705.5, Gene, chemistry.chemical_classification, DNA ligase, Protein Stability, Virion, Reproducibility of Results, virus diseases, ISG15, Transmembrane protein, 3. Good health, HEK293 Cells, 030104 developmental biology, lcsh:Biology (General), Viral replication, chemistry, Proteolysis, HIV-1, Interferons, HeLa Cells

Abstract

Summary: Accessory proteins of lentiviruses, such as HIV-1, target cellular restriction factors to enhance viral replication. Systematic analyses of proteins that are targeted for degradation by HIV-1 accessory proteins may provide a better understanding of viral immune evasion strategies. Here, we describe a high-throughput platform developed to study cellular protein stability in a highly parallelized matrix format. We used this approach to identify cellular targets of the HIV-1 accessory protein Vpu through arrayed coexpression with 433 interferon-stimulated genes, followed by differential fluorescent labeling and automated image analysis. Among the previously unreported Vpu targets identified by this approach, we find that the E2 ligase mediating ISG15 conjugation, UBE2L6, and the transmembrane protein PLP2 are targeted by Vpu during HIV-1 infection to facilitate late-stage replication. This study provides a framework for the systematic and high-throughput evaluation of protein stability and establishes a more comprehensive portrait of cellular Vpu targets. : Retroviruses use their accessory proteins to evade immune detection and enhance viral replication. Jain et al. developed a high-throughput–high-content imaging platform to study protein stability and degradation. This method was then applied to reveal cellular targets of the HIV-1 accessory factor Vpu. Keywords: Vpu, HIV-1, high-content imaging, protein degradation, interferon-stimulated genes, antiviral, ISGylation, immune evasion

Published

2018

11. Broad Spectrum Inhibitor of Influenza A and B Viruses Targeting the Viral Nucleoprotein

Author

Sumit K. Chanda, Pablo Abreu, Balaji Manicassamy, Kris M. White, Paul D. De Jesus, Megan L. Shaw, Robert J. DeVita, Adolfo García-Sastre, and Hui Wang

Subjects

Gene Expression Regulation, Viral, 0301 basic medicine, Influenzavirus B, Microbial Sensitivity Tests, Virus Replication, Antiviral Agents, Article, Cell Line, Protein Aggregates, 03 medical and health sciences, Oseltamivir, Transcription (biology), medicine, Animals, Humans, Binding site, Cytotoxicity, IC50, Cellular localization, Molecular Structure, Chemistry, Viral Core Proteins, Drug Synergism, Virus Internalization, Virology, Nucleoprotein, 030104 developmental biology, Infectious Diseases, Mechanism of action, Viral replication, Influenza A virus, medicine.symptom, Protein Binding

Abstract

S119 was a top hit from an ultrahigh throughput screen performed to identify novel inhibitors of influenza virus replication. It showed a potent antiviral effect (50% inhibitory concentration, IC50 = 20 nM) and no detectable cytotoxicity (50% cytotoxic concentration, CC50 > 500 μM) to yield a selectivity index greater than 25 000. Upon investigation, we found that S119 selected for resistant viruses carrying mutations in the viral nucleoprotein (NP). These resistance mutations highlight a likely S119 binding site overlapping with but not identical to that found for the compound nucleozin. Mechanism of action studies revealed that S119 affects both the oligomerization state and cellular localization of the NP protein which has an impact on viral transcription, replication, and protein expression. Through a hit-to-lead structure−activity relationship (SAR) study, we found an analog of S119, named S119–8, which had increased breadth of inhibition against influenza A and B viruses accompanied by only a small loss in potency. Finally, in vitro viral inhibition assays showed a synergistic relationship between S119–8 and oseltamivir when they were combined, indicating the potential for future drug cocktails.

Published

2018

12. Functional landscape of SARS-CoV-2 cellular restriction

Author

Trey Ideker, Megan L. Shaw, Sara Brin Rosenthal, Matthew Urbanowski, Sumit K. Chanda, Chunxiang Wu, Thomas J. Hope, Yong Xiong, Charlotte A. Stoneham, Matthew B. Frieman, Aaron L. Oom, John C. Guatelli, Dexter Pratt, Sophie Liu, Christopher Churas, Courtney Nguyen, Anshu P. Gounder, Mary K. Lewinski, Lisa Miorin, Adolfo García-Sastre, Mark E. Becker, Stuart Weston, Yuan Pu, Alan M. O’Neill, Max W. Chang, Laura Martin-Sancho, Christopher Benner, Fan Zheng, Heather M. Curry, Paul D. De Jesus, Judd F. Hultquist, Ariel Rodriguez-Frandsen, Xin Yin, and Lars Pache

Subjects

Protein Conformation, viruses, Golgi Apparatus, RNA-binding protein, Endoplasmic Reticulum, Virus Replication, Medical and Health Sciences, 0302 clinical medicine, Interferon, Chlorocebus aethiops, Innate, Orf7a, 2.1 Biological and endogenous factors, Aetiology, innate immunity, Lung, Virus Release, 0303 health sciences, Tumor, Effector, viral evasion, virus diseases, interferon, Biological Sciences, CD, Molecular Docking Simulation, Infectious Diseases, Interferon Type I, Interferon Regulatory Factors, Host-Pathogen Interactions, Pneumonia & Influenza, Infection, Signal Transduction, Protein Binding, medicine.drug, Resource, BST2, Biology, GPI-Linked Proteins, Cell Line, ISG, Vaccine Related, Viral Proteins, 03 medical and health sciences, Viral entry, Biodefense, Genetics, medicine, Animals, Humans, Protein Interaction Domains and Motifs, Antigens, Vero Cells, Molecular Biology, Gene, 030304 developmental biology, Binding Sites, Innate immune system, SARS-CoV-2, Prevention, alpha-Helical, Immunity, Pneumonia, Cell Biology, Virus Internalization, Virology, HEK293 Cells, Emerging Infectious Diseases, Good Health and Well Being, Gene Expression Regulation, Viral replication, Tetherin, beta-Strand, 030217 neurology & neurosurgery, Developmental Biology

Abstract

A deficient interferon (IFN) response to severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection has been implicated as a determinant of severe coronavirus disease 2019 (COVID-19). To identify the molecular effectors that govern IFN control of SARS-CoV-2 infection, we conducted a large-scale gain-of-function analysis that evaluated the impact of human IFN-stimulated genes (ISGs) on viral replication. A limited subset of ISGs were found to control viral infection, including endosomal factors inhibiting viral entry, RNA binding proteins suppressing viral RNA synthesis, and a highly enriched cluster of endoplasmic reticulum (ER)/Golgi-resident ISGs inhibiting viral assembly/egress. These included broad-acting antiviral ISGs and eight ISGs that specifically inhibited SARS-CoV-2 and SARS-CoV-1 replication. Among the broad-acting ISGs was BST2/tetherin, which impeded viral release and is antagonized by SARS-CoV-2 Orf7a protein. Overall, these data illuminate a set of ISGs that underlie innate immune control of SARS-CoV-2/SARS-CoV-1 infection, which will facilitate the understanding of host determinants that impact disease severity and offer potential therapeutic strategies for COVID-19., Graphical abstract, Deficient interferon responses to SARS-CoV-2 infection have been associated with severe COVID-19. Martin-Sancho et al. utilized a gain-of-function screen to identify interferon-stimulated effectors that govern innate immune responses to SARS-CoV-2. These factors could underlie genetic predisposition to severe COVID-19 and can serve as candidates for development of antiviral therapies.

Published

2021

13. Viral Determinants in H5N1 Influenza A Virus Enable Productive Infection of HeLa Cells

Author

Courtney Nguyen, Wen-Chun Liu, Sumit K. Chanda, Ariel Rodriguez-Frandsen, Paul D. De Jesus, Adolfo García-Sastre, Monica Chavarria, Saunil Dobariya, Max W. Chang, Kristina M. Herbert, Ignacio Mena, Laura Riva, Jessica von Recum-Knepper, Nicholas J Huffmaster, Miriam S. Dutra, Christopher Benner, Randy A. Albrecht, Anshu P. Gounder, and Laura Martin-Sancho

Subjects

Viral budding, viruses, Immunology, Hemagglutinin (influenza), medicine.disease_cause, Virus Replication, Microbiology, Cell Line, Madin Darby Canine Kidney Cells, Birds, Dogs, Influenza A Virus, H1N1 Subtype, Virology, Influenza, Human, medicine, Influenza A virus, Animals, Humans, Tropism, Host factor, biology, Influenza A Virus, H5N1 Subtype, Influenza A Virus, H3N2 Subtype, virus diseases, Influenza A virus subtype H5N1, Nucleoprotein, Virus-Cell Interactions, Viral Tropism, HEK293 Cells, Cell culture, A549 Cells, Insect Science, Influenza in Birds, biology.protein, HeLa Cells

Abstract

Influenza A virus (IAV) is a human respiratory pathogen that causes yearly global epidemics, as well as sporadic pandemics due to human adaptation of pathogenic strains. Efficient replication of IAV in different species is, in part, dictated by its ability to exploit the genetic environment of the host cell. To investigate IAV tropism in human cells, we evaluated the replication of IAV strains in a diverse subset of epithelial cell lines. HeLa cells were refractory to the growth of human H1N1 and H3N2 viruses and low-pathogenic avian influenza (LPAI) viruses. Interestingly, a human isolate of the highly pathogenic avian influenza (HPAI) H5N1 virus successfully propagated in HeLa cells to levels comparable to those in a human lung cell line. Heterokaryon cells generated by fusion of HeLa and permissive cells supported H1N1 virus growth, suggesting the absence of a host factor(s) required for the replication of H1N1, but not H5N1, viruses in HeLa cells. The absence of this factor(s) was mapped to reduced nuclear import, replication, and translation, as well as deficient viral budding. Using reassortant H1N1:H5N1 viruses, we found that the combined introduction of nucleoprotein (NP) and hemagglutinin (HA) from an H5N1 virus was necessary and sufficient to enable H1N1 virus growth. Overall, this study suggests that the absence of one or more cellular factors in HeLa cells results in abortive replication of H1N1, H3N2, and LPAI viruses, which can be circumvented upon the introduction of H5N1 virus NP and HA. Further understanding of the molecular basis of this restriction will provide important insights into the virus-host interactions that underlie IAV pathogenesis and tropism. IMPORTANCE Many zoonotic avian influenza A viruses have successfully crossed the species barrier and caused mild to life-threatening disease in humans. While human-to-human transmission is limited, there is a risk that these zoonotic viruses may acquire adaptive mutations enabling them to propagate efficiently and cause devastating human pandemics. Therefore, it is important to identify viral determinants that provide these viruses with a replicative advantage in human cells. Here, we tested the growth of influenza A virus in a subset of human cell lines and found that abortive replication of H1N1 viruses in HeLa cells can be circumvented upon the introduction of H5N1 virus HA and NP. Overall, this work leverages the genetic diversity of multiple human cell lines to highlight viral determinants that could contribute to H5N1 virus pathogenesis and tropism.

Published

2019

14. HIV-1 Vpu is a potent transcriptional suppressor of NF-κB-elicited antiviral immune responses

Author

Simon Langer, Christian Hammer, Kristina Hopfensperger, Lukas Klein, Dominik Hotter, Paul D De Jesus, Kristina M Herbert, Lars Pache, Nikaïa Smith, Johannes A van der Merwe, Sumit K Chanda, Jacques Fellay, Frank Kirchhoff, and Daniel Sauter

Subjects

CD4-Positive T-Lymphocytes, Transcription, Genetic, animal diseases, viruses, Human Immunodeficiency Virus Proteins, Communicable diseases, NF-κB, Immunology and Inflammation, Viral Regulatory and Accessory Proteins, RNA-Seq, Allergy and immunology, Biology (General), Cells, Cultured, Microbiology and Infectious Disease, T-Lymphocytes, Immunology, Tetherin, NF-kappa B, virus diseases, tetherin, Virus, Nuklearfaktor Kappa B, Host-Pathogen Interactions, Medicine, Research Article, Human, QH301-705.5, Science, Down-Regulation, Infectious Disease, Microbiology, immune activation, NF-��B, Vpu, Humans, ddc:610, Immune Evasion, Inflammation, Immune activation, Immunity, HIV, Viral proteins, biochemical phenomena, metabolism, and nutrition, Immunity, Innate, FOS: Biological sciences, Mikrobiologie, HIV-1, Infektionskrankheit, DDC 610 / Medicine & health

Abstract

Many viral pathogens target innate sensing cascades and/or cellular transcription factors to suppress antiviral immune responses. Here, we show that the accessory viral protein U (Vpu) of HIV-1 exerts broad immunosuppressive effects by inhibiting activation of the transcription factor NF-κB. Global transcriptional profiling of infected CD4 +T cells revealed that vpu-deficient HIV-1 strains induce substantially stronger immune responses than the respective wild type viruses. Gene set enrichment analyses and cytokine arrays showed that Vpu suppresses the expression of NF-κB targets including interferons and restriction factors. Mutational analyses demonstrated that this immunosuppressive activity of Vpu is independent of its ability to counteract the restriction factor and innate sensor tetherin. However, Vpu-mediated inhibition of immune activation required an arginine residue in the cytoplasmic domain that is critical for blocking NF-κB signaling downstream of tetherin. In summary, our findings demonstrate that HIV-1 Vpu potently suppresses NF-κB-elicited antiviral immune responses at the transcriptional level., eLife digest The Human Immunodeficiency Virus (or HIV for short) has infected more than 70 million people worldwide. Although effective therapies exist to prevent the replication of the virus and the development to AIDS, there is no cure or vaccine, and the virus still spreads efficiently in human populations, infecting about 1.8 million new people every year. The unfortunate success of HIV can in part be explained by several viral proteins that trick our immune system and enable the virus to persist at high levels in the human body. For example, an HIV protein called viral protein U (Vpu) prevents infected cells from producing alarm signals such as interferons, which usually help healthy, uninfected cells to defend themselves against viruses. However, the extent to which Vpu interferes with interferons and other proteins involved in immune responses has remained unclear. To address this question, Langer, Hammer, Hopfensperger et al. compared how different variants of HIV affect immune responses in human cells. The experiments showed that cells infected with HIV variants lacking Vpu released larger amounts of interferons and other cellular proteins that are involved in immune responses compared to HIV variants with Vpu. Further experiments showed that Vpu works by inhibiting the activation of a protein called NF-κB, which usually switches on genes that encode interferons and many other proteins involved in immune responses. These findings demonstrate that Vpu has a broader impact on the human immune response than previously thought. In order to multiply efficiently, HIV initially requires the NF-κB protein to be active. Therefore, when NF-κB is inactive, HIV may adopt a dormant state that prevents current antiviral drug treatments from eradicating the virus in the human body. In the future, developing new drugs that can activate dormant HIV particles may therefore have the potential to help cure HIV infections.

Published

2019

15. Author response: HIV-1 Vpu is a potent transcriptional suppressor of NF-κB-elicited antiviral immune responses

Author

Kristina M. Herbert, Simon Langer, Dominik Hotter, Johannes A. van der Merwe, Christian Hammer, Lars Pache, Jacques Fellay, Lukas Klein, Kristina Hopfensperger, Frank Kirchhoff, Sumit K. Chanda, Nikaïa Smith, Daniel Sauter, and Paul D. De Jesus

Subjects

chemistry.chemical_compound, Immune system, chemistry, law, Human immunodeficiency virus (HIV), medicine, Cancer research, Suppressor, NF-κB, Biology, medicine.disease_cause, law.invention

Published

2019

16. SNW1, a Novel Transcriptional Regulator of the NF-κB Pathway

Author

Inder M. Verma, Suneer Verma, Paul D. De Jesus, and Sumit K. Chanda

Subjects

Transcriptional Activation, Transcription, Genetic, THP-1 Cells, Nuclear Receptor Coactivators, Biology, Splicing factor, chemistry.chemical_compound, Transcription (biology), RNA interference, Transcriptional regulation, Humans, Positive Transcriptional Elongation Factor B, Promoter Regions, Genetic, Molecular Biology, Gene, Transcription factor, Tumor Necrosis Factor-alpha, Macrophages, NF-kappa B, Transcription Factor RelA, NF-κB, Cell Biology, Cell biology, chemistry, Gene Expression Regulation, RNA splicing, Research Article, Signal Transduction, Transcription Factors

Abstract

The nuclear factor kappa B (NF-κB) family of transcription factors plays a central role in coordinating the expression of genes that control inflammation, immune responses, cell proliferation, and a variety of other biological processes. In an attempt to identify novel regulators of this pathway, we performed whole-genome RNA interference (RNAi) screens in physiologically relevant human macrophages in response to lipopolysaccharide and tumor necrosis factor alpha (TNF-α). The top hit was SNW1, a splicing factor and transcriptional coactivator. SNW1 does not regulate the cytoplasmic components of the NF-κB pathway but complexes with the NF-κB heterodimer in the nucleus for transcriptional activation. We show that SNW1 detaches from its splicing complex (formed with SNRNP200 and SNRNP220) upon NF-κB activation and binds to NF-κB's transcriptional elongation partner p-TEFb. We also show that SNW1 is indispensable for the transcriptional elongation of NF-κB target genes such as the interleukin 8 (IL-8) and TNF genes. SNW1 is a unique protein previously shown to be involved in both splicing and transcription, and in this case, its role involves binding to the NF-κB-p-TEFb complex to facilitate transcriptional elongation of some NF-κB target genes.

Published

2019

17. RIOK3 Is an Adaptor Protein Required for IRF3-Mediated Antiviral Type I Interferon Production

Author

Victoria Su, Ting-Ting Wu, Paul D. De Jesus, Stephanie Han, Yuan Tian, Xudong Li, Nicholas C. Wu, Jun Feng, Sumit K. Chanda, Danyang Gong, Ren Sun, and Hutt-Fletcher, L

Subjects

1.1 Normal biological development and functioning, viruses, Immunology, Cellular Response to Infection, Protein Serine-Threonine Kinases, Biology, Medical and Health Sciences, Microbiology, Cell Line, Vaccine Related, Gammaherpesvirinae, Underpinning research, RNA interference, Interferon, Biodefense, Virology, Genetics, medicine, 2.1 Biological and endogenous factors, Animals, Humans, Aetiology, Innate immune system, Agricultural and Veterinary Sciences, Prevention, Inflammatory and immune system, Pattern recognition receptor, virus diseases, Biological Sciences, biochemical phenomena, metabolism, and nutrition, Protein-Serine-Threonine Kinases, Type I interferon production, Acquired immune system, Infectious Diseases, Emerging Infectious Diseases, Good Health and Well Being, Influenza A virus, Insect Science, Interferon Type I, HIV/AIDS, Interferon Regulatory Factor-3, Infection, Transcriptome, IRF3, Interferon type I, Protein Binding, medicine.drug

Abstract

Detection of cytosolic nucleic acids by pattern recognition receptors leads to the induction of type I interferons (IFNs) and elicits the innate immune response. We report here the identification of RIOK3 as a novel adaptor protein that is essential for the cytosolic nucleic acid-induced type I IFN production and for the antiviral response to gammaherpesvirus through two independent kinome-wide RNA interference screens. RIOK3 knockdown blocks both cytosolic double-stranded B-form DNA and double-stranded RNA-induced IRF3 activation and IFN-β production. In contrast, the overexpression of RIOK3 activates IRF3 and induces IFN-β. RIOK3 functions downstream of TBK1 and upstream of IRF3 activation. Furthermore, RIOK3 physically interacts with both IRF3 and TBK1 and is necessary for the interaction between TBK1 and IRF3. In addition, global transcriptome analysis shows that the expression of many gene involved antiviral responses is dependent on RIOK3. Thus, knockdown of RIOK3 inhibits cellular antiviral responses against both DNA and RNA viruses (herpesvirus and influenza A virus). Our data suggest that RIOK3 plays a critical role in the antiviral type I IFN pathway by bridging TBK1 and IRF3. IMPORTANCE The innate immune response, such as the production of type I interferons, acts as the first line of defense, limiting infectious pathogens directly and shaping the adaptive immune response. In this study, we identified RIOK3 as a novel regulator of the antiviral type I interferon pathway. Specifically, we found that RIOK3 physically interacts with TBK1 and IRF3 and bridges the functions between TBK1 and IRF3 in the activation of type I interferon pathway. The identification of a cellular kinase that plays a role the type I interferon pathway adds another level of complexity in the regulation of innate immunity and will have implications for developing novel strategies to combat viral infection.

Published

2014

18. Cofactors Required for TLR7- and TLR9-Dependent Innate Immune Responses

Author

Ismael Secundino, Loren Miraglia, Paul D. De Jesus, Ana Fernandez-Sesma, Quy T. Nguyen, Irene Ramos, Chih-yuan Chiang, Yingyao Zhou, Ghislain M. C. Bonamy, Genevieve Welch, Victor Nizet, Ana M. Maestre, Anthony P. Orth, Amanda M. Opaluch, Gregory M. Barton, Alex Engel, and Sumit K. Chanda

Subjects

Cancer Research, Support Vector Machine, Endocytic cycle, Chick Embryo, Endosomes, Biology, Models, Biological, Microbiology, Article, 03 medical and health sciences, 0302 clinical medicine, RNA interference, Immunology and Microbiology(all), Virology, Animals, Humans, Computer Simulation, Gene Regulatory Networks, Molecular Biology, 030304 developmental biology, 0303 health sciences, Innate immune system, Endosomal Sorting Complexes Required for Transport, Gene Expression Profiling, Intracellular Signaling Peptides and Proteins, Pattern recognition receptor, TLR7, Phosphoproteins, Endolysosome, Immunity, Innate, Cell biology, Chromatin, Protein Transport, HEK293 Cells, Toll-Like Receptor 7, Gene Knockdown Techniques, Toll-Like Receptor 9, 030220 oncology & carcinogenesis, Myeloid Differentiation Factor 88, RNA Interference, Parasitology, Signal transduction, Signal Transduction

Abstract

SummaryPathogens commonly utilize endocytic pathways to gain cellular access. The endosomal pattern recognition receptors TLR7 and TLR9 detect pathogen-encoded nucleic acids to initiate MyD88-dependent proinflammatory responses to microbial infection. Using genome-wide RNAi screening and integrative systems-based analysis, we identify 190 cofactors required for TLR7- and TLR9-directed signaling responses. A set of cofactors were crossprofiled for their activities downstream of several immunoreceptors and then functionally mapped based on the known architecture of NF-κB signaling pathways. Protein complexes and pathways involved in ubiquitin-protein ligase activities, sphingolipid metabolism, chromatin modifications, and ancient stress responses were found to modulate innate recognition of endosomal nucleic acids. Additionally, hepatocyte growth factor-regulated tyrosine kinase substrate (HRS) was characterized as necessary for ubiquitin-dependent TLR9 targeting to the endolysosome. Proteins and pathways identified here should prove useful in delineating strategies to manipulate innate responses for treatment of autoimmune disorders and microbial infection.

Published

2012

19. Systems-based Analysis of RIG-I-dependent Signaling Identifies KHSRP as an Inhibitor of RIG-I Receptor Activation

Author

Stephen Soonthornvacharin, Yingyao Zhou, Ariel Rodriguez-Frandsen, Elisa de Castro, Hong M. Moulton, Maria Teresa Sánchez-Aparicio, Adolfo García-Sastre, David A. Stein, Vinod Balasubramaniam, Shashank Tripathi, Atsushi Inoue, Nicholas J Huffmaster, Felipe Galvez, Paul D. De Jesus, Quy T. Nguyen, Renate König, Sumit K. Chanda, Sunnie M. Yoh, and Nevan J. Krogan

Subjects

0301 basic medicine, Microbiology (medical), viruses, Immunology, Regulator, Biology, Applied Microbiology and Biotechnology, Microbiology, Article, 03 medical and health sciences, 0302 clinical medicine, Influenza A Virus, H1N1 Subtype, RNA interference, Protein Interaction Mapping, Genetics, Humans, Protein Interaction Maps, Receptors, Immunologic, Regulation of gene expression, RIG-I, RNA, RNA-Binding Proteins, Cell Biology, Immunity, Innate, Cell biology, 030104 developmental biology, HEK293 Cells, RNA splicing, Unfolded protein response, Trans-Activators, DEAD Box Protein 58, RNA, Viral, Signal transduction, 030215 immunology, Protein Binding, Signal Transduction

Abstract

Retinoic acid-inducible gene I (RIG-I) receptor recognizes 5'-triphosphorylated RNA and triggers a signalling cascade that results in the induction of type-I interferon (IFN)-dependent responses. Its precise regulation represents a pivotal balance between antiviral defences and autoimmunity. To elucidate the cellular cofactors that regulate RIG-I signalling, we performed two global RNA interference analyses to identify both positive and negative regulatory nodes operating on the signalling pathway during virus infection. These factors were integrated with experimentally and computationally derived interactome data to build a RIG-I protein interaction network. Our analysis revealed diverse cellular processes, including the unfolded protein response, Wnt signalling and RNA metabolism, as critical cellular components governing innate responses to non-self RNA species. Importantly, we identified K-Homology Splicing Regulatory Protein (KHSRP) as a negative regulator of this pathway. We find that KHSRP associates with the regulatory domain of RIG-I to maintain the receptor in an inactive state and attenuate its sensing of viral RNA (vRNA). Consistent with increased RIG-I antiviral signalling in the absence of KHSRP, viral replication is reduced when KHSRP expression is knocked down both in vitro and in vivo. Taken together, these data indicate that KHSRP functions as a checkpoint regulator of the innate immune response to pathogen challenge.

Published

2017

20. A Potent Anti-influenza Compound Blocks Fusion through Stabilization of the Prefusion Conformation of the Hemagglutinin Protein

Author

Peter Palese, Adolfo García-Sastre, Quy T. Nguyen, Renate Koenig, Kelli Kuhen, Paul D. De Jesus, Atsushi Inoue, Pablo Abreu, Paul Anderson, Megan L. Shaw, Puiying A. Mak, Elisa Barile, Zhong Chen, Silke Stertz, Sumit K. Chanda, Maurizio Pellecchia, and Kris M. White

Subjects

fusion, Lipid bilayer fusion, screen, Biology, medicine.disease_cause, Virology, Small molecule, antiviral, Virus, Influenza A virus subtype H5N1, Article, law.invention, Infectious Diseases, Viral replication, Docking (molecular), law, docking, medicine, Recombinant DNA, hemagglutinin, Binding site, influenza

Abstract

An ultrahigh-throughput screen was performed to identify novel small molecule inhibitors of influenza virus replication. The screen employed a recombinant influenza A/WSN/33 virus expressing Renilla luciferase and yielded a hit rate of 0.5%, of which the vast majority showed little cytotoxicity at the inhibitory concentration. One of the top hits from this screen, designated S20, inhibits HA-mediated membrane fusion. S20 shows potent antiviral activity (IC50 = 80 nM) and low toxicity (CC50 = 40 μM), yielding a selectivity index of 500 and functionality against all of the group 1 influenza A viruses tested in this study, including the pandemic H1N1 and avian H5N1 viruses. Mechanism of action studies proved a direct S20-HA interaction and showed that S20 inhibits fusion by stabilizing the prefusion conformation of HA. In silico docking studies were performed, and the predicted binding site in HA2 corresponds with the area where resistance mutations occurred and correlates with the known role of this region in fusion. This high-throughput screen has yielded many promising new lead compounds, including S20, which will potentially shed light on the molecular mechanisms of viral infection and serve as research tools or be developed for clinical use as antivirals.

Published

2014

21. Positive regulation of TRAF6-dependent innate immune responses by protein phosphatase PP1-γ

Author

Viviana Simon, Lubbertus C. F. Mulder, Quy T. Nguyen, Sumit K. Chanda, Susannah Varmuza, Renate König, Ismael Secundino, Chih-yuan Chiang, Paul D. De Jesus, Victor Nizet, Monika Schneider, Ana Fernandez-Sesma, Graham MacLeod, Amanda M. Opaluch, and Ana M. Maestre

Subjects

Mouse, lcsh:Medicine, Monocytes, Mice, Protein Phosphatase 1, Molecular Cell Biology, RNA, Small Interfering, lcsh:Science, Cells, Cultured, Multidisciplinary, Reverse Transcriptase Polymerase Chain Reaction, Mechanisms of Signal Transduction, Toll-Like Receptors, NF-kappa B, High-Throughput Nucleotide Sequencing, Signal transducing adaptor protein, Animal Models, Innate Immunity, 3. Good health, Cell biology, Ubiquitin ligase, Host-Pathogen Interaction, medicine.anatomical_structure, Research Article, Signal Transduction, Immune Cells, Immunology, Blotting, Western, Phosphatase, Enzyme-Linked Immunosorbent Assay, Biology, Real-Time Polymerase Chain Reaction, Microbiology, Signaling Pathways, Model Organisms, Immune system, Streptococcal Infections, medicine, Animals, Humans, Immunoprecipitation, RNA, Messenger, Immunity to Infections, Inflammation, TNF Receptor-Associated Factor 6, Innate immune system, Macrophages, Monocyte, lcsh:R, Immunity, Streptococcus, Protein phosphatase 1, Dendritic Cells, NFKB1, Molecular biology, Immunity, Innate, Gene Expression Regulation, 13. Climate action, Mutation, Myeloid Differentiation Factor 88, biology.protein, lcsh:Q

Abstract

Innate immune sensors such as Toll-like receptors (TLRs) differentially utilize adaptor proteins and additional molecular mediators to ensure robust and precise immune responses to pathogen challenge. Through a gain-of-function genetic screen, we identified the gamma catalytic subunit of protein phosphatase 1 (PP1-γ) as a positive regulator of MyD88-dependent proinflammatory innate immune activation. PP1-γ physically interacts with the E3 ubiquitin ligase TRAF6, and enhances the activity of TRAF6 towards itself and substrates such as IKKγ, whereas enzymatically inactive PP1-γ represses these events. Importantly, these activities were found to be critical for cellular innate responses to pathogen challenge and microbial clearance in both mouse macrophages and human monocyte lines. These data indicate that PP1-γ phosphatase activity regulates overall TRAF6 E3 ubiquitin ligase function and promotes NF-κB-mediated innate signaling responses.

Published

2014

22. Tumor suppressor protein (p)53, is a regulator of NF-kappaB repression by the glucocorticoid receptor

Author

Samantha H. Murphy, Michael Downes, Genevieve Welch, Paul D. De Jesus, Ronald M. Evans, Sumit K. Chanda, Kotaro Suzuki, Loren Miraglia, Anthony P. Orth, and Inder M. Verma

Subjects

Lipopolysaccharides, Biology, Dexamethasone, Proinflammatory cytokine, chemistry.chemical_compound, Mice, Glucocorticoid receptor, Receptors, Glucocorticoid, medicine, Animals, Protein Interaction Maps, RNA, Messenger, RNA, Small Interfering, Psychological repression, Transcription factor, Mice, Knockout, Multidisciplinary, NF-kappa B, NF-κB, Biological Sciences, NFKB1, Shock, Septic, High-Throughput Screening Assays, Mice, Inbred C57BL, chemistry, Cancer research, RNA Interference, Signal transduction, Tumor Suppressor Protein p53, Glucocorticoid, medicine.drug, Signal Transduction

Abstract

Glucocorticoids can inhibit inflammation by abrogating the activity of NF-κB, a family of transcription factors that regulates the production of proinflammatory cytokines. To understand the molecular mechanism of repression of NF-κB activity by glucocorticoids, we performed a high-throughput siRNA oligo screen to identify novel genes involved in this process. Here, we report that loss of p53, a tumor suppressor protein, impaired repression of NF-κB target gene transcription by glucocorticoids. Additionally, loss of p53 also impaired transcription of glucocorticoid receptor (GR) target genes, whereas upstream NF-κB and glucocorticoid receptor signaling cascades remained intact. We further demonstrate that p53 loss severely impaired glucocorticoid rescue of death in a mouse model of LPS shock. Our findings unveil a new role for p53 in the repression of NF-κB by glucocorticoids and suggest important implications for treatment of the proinflammatory microenvironments found in tumors with aberrant p53 activity.

Published

2011

23. Human host factors required for influenza virus replication

Author

Trey Ideker, Shane E. Andrews, Yingyao Zhou, Qinshan Gao, Peter Palese, Yuhong Liang, H.-Heinrich Hoffmann, Mila Brum Ortigoza, Megan L. Shaw, Lars Pache, Suchita Bhattacharyya, Loren Miraglia, Ghislain M. C. Bonamy, Crystal Shih, Paul D. De Jesus, Adolfo García-Sastre, Sumit K. Chanda, Anthony P. Orth, Atsushi Inoue, Judith G. Alamares, Buu P. Tu, John A. T. Young, Donna M. Tscherne, Renate König, Silke Stertz, and Sourav Bandyopadhyay

Subjects

General Science & Technology, Orthomyxoviridae, medicine.disease_cause, Virus Replication, Virus, Article, Cell Line, Cercopithecus aethiops, 03 medical and health sciences, Biological Factors, Influenza A Virus, H1N1 Subtype, RNA interference, Viral entry, Influenza, Human, Chlorocebus aethiops, Influenza A virus, medicine, Animals, Humans, H1N1 Subtype, Vero Cells, 030304 developmental biology, Gene Library, 0303 health sciences, Multidisciplinary, Genome, biology, Genome, Human, 030302 biochemistry & molecular biology, RNA virus, Virus Internalization, biology.organism_classification, Virology, Influenza, 3. Good health, Cell biology, NS2-3 protease, Viral replication, Host-Pathogen Interactions, RNA Interference, Human

Abstract

Influenza A virus is an RNA virus that encodes up to 11 proteins and this small coding capacity demands that the virus use the host cellular machinery for many aspects of its life cycle. Knowledge of these host cell requirements not only informs us of the molecular pathways exploited by the virus but also provides further targets that could be pursued for antiviral drug development. Here we use an integrative systems approach, based on genome-wide RNA interference screening, to identify 295 cellular cofactors required for early-stage influenza virus replication. Within this group, those involved in kinase-regulated signalling, ubiquitination and phosphatase activity are the most highly enriched, and 181 factors assemble into a highly significant host-pathogen interaction network. Moreover, 219 of the 295 factors were confirmed to be required for efficient wild-type influenza virus growth, and further analysis of a subset of genes showed 23 factors necessary for viral entry, including members of the vacuolar ATPase (vATPase) and COPI-protein families, fibroblast growth factor receptor (FGFR) proteins, and glycogen synthase kinase 3 (GSK3)-beta. Furthermore, 10 proteins were confirmed to be involved in post-entry steps of influenza virus replication. These include nuclear import components, proteases, and the calcium/calmodulin-dependent protein kinase (CaM kinase) IIbeta (CAMK2B). Notably, growth of swine-origin H1N1 influenza virus is also dependent on the identified host factors, and we show that small molecule inhibitors of several factors, including vATPase and CAMK2B, antagonize influenza virus replication.

Published

2010

24. Global analysis of host-pathogen interactions that regulate early-stage HIV-1 replication

Author

Caroline E. Lilley, Ghislain M. C. Bonamy, Jeremy S. Caldwell, Yingyao Zhou, Amanda M. Opaluch, Matthew D. Weitzman, Buu P. Tu, Trey Ideker, Sourav Bandyopadhyay, Daniel Elleder, Paul D. De Jesus, Jeffrey T. Irelan, Shannon Seidel, Chih-yuan Chiang, Loren Miraglia, Frederic D. Bushman, Sumit K. Chanda, Anthony P. Orth, John A. T. Young, Kelli Kuhen, Tracy L. Diamond, and Renate König

Subjects

HUMDISEASE, HIV Infections, Biology, Virus Replication, General Biochemistry, Genetics and Molecular Biology, Article, Cell Line, Human interactome, Ubiquitin, RNA interference, Transcription (biology), Two-Hybrid System Techniques, Humans, SYSBIO, DNA synthesis, Biochemistry, Genetics and Molecular Biology(all), Proteins, Cell biology, Viral replication, RNA splicing, Host-Pathogen Interactions, biology.protein, HIV-1, CELLBIO, RNA Interference, Nuclear transport

Abstract

SummaryHuman Immunodeficiency Viruses (HIV-1 and HIV-2) rely upon host-encoded proteins to facilitate their replication. Here, we combined genome-wide siRNA analyses with interrogation of human interactome databases to assemble a host-pathogen biochemical network containing 213 confirmed host cellular factors and 11 HIV-1-encoded proteins. Protein complexes that regulate ubiquitin conjugation, proteolysis, DNA-damage response, and RNA splicing were identified as important modulators of early-stage HIV-1 infection. Additionally, over 40 new factors were shown to specifically influence the initiation and/or kinetics of HIV-1 DNA synthesis, including cytoskeletal regulatory proteins, modulators of posttranslational modification, and nucleic acid-binding proteins. Finally, 15 proteins with diverse functional roles, including nuclear transport, prostaglandin synthesis, ubiquitination, and transcription, were found to influence nuclear import or viral DNA integration. Taken together, the multiscale approach described here has uncovered multiprotein virus-host interactions that likely act in concert to facilitate the early steps of HIV-1 infection.

Published

2008

25. PQBP1 Is a Proximal Sensor of the cGAS-Dependent Innate Response to HIV-1

Author

Adolfo García-Sastre, Monika Schneider, David Germanaud, Janna Seifried, Renate König, Sumit K. Chanda, Stephen Soonthornvacharin, Elisa de Castro, Paul D. De Jesus, Rana E. Akleh, Kevin Olivieri, Vincent des Portes, Chunhai Ruan, Pedro A. Ruiz, and Sunnie M. Yoh

Subjects

Molecular Sequence Data, Biology, Article, General Biochemistry, Genetics and Molecular Biology, Cell Line, chemistry.chemical_compound, Immune system, Humans, Nuclear protein, Innate immune system, Base Sequence, Biochemistry, Genetics and Molecular Biology(all), Cerebral Palsy, Binding protein, Nuclear Proteins, biochemical phenomena, metabolism, and nutrition, Acquired immune system, Nucleotidyltransferase, Nucleotidyltransferases, Immunity, Innate, DNA-Binding Proteins, chemistry, Cell culture, DNA, Viral, Immunology, HIV-1, Mental Retardation, X-Linked, Carrier Proteins, DNA

Abstract

SummaryDendritic cells (DCs) play a critical role in the immune response to viral infection through the facilitation of cell-intrinsic antiviral activity and the activation of adaptive immunity. HIV-1 infection of DCs triggers an IRF3-dependent innate immune response, which requires the activity of cyclic GAMP synthase (cGAS). We report the results of a targeted RNAi screen utilizing primary human monocyte-derived DCs (MDDCs) to identify immune regulators that directly interface with HIV-1-encoded features to initiate this innate response. Polyglutamine binding protein 1 (PQBP1) emerged as a strong candidate through this analysis. We found that PQBP1 directly binds to reverse-transcribed HIV-1 DNA and interacts with cGAS to initiate an IRF3-dependent innate response. MDDCs derived from Renpenning syndrome patients, who harbor mutations in the PQBP1 locus, possess a severely attenuated innate immune response to HIV-1 challenge, underscoring the role of PQBP1 as a proximal innate sensor of a HIV-1 infection.