Your search keyword '"host-viral interactions"' showing total 27 results

1. The proteasome activator subunit PSME1 promotes HBV replication by inhibiting the degradation of HBV core protein

Author

Yu Liu, Jiaxin Yang, Yanyan Wang, Qiqi Zeng, Yao Fan, Ailong Huang, and Hui Fan

Subjects

26S proteasome, APEX2, HBc, HBV, Host-viral interactions, PSME1, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Chronic hepatitis B virus (HBV) infection is a leading cause of liver cirrhosis and hepatocellular carcinoma, representing a global health problem for which a functional cure is difficult to achieve. The HBV core protein (HBc) is essential for multiple steps in the viral life cycle. It is the building block of the nucleocapsid in which viral DNA reverse transcription occurs, and its mediation role in viral-host cell interactions is critical to HBV infection persistence. However, systematic studies targeting HBc-interacting proteins remain lacking. Here, we combined HBc with the APEX2 to systematically identify HBc-related host proteins in living cells. Using functional screening, we confirmed that proteasome activator subunit 1 (PSME1) is a potent HBV-associated host factor. PSME1 expression was up-regulated upon HBV infection, and the protein level of HBc decreased after PSME1 knockdown. Mechanistically, the interaction between PSME1 and HBc inhibited the degradation of HBc by the 26S proteasome, thereby improving the stability of the HBc protein. Furthermore, PSME1 silencing inhibits HBV transcription in the HBV infection system. Our findings reveal an important mechanism by which PSME1 regulates HBc proteins and may facilitate the development of new antiviral therapies targeting PSME1 function.

Published

2024

2. Hepatic proinflammatory myeloid phenotypes are a hallmark of Ebola virus Kikwit pathogenesis in rhesus monkeys.

Author

Tseng, Anna E., Carossino, Mariano, Gertje, Hans P., O'Connell, Aoife K., Gummuluru, Suryaram, Kolachalama, Vijaya B, Balasuriya, Udeni B. R., Connor, John H., Bennett, Richard S., Liu, David X., Hensley, Lisa E., and Crossland, Nicholas A.

Subjects

EBOLA virus, RHESUS monkeys, EBOLA virus disease, LIVER cells, MACAQUES, MYELOID cells, PHENOTYPES

Abstract

The liver is an early systemic target of Ebola virus (EBOV), but characterization beyond routine histopathology and viral antigen distribution is limited. We hypothesized Ebola virus disease (EVD) systemic proinflammatory responses would be reflected in temporally altered liver myeloid phenotypes. We utilized multiplex fluorescent immunohistochemistry (mfIHC), multispectral whole slide imaging, and image analysis to quantify molecular phenotypes of myeloid cells in the liver of rhesus macaques (Macaca mulatta; n = 21) infected with EBOV Kikwit. Liver samples included uninfected controls (n = 3), 3 days postinoculation (DPI; n = 3), 4 DPI (n = 3), 5 DPI (n = 3), 6 DPI (n = 3), and terminal disease (6–8 DPI; n = 6). Alterations in hepatic macrophages occurred at ≥ 5 DPI characterized by a 1.4-fold increase in CD68+ immunoreactivity and a transition from primarily CD14−CD16+ to CD14+CD16− macrophages, with a 2.1-fold decrease in CD163 expression in terminal animals compared with uninfected controls. An increase in the neutrophil chemoattractant and alarmin S100A9 occurred within hepatic myeloid cells at 5 DPI, followed by rapid neutrophil influx at ≥ 6 DPI. An acute rise in the antiviral myxovirus resistance protein 1 (MxA) occurred at ≥ 4 DPI, with a predilection for enhanced expression in uninfected cells. Distinctive expression of major histocompatibility complex (MHC) class II was observed in hepatocytes during terminal disease. Results illustrate that EBOV causes macrophage phenotype alterations as well as neutrophil influx and prominent activation of interferon host responses in the liver. Results offer insight into potential therapeutic strategies to prevent and/or modulate the host proinflammatory response to normalize hepatic myeloid functionality. [ABSTRACT FROM AUTHOR]

Published

2023

3. Host tRNA-Derived RNAs Target the 3′Untranslated Region of SARS-CoV-2.

Author

Hendrickson, Emily N., Ericson, Marna E., and Bemis, Lynne T.

Subjects

SARS-CoV-2, TRANSFER RNA, NON-coding RNA, VIRUS diseases, RNA, COVID-19 pandemic

Abstract

The COVID-19 pandemic revealed a need for new understanding of the mechanisms regulating host–pathogen interactions during viral infection. Transfer RNA-derived RNAs (tDRs), previously called transfer RNA fragments (tRFs), have recently emerged as potential regulators of viral pathogenesis. Many predictive studies using bioinformatic approaches have been conducted providing a repertoire of potential small RNA candidates for further analyses; however, few targets have been validated to directly bind to SARS-CoV-2 sequences. In this study, we used available data sets to identify host tDR expression altered in response to SARS-CoV-2 infection. RNA-interaction-prediction tools were used to identify sequences in the SARS-CoV-2 genome where tDRs could potentially bind. We then developed luciferase assays to confirm direct regulation through a predicted region of SARS-CoV-2 by tDRs. We found that two tDRs were downregulated in both clinical and in vitro cell culture studies of SARS-CoV-2 infection. Binding sites for these two tDRs were present in the 3′ untranslated region (3′UTR) of the SARS-CoV-2 reference virus and both sites were altered in Variants of Concern (VOCs) that emerged later in the pandemic. These studies directly confirm the binding of human tDRs to a specific region of the 3′UTR of SARS-CoV-2 providing evidence for a novel mechanism for host–pathogen regulation. [ABSTRACT FROM AUTHOR]

Published

2022

4. Uncovering cell-type-specific immunomodulatory variants and molecular phenotypes in COVID-19 using structurally resolved protein networks.

Author

Chhibbar P, Guha Roy P, Harioudh MK, McGrail DJ, Yang D, Singh H, Hinterleitner R, Gong YN, Yi SS, Sahni N, Sarkar SN, and Das J

Subjects

Humans, 2',5'-Oligoadenylate Synthetase metabolism, 2',5'-Oligoadenylate Synthetase genetics, Immunomodulation, Signal Transduction, COVID-19 immunology, COVID-19 virology, COVID-19 genetics, SARS-CoV-2 genetics, SARS-CoV-2 immunology, SARS-CoV-2 metabolism, Phenotype, Protein Interaction Maps

Abstract

Immunomodulatory variants that lead to the loss or gain of specific protein interactions often manifest only as organismal phenotypes in infectious disease. Here, we propose a network-based approach to integrate genetic variation with a structurally resolved human protein interactome network to prioritize immunomodulatory variants in COVID-19. We find that, in addition to variants that pass genome-wide significance thresholds, variants at the interface of specific protein-protein interactions, even though they do not meet genome-wide thresholds, are equally immunomodulatory. The integration of these variants with single-cell epigenomic and transcriptomic data prioritizes myeloid and T cell subsets as the most affected by these variants across both the peripheral blood and the lung compartments. Of particular interest is a common coding variant that disrupts the OAS1-PRMT6 interaction and affects downstream interferon signaling. Critically, our framework is generalizable across infectious disease contexts and can be used to implicate immunomodulatory variants that do not meet genome-wide significance thresholds., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2024 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2024

5. Host tRNA-Derived RNAs Target the 3′Untranslated Region of SARS-CoV-2

Author

Emily N. Hendrickson, Marna E. Ericson, and Lynne T. Bemis

Subjects

tRNA fragments, tRF, tRNA-derived RNAs, tDR, small noncoding RNA, host-viral interactions, Medicine

Abstract

The COVID-19 pandemic revealed a need for new understanding of the mechanisms regulating host–pathogen interactions during viral infection. Transfer RNA-derived RNAs (tDRs), previously called transfer RNA fragments (tRFs), have recently emerged as potential regulators of viral pathogenesis. Many predictive studies using bioinformatic approaches have been conducted providing a repertoire of potential small RNA candidates for further analyses; however, few targets have been validated to directly bind to SARS-CoV-2 sequences. In this study, we used available data sets to identify host tDR expression altered in response to SARS-CoV-2 infection. RNA-interaction-prediction tools were used to identify sequences in the SARS-CoV-2 genome where tDRs could potentially bind. We then developed luciferase assays to confirm direct regulation through a predicted region of SARS-CoV-2 by tDRs. We found that two tDRs were downregulated in both clinical and in vitro cell culture studies of SARS-CoV-2 infection. Binding sites for these two tDRs were present in the 3′ untranslated region (3′UTR) of the SARS-CoV-2 reference virus and both sites were altered in Variants of Concern (VOCs) that emerged later in the pandemic. These studies directly confirm the binding of human tDRs to a specific region of the 3′UTR of SARS-CoV-2 providing evidence for a novel mechanism for host–pathogen regulation.

Published

2022

6. Cross-Reactivity to Mutated Viral Immune Targets Can Influence CD8+ T Cell Functionality: An Alternative Viral Adaptation Strategy

Author

Jennifer Currenti, Becker M.P. Law, Kai Qin, Mina John, Mark A. Pilkinton, Anju Bansal, Shay Leary, Ramesh Ram, Abha Chopra, Rama Gangula, Ling Yue, Christian Warren, Louise Barnett, Eric Alves, Wyatt J. McDonnell, Anuradha Sooda, Sonya L. Heath, Simon Mallal, Paul Goepfert, Spyros A. Kalams, and Silvana Gaudieri

Subjects

HIV, adaptation, host-viral interactions, T cell receptor, transcriptome, Immunologic diseases. Allergy, RC581-607

Abstract

Loss of T cell immunogenicity due to mutations in virally encoded epitopes is a well-described adaptation strategy to limit host anti-viral immunity. Another described, but less understood, adaptation strategy involves the selection of mutations within epitopes that retain immune recognition, suggesting a benefit for the virus despite continued immune pressure (termed non-classical adaptation). To understand this adaptation strategy, we utilized a single cell transcriptomic approach to identify features of the HIV-specific CD8+ T cell responses targeting non-adapted (NAE) and adapted (AE) forms of epitopes containing a non-classical adaptation. T cell receptor (TCR) repertoire and transcriptome were obtained from antigen-specific CD8+ T cells of chronic (n=7) and acute (n=4) HIV-infected subjects identified by either HLA class I tetramers or upregulation of activation markers following peptide stimulation. CD8+ T cells were predominantly dual tetramer+, confirming a large proportion of cross-reactive TCR clonotypes capable of recognizing the NAE and AE form. However, single-reactive CD8+ T cells were identified in acute HIV-infected subjects only, providing the potential for the selection of T cell clones over time. The transcriptomic profile of CD8+ T cells was dependent on the autologous virus: subjects whose virus encoded the NAE form of the epitope (and who transitioned to the AE form at a later timepoint) exhibited an ‘effective’ immune response, as indicated by expression of transcripts associated with polyfunctionality, cytotoxicity and apoptosis (largely driven by the genes GZMB, IFNɣ, CCL3, CCL4 and CCL5). These data suggest that viral adaptation at a single amino acid residue can provide an alternative strategy for viral survival by modulating the transcriptome of CD8+ T cells and potentially selecting for less effective T cell clones from the acute to chronic phase.

Published

2021

7. Cross-Reactivity to Mutated Viral Immune Targets Can Influence CD8+ T Cell Functionality: An Alternative Viral Adaptation Strategy.

Author

Currenti, Jennifer, Law, Becker M.P., Qin, Kai, John, Mina, Pilkinton, Mark A., Bansal, Anju, Leary, Shay, Ram, Ramesh, Chopra, Abha, Gangula, Rama, Yue, Ling, Warren, Christian, Barnett, Louise, Alves, Eric, McDonnell, Wyatt J., Sooda, Anuradha, Heath, Sonya L., Mallal, Simon, Goepfert, Paul, and Kalams, Spyros A.

Subjects

T cells, T cell receptors, AMINO acid residues, CROSS reactions (Immunology), IMMUNE recognition

Abstract

Loss of T cell immunogenicity due to mutations in virally encoded epitopes is a well-described adaptation strategy to limit host anti-viral immunity. Another described, but less understood, adaptation strategy involves the selection of mutations within epitopes that retain immune recognition, suggesting a benefit for the virus despite continued immune pressure (termed non-classical adaptation). To understand this adaptation strategy, we utilized a single cell transcriptomic approach to identify features of the HIV-specific CD8+ T cell responses targeting non-adapted (NAE) and adapted (AE) forms of epitopes containing a non-classical adaptation. T cell receptor (TCR) repertoire and transcriptome were obtained from antigen-specific CD8+ T cells of chronic (n=7) and acute (n=4) HIV-infected subjects identified by either HLA class I tetramers or upregulation of activation markers following peptide stimulation. CD8+ T cells were predominantly dual tetramer+, confirming a large proportion of cross-reactive TCR clonotypes capable of recognizing the NAE and AE form. However, single-reactive CD8+ T cells were identified in acute HIV-infected subjects only, providing the potential for the selection of T cell clones over time. The transcriptomic profile of CD8+ T cells was dependent on the autologous virus: subjects whose virus encoded the NAE form of the epitope (and who transitioned to the AE form at a later timepoint) exhibited an 'effective' immune response, as indicated by expression of transcripts associated with polyfunctionality, cytotoxicity and apoptosis (largely driven by the genes GZMB, IFNɣ, CCL3, CCL4 and CCL5). These data suggest that viral adaptation at a single amino acid residue can provide an alternative strategy for viral survival by modulating the transcriptome of CD8+ T cells and potentially selecting for less effective T cell clones from the acute to chronic phase. [ABSTRACT FROM AUTHOR]

Published

2021

8. Epigenetic susceptibility to severe respiratory viral infections and its therapeutic implications: a narrative review.

Author

Crimi, Ettore, Benincasa, Giuditta, Figueroa-Marrero, Neisaliz, Galdiero, Massimiliano, and Napoli, Claudio

Subjects

*VIRUS diseases, *RESPIRATORY infections, *INFLUENZA A virus, H5N1 subtype, *COVID-19, *DNA, *RNA, *INFLUENZA treatment, *CORONAVIRUS disease treatment, *VIRAL pneumonia, *DISEASE susceptibility, *GENES, *INFLUENZA, *EPIDEMICS, RESPIRATORY infection treatment

Abstract

The emergence of highly pathogenic strains of influenza virus and coronavirus (CoV) has been responsible for large epidemic and pandemic outbreaks characterised by severe pulmonary illness associated with high morbidity and mortality. One major challenge for critical care is to stratify and minimise the risk of multi-organ failure during the stay in the intensive care unit (ICU). Epigenetic-sensitive mechanisms, including deoxyribonucleic acid (DNA) and ribonucleic acid (RNA) methylation, histone modifications, and non-coding RNAs may lead to perturbations of the host immune-related transcriptional programmes by regulating chromatin structure and gene expression patterns. Viruses causing severe pulmonary illness can use epigenetic-regulated mechanisms during host-pathogen interaction to interfere with innate and adaptive immunity, adequacy of inflammatory response, and overall outcome of viral infections. For example, Middle East respiratory syndrome-CoV and H5N1 can affect host antigen presentation through DNA methylation and histone modifications. The same mechanisms would presumably occur in patients with coronavirus disease 2019, in which tocilizumab may epigenetically reduce microvascular damage. Targeting epigenetic pathways by immune modulators (e.g. tocilizumab) or repurposed drugs (e.g. statins) may provide novel therapeutic opportunities to control viral-host interaction during critical illness. In this review, we provide an update on epigenetic-sensitive mechanisms and repurposed drugs interfering with epigenetic pathways which may be clinically suitable for risk stratification and beneficial for treatment of patients affected by severe viral respiratory infections. [ABSTRACT FROM AUTHOR]

Published

2020

9. The Viral Capsid: A Master Key to Access the Host Nucleus

Author

Guillermo Blanco-Rodriguez and Francesca Di Nunzio

Subjects

viral nuclear entry, viral replication, host–viral interactions, Microbiology, QR1-502

Abstract

Viruses are pathogens that have evolved to hijack the cellular machinery to replicate themselves and spread to new cells. During the course of evolution, viruses developed different strategies to overcome the cellular defenses and create new progeny. Among them, some RNA and many DNA viruses require access to the nucleus to replicate their genome. In non-dividing cells, viruses can only access the nucleus through the nuclear pore complex (NPC). Therefore, viruses have developed strategies to usurp the nuclear transport machinery and gain access to the nucleus. The majority of these viruses use the capsid to manipulate the nuclear import machinery. However, the particular tactics employed by each virus to reach the host chromatin compartment are very different. Nevertheless, they all require some degree of capsid remodeling. Recent notions on the interplay between the viral capsid and cellular factors shine new light on the quest for the nuclear entry step and for the fate of these viruses. In this review, we describe the main components and function of nuclear transport machinery. Next, we discuss selected examples of RNA and DNA viruses (HBV, HSV, adenovirus, and HIV) that remodel their capsid as part of their strategies to access the nucleus and to replicate.

Published

2021

10. Host Transcription Factors in Hepatitis B Virus RNA Synthesis

Author

Kristi L. Turton, Vanessa Meier-Stephenson, Maulik D. Badmalia, Carla S. Coffin, and Trushar R. Patel

Subjects

hepatitis b virus (hbv), viral replication, transcription factors, covalently closed circular dna (cccdna), host–viral interactions, Microbiology, QR1-502

Abstract

The hepatitis B virus (HBV) chronically infects over 250 million people worldwide and is one of the leading causes of liver cancer and hepatocellular carcinoma. HBV persistence is due in part to the highly stable HBV minichromosome or HBV covalently closed circular DNA (cccDNA) that resides in the nucleus. As HBV replication requires the help of host transcription factors to replicate, focusing on host protein−HBV genome interactions may reveal insights into new drug targets against cccDNA. The structural details on such complexes, however, remain poorly defined. In this review, the current literature regarding host transcription factors’ interactions with HBV cccDNA is discussed.

Published

2020

11. The proteasome activator subunit PSME1 promotes HBV replication by inhibiting the degradation of HBV core protein.

Author

Liu Y, Yang J, Wang Y, Zeng Q, Fan Y, Huang A, and Fan H

Abstract

Chronic hepatitis B virus (HBV) infection is a leading cause of liver cirrhosis and hepatocellular carcinoma, representing a global health problem for which a functional cure is difficult to achieve. The HBV core protein (HBc) is essential for multiple steps in the viral life cycle. It is the building block of the nucleocapsid in which viral DNA reverse transcription occurs, and its mediation role in viral-host cell interactions is critical to HBV infection persistence. However, systematic studies targeting HBc-interacting proteins remain lacking. Here, we combined HBc with the APEX2 to systematically identify HBc-related host proteins in living cells. Using functional screening, we confirmed that proteasome activator subunit 1 (PSME1) is a potent HBV-associated host factor. PSME1 expression was up-regulated upon HBV infection, and the protein level of HBc decreased after PSME1 knockdown. Mechanistically, the interaction between PSME1 and HBc inhibited the degradation of HBc by the 26S proteasome, thereby improving the stability of the HBc protein. Furthermore, PSME1 silencing inhibits HBV transcription in the HBV infection system. Our findings reveal an important mechanism by which PSME1 regulates HBc proteins and may facilitate the development of new antiviral therapies targeting PSME1 function., (© 2023 The Authors. Publishing services by Elsevier B.V. on behalf of KeAi Communications Co., Ltd.)

Published

2023

12. Epigenetic susceptibility to severe respiratory viral infections and its therapeutic implications: a narrative review

Author

Massimiliano Galdiero, Giuditta Benincasa, Ettore Crimi, Neisaliz Figueroa-Marrero, Claudio Napoli, Crimi, E., Benincasa, G., Figueroa-Marrero, N., Galdiero, M., and Napoli, C.

Subjects

influenza viru, Pneumonia, Viral, coronavirus, severe acute respiratory syndrome, medicine.disease_cause, Article, influenza virus, Virus, Epigenesis, Genetic, Betacoronavirus, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Tocilizumab, 030202 anesthesiology, Intensive care, Influenza, Human, medicine, Humans, Genetic Predisposition to Disease, Epigenetics, Pandemics, Respiratory Tract Infections, epigenetic drug, intensive care, Coronavirus, epigenetics, SARS-CoV-2, business.industry, COVID-19, epigenetic drugs, host–viral interactions, Acquired immune system, Chromatin, coronaviru, Anesthesiology and Pain Medicine, chemistry, DNA methylation, Immunology, host–viral interaction, Coronavirus Infections, business, epigenetic

Abstract

Summary The emergence of highly pathogenic strains of influenza virus and coronavirus (CoV) has been responsible for large epidemic and pandemic outbreaks characterised by severe pulmonary illness associated with high morbidity and mortality. One major challenge for critical care is to stratify and minimise the risk of multi-organ failure during the stay in the intensive care unit (ICU). Epigenetic-sensitive mechanisms, including deoxyribonucleic acid (DNA) and ribonucleic acid (RNA) methylation, histone modifications, and non-coding RNAs may lead to perturbations of the host immune-related transcriptional programmes by regulating chromatin structure and gene expression patterns. Viruses causing severe pulmonary illness can use epigenetic-regulated mechanisms during host–pathogen interaction to interfere with innate and adaptive immunity, adequacy of inflammatory response, and overall outcome of viral infections. For example, Middle East respiratory syndrome-CoV and H5N1 can affect host antigen presentation through DNA methylation and histone modifications. The same mechanisms would presumably occur in patients with coronavirus disease 2019, in which tocilizumab may epigenetically reduce microvascular damage. Targeting epigenetic pathways by immune modulators (e.g. tocilizumab) or repurposed drugs (e.g. statins) may provide novel therapeutic opportunities to control viral–host interaction during critical illness. In this article, we provide an update on epigenetic-sensitive mechanisms and repurposed drugs interfering with epigenetic pathways which may be clinically suitable for risk stratification and beneficial for treatment of patients affected by severe viral respiratory infections.

Published

2020

13. Human DDX17 Unwinds Rift Valley Fever Virus Non-Coding RNAs

Author

Corey R. Nelson, Hans-Joachim Wieden, Tyler Mrozowich, Raymond J. Owens, Justin R.J. Vigar, Borries Demeler, Sean M. Park, Simmone D'souza, Trushar R. Patel, and Amy Henrickson

Subjects

0301 basic medicine, Models, Molecular, RNA, Untranslated, Rift Valley Fever, Protein Conformation, viruses, Genome, DEAD-box RNA Helicases, lcsh:Chemistry, Intergenic region, Adenosine Triphosphate, analytical ultracentrifuge, helicase assay, lcsh:QH301-705.5, Spectroscopy, biology, RNA-Binding Proteins, General Medicine, RNA Helicase A, 3. Good health, Computer Science Applications, Host-Pathogen Interactions, helicase DDX17, RNA, Viral, Bunyaviridae, Protein Binding, small angle X-ray scattering, Catalysis, Virus, Article, Inorganic Chemistry, 03 medical and health sciences, Structure-Activity Relationship, Animals, Humans, Protein Interaction Domains and Motifs, Physical and Theoretical Chemistry, Molecular Biology, 030102 biochemistry & molecular biology, Oligonucleotide, Microscale thermophoresis, Organic Chemistry, Helicase, fluorescent labeling, host–viral interactions, biology.organism_classification, Rift Valley fever virus, Virology, microscale thermophoresis, 030104 developmental biology, Rift Valley fever virus RNA, lcsh:Biology (General), lcsh:QD1-999, biology.protein

Abstract

Rift Valley fever virus (RVFV) is a mosquito-transmitted virus from the Bunyaviridae family that causes high rates of mortality and morbidity in humans and ruminant animals. Previous studies indicated that DEAD-box helicase 17 (DDX17) restricts RVFV replication by recognizing two primary non-coding RNAs in the S-segment of the genome: the intergenic region (IGR) and 5&prime, non-coding region (NCR). However, we lack molecular insights into the direct binding of DDX17 with RVFV non-coding RNAs and information on the unwinding of both non-coding RNAs by DDX17. Therefore, we performed an extensive biophysical analysis of the DDX17 helicase domain (DDX17135&ndash, 555) and RVFV non-coding RNAs, IGR and 5&rsquo, NCR. The homogeneity studies using analytical ultracentrifugation indicated that DDX17135&ndash, 555, IGR, and 5&rsquo, NCR are pure. Next, we performed small-angle X-ray scattering (SAXS) experiments, which suggested that DDX17 and both RNAs are homogenous as well. SAXS analysis also demonstrated that DDX17 is globular to an extent, whereas the RNAs adopt an extended conformation in solution. Subsequently, microscale thermophoresis (MST) experiments were performed to investigate the direct binding of DDX17 to the non-coding RNAs. The MST experiments demonstrated that DDX17 binds with the IGR and 5&rsquo, NCR with a dissociation constant of 5.77 &plusmn, 0.15 &micro, M and 9.85 &plusmn, 0.11 &micro, M, respectively. As DDX17135&ndash, 555 is an RNA helicase, we next determined if it could unwind IGR and NCR. We developed a helicase assay using MST and fluorescently-labeled oligos, which suggested DDX17135&ndash, 555 can unwind both RNAs. Overall, our study provides direct evidence of DDX17135&ndash, 555 interacting with and unwinding RVFV non-coding regions.

Published

2021

14. Cross-Reactivity to Mutated Viral Immune Targets Can Influence CD8+ T Cell Functionality: An Alternative Viral Adaptation Strategy

Author

Kai Qin, Wyatt J. McDonnell, Christian M Warren, Mina John, Abha Chopra, Simon Mallal, Silvana Gaudieri, Ling Yue, Rama Gangula, Becker M.P. Law, Shay Leary, Ramesh Ram, Mark A. Pilkinton, Paul A. Goepfert, Spyros A. Kalams, Louise Barnett, Jennifer Currenti, Anuradha Sooda, Sonya L. Heath, Anju Bansal, and Eric Alves

Subjects

T cell, Immunology, T-cell receptor, HIV, adaptation, Human leukocyte antigen, RC581-607, Biology, CCL5, Epitope, Cell biology, medicine.anatomical_structure, Immune system, medicine, Immunology and Allergy, Cytotoxic T cell, host-viral interactions, T cell receptor, Immunologic diseases. Allergy, transcriptome, CD8

Abstract

Loss of T cell immunogenicity due to mutations in virally encoded epitopes is a well-described adaptation strategy to limit host anti-viral immunity. Another described, but less understood, adaptation strategy involves the selection of mutations within epitopes that retain immune recognition, suggesting a benefit for the virus despite continued immune pressure (termed non-classical adaptation). To understand this adaptation strategy, we utilized a single cell transcriptomic approach to identify features of the HIV-specific CD8+ T cell responses targeting non-adapted (NAE) and adapted (AE) forms of epitopes containing a non-classical adaptation. T cell receptor (TCR) repertoire and transcriptome were obtained from antigen-specific CD8+ T cells of chronic (n=7) and acute (n=4) HIV-infected subjects identified by either HLA class I tetramers or upregulation of activation markers following peptide stimulation. CD8+ T cells were predominantly dual tetramer+, confirming a large proportion of cross-reactive TCR clonotypes capable of recognizing the NAE and AE form. However, single-reactive CD8+ T cells were identified in acute HIV-infected subjects only, providing the potential for the selection of T cell clones over time. The transcriptomic profile of CD8+ T cells was dependent on the autologous virus: subjects whose virus encoded the NAE form of the epitope (and who transitioned to the AE form at a later timepoint) exhibited an ‘effective’ immune response, as indicated by expression of transcripts associated with polyfunctionality, cytotoxicity and apoptosis (largely driven by the genes GZMB, IFNɣ, CCL3, CCL4 and CCL5). These data suggest that viral adaptation at a single amino acid residue can provide an alternative strategy for viral survival by modulating the transcriptome of CD8+ T cells and potentially selecting for less effective T cell clones from the acute to chronic phase.

Published

2021

15. Human DDX3X unwinds Japanese encephalitis and Zika viral 5' terminal regions

Author

Nelson, Corey R., Mrozowich, Tyler, Gemmill, Darren L., Park, Sean M., Patel, Trushar R., Nelson, Corey R., Mrozowich, Tyler, Gemmill, Darren L., Park, Sean M., and Patel, Trushar R.

Abstract

Flavivirus genus includes many deadly viruses such as the Japanese encephalitis virus (JEV) and Zika virus (ZIKV). The 5′ terminal regions (TR) of flaviviruses interact with human proteins and such interactions are critical for viral replication. One of the human proteins identified to interact with the 5′ TR of JEV is the DEAD-box helicase, DDX3X. In this study, we in vitro transcribed the 5′ TR of JEV and demonstrated its direct interaction with recombinant DDX3X (Kd of 1.66 ± 0.21 µM) using microscale thermophoresis (MST). Due to the proposed structural similarities of 5′ and 3′ TRs of flaviviruses, we investigated if the ZIKV 5′ TR could also interact with human DDX3X. Our MST studies suggested that DDX3X recognizes ZIKV 5′ TR with a Kd of 7.05 ± 0.75 µM. Next, we performed helicase assays that suggested that the binding of DDX3X leads to the unwinding of JEV and ZIKV 5′ TRs. Overall, our data indicate, for the first time, that DDX3X can directly bind and unwind in vitro transcribed flaviviral TRs. In summary, our work indicates that DDX3X could be further explored as a therapeutic target to inhibit Flaviviral replication

Published

2021

16. The Viral Capsid: A Master Key to Access the Host Nucleus

Author

Francesca Di Nunzio, Guillermo Blanco-Rodriguez, Département de Virologie - Department of Virology, Institut Pasteur [Paris], Immunité et cancer (U932), Institut Curie [Paris]-Institut National de la Santé et de la Recherche Médicale (INSERM), This research was funded by Agence Nationale de Recherches sur le Sida et les Hépatites Virales (ANRS), grant number ECTZ88162., We thank Alex Evilevitch, Yu Wei, and Maryline Bourgine for critically reading the session of the manuscript on HBV and HSV., Institut Pasteur [Paris] (IP), and Di Nunzio, Francesca

Subjects

0301 basic medicine, [SDV]Life Sciences [q-bio], viruses, Active Transport, Cell Nucleus, Review, Biology, Virus Replication, Genome, Microbiology, Virus, 03 medical and health sciences, Capsid, Virology, Humans, Nuclear pore, [SDV.MP.VIR] Life Sciences [q-bio]/Microbiology and Parasitology/Virology, Cell Nucleus, 030102 biochemistry & molecular biology, Host Microbial Interactions, Virion, RNA, viral nuclear entry, host–viral interactions, QR1-502, Chromatin, Cell biology, [SDV] Life Sciences [q-bio], 030104 developmental biology, Infectious Diseases, Viral replication, [SDV.MP.VIR]Life Sciences [q-bio]/Microbiology and Parasitology/Virology, Viruses, Nuclear Pore, viral replication, Nuclear transport, Virus Physiological Phenomena

Abstract

International audience; Viruses are pathogens that have evolved to hijack the cellular machinery to replicate themselves and spread to new cells. During the course of evolution, viruses developed different strategies to overcome the cellular defenses and create new progeny. Among them, some RNA and many DNA viruses require access to the nucleus to replicate their genome. In non-dividing cells, viruses can only access the nucleus through the nuclear pore complex (NPC). Therefore, viruses have developed strategies to usurp the nuclear transport machinery and gain access to the nucleus. The majority of these viruses use the capsid to manipulate the nuclear import machinery. However, the particular tactics employed by each virus to reach the host chromatin compartment are very different. Nevertheless, they all require some degree of capsid remodeling. Recent notions on the interplay between the viral capsid and cellular factors shine new light on the quest for the nuclear entry step and for the fate of these viruses. In this review, we describe the main components and function of nuclear transport machinery. Next, we discuss selected examples of RNA and DNA viruses (HBV, HSV, adenovirus, and HIV) that remodel their capsid as part of their strategies to access the nucleus and to replicate.

Published

2021

17. Human DDX3X Unwinds Japanese Encephalitis and Zika Viral 5′ Terminal Regions

Author

Corey R. Nelson, Trushar R. Patel, Darren L. Gemmill, Sean M. Park, and Tyler Mrozowich

Subjects

viruses, Gene Expression, Virus Replication, law.invention, Zika virus, DEAD-box RNA Helicases, lcsh:Chemistry, 0302 clinical medicine, law, lcsh:QH301-705.5, Spectroscopy, Encephalitis Virus, Japanese, 0303 health sciences, biology, virus diseases, General Medicine, Up-Regulation, 3. Good health, Computer Science Applications, Flavivirus, viral terminal regions, RNA helicase assays, Recombinant DNA, DDX3X, Article, Catalysis, Virus, Inorganic Chemistry, 03 medical and health sciences, Protein Domains, medicine, Humans, Physical and Theoretical Chemistry, Molecular Biology, 030304 developmental biology, Host Microbial Interactions, Microscale thermophoresis, Organic Chemistry, Helicase, host–viral interactions, biochemical phenomena, metabolism, and nutrition, Japanese encephalitis, medicine.disease, biology.organism_classification, microscale thermophoresis, Virology, Japanese encephalitis virus, Viral replication, lcsh:Biology (General), lcsh:QD1-999, biology.protein, 5' Untranslated Regions, in vitro transcription, 030217 neurology & neurosurgery

Abstract

Flavivirus genus includes many deadly viruses such as the Japanese encephalitis virus (JEV) and Zika virus (ZIKV). The 5&prime, terminal regions (TR) of flaviviruses interact with human proteins and such interactions are critical for viral replication. One of the human proteins identified to interact with the 5&prime, TR of JEV is the DEAD-box helicase, DDX3X. In this study, we in vitro transcribed the 5&prime, TR of JEV and demonstrated its direct interaction with recombinant DDX3X (Kd of 1.66 &plusmn, 0.21 &micro, M) using microscale thermophoresis (MST). Due to the proposed structural similarities of 5&prime, and 3&prime, TRs of flaviviruses, we investigated if the ZIKV 5&prime, TR could also interact with human DDX3X. Our MST studies suggested that DDX3X recognizes ZIKV 5&prime, TR with a Kd of 7.05 &plusmn, 0.75 &micro, M. Next, we performed helicase assays that suggested that the binding of DDX3X leads to the unwinding of JEV and ZIKV 5&prime, TRs. Overall, our data indicate, for the first time, that DDX3X can directly bind and unwind in vitro transcribed flaviviral TRs. In summary, our work indicates that DDX3X could be further explored as a therapeutic target to inhibit Flaviviral replication

Published

2021

18. Human DDX17 unwinds Rift Valley fever virus non-coding RNAs

Author

Nelson, Corey R., Mrozowich, Tyler, Park, Sean M., D'souza, Simmone, Henrickson, Amy, Vigar, Justin R. J., Wieden, Hans-Joachim, Owens, Raymond J., Demeler, Borries, Patel, Trushar R., Nelson, Corey R., Mrozowich, Tyler, Park, Sean M., D'souza, Simmone, Henrickson, Amy, Vigar, Justin R. J., Wieden, Hans-Joachim, Owens, Raymond J., Demeler, Borries, and Patel, Trushar R.

Abstract

Rift Valley fever virus (RVFV) is a mosquito-transmitted virus from the Bunyaviridae family that causes high rates of mortality and morbidity in humans and ruminant animals. Previous studies indicated that DEAD-box helicase 17 (DDX17) restricts RVFV replication by recognizing two primary non-coding RNAs in the S-segment of the genome: the intergenic region (IGR) and 5′ non-coding region (NCR). However, we lack molecular insights into the direct binding of DDX17 with RVFV non-coding RNAs and information on the unwinding of both non-coding RNAs by DDX17. Therefore, we performed an extensive biophysical analysis of the DDX17 helicase domain (DDX17135–555) and RVFV non-coding RNAs, IGR and 5’ NCR. The homogeneity studies using analytical ultracentrifugation indicated that DDX17135–555, IGR, and 5’ NCR are pure. Next, we performed small-angle X-ray scattering (SAXS) experiments, which suggested that DDX17 and both RNAs are homogenous as well. SAXS analysis also demonstrated that DDX17 is globular to an extent, whereas the RNAs adopt an extended conformation in solution. Subsequently, microscale thermophoresis (MST) experiments were performed to investigate the direct binding of DDX17 to the non-coding RNAs. The MST experiments demonstrated that DDX17 binds with the IGR and 5’ NCR with a dissociation constant of 5.77 ± 0.15 µM and 9.85 ± 0.11 µM, respectively. As DDX17135–555 is an RNA helicase, we next determined if it could unwind IGR and NCR. We developed a helicase assay using MST and fluorescently-labeled oligos, which suggested DDX17135–555 can unwind both RNAs. Overall, our study provides direct evidence of DDX17135–555 interacting with and unwinding RVFV non-coding regions

Published

2020

19. Host transcription factors in hepatitis B virus RNA synthesis

Author

Turton, Kristi L., Meier-Stephenson, Vanessa, Badmalia, Maulik D., Coffin, Carla S., Patel, Trushar R., Turton, Kristi L., Meier-Stephenson, Vanessa, Badmalia, Maulik D., Coffin, Carla S., and Patel, Trushar R.

Abstract

The hepatitis B virus (HBV) chronically infects over 250 million people worldwide and is one of the leading causes of liver cancer and hepatocellular carcinoma. HBV persistence is due in part to the highly stable HBV minichromosome or HBV covalently closed circular DNA (cccDNA) that resides in the nucleus. As HBV replication requires the help of host transcription factors to replicate, focusing on host protein–HBV genome interactions may reveal insights into new drug targets against cccDNA. The structural details on such complexes, however, remain poorly defined. In this review, the current literature regarding host transcription factors’ interactions with HBV cccDNA is discussed.

Published

2020

20. Use of viral motif mimicry improves the proteome-wide discovery of human linear motifs.

Author

Wadie B, Kleshchevnikov V, Sandaltzopoulou E, Benz C, and Petsalaki E

Subjects

Amino Acid Motifs, Humans, Viral Proteins metabolism, Evolution, Molecular, Proteome genetics

Abstract

Linear motifs have an integral role in dynamic cell functions, including cell signaling. However, due to their small size, low complexity, and frequent mutations, identifying novel functional motifs poses a challenge. Viruses rely extensively on the molecular mimicry of cellular linear motifs. In this study, we apply systematic motif prediction combined with functional filters to identify human linear motifs convergently evolved also in viral proteins. We observe an increase in the sensitivity of motif prediction and improved enrichment in known instances. We identify >7,300 non-redundant motif instances at various confidence levels, 99 of which are supported by all functional and structural filters. Overall, we provide a pipeline to improve the identification of functional linear motifs from interactomics datasets and a comprehensive catalog of putative human motifs that can contribute to our understanding of the human domain-linear motif code and the associated mechanisms of viral interference., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2022 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2022

21. The Viral Capsid: A Master Key to Access the Host Nucleus.

Author

Blanco-Rodriguez, Guillermo and Di Nunzio, Francesca

Subjects

*DNA viruses, *RNA viruses, *HERPES simplex virus, *NUCLEAR warfare, *ADENOVIRUSES

Abstract

Viruses are pathogens that have evolved to hijack the cellular machinery to replicate themselves and spread to new cells. During the course of evolution, viruses developed different strategies to overcome the cellular defenses and create new progeny. Among them, some RNA and many DNA viruses require access to the nucleus to replicate their genome. In non-dividing cells, viruses can only access the nucleus through the nuclear pore complex (NPC). Therefore, viruses have developed strategies to usurp the nuclear transport machinery and gain access to the nucleus. The majority of these viruses use the capsid to manipulate the nuclear import machinery. However, the particular tactics employed by each virus to reach the host chromatin compartment are very different. Nevertheless, they all require some degree of capsid remodeling. Recent notions on the interplay between the viral capsid and cellular factors shine new light on the quest for the nuclear entry step and for the fate of these viruses. In this review, we describe the main components and function of nuclear transport machinery. Next, we discuss selected examples of RNA and DNA viruses (HBV, HSV, adenovirus, and HIV) that remodel their capsid as part of their strategies to access the nucleus and to replicate. [ABSTRACT FROM AUTHOR]

Published

2021

22. Cross-Reactivity to Mutated Viral Immune Targets Can Influence CD8 + T Cell Functionality: An Alternative Viral Adaptation Strategy.

Author

Currenti J, Law BMP, Qin K, John M, Pilkinton MA, Bansal A, Leary S, Ram R, Chopra A, Gangula R, Yue L, Warren C, Barnett L, Alves E, McDonnell WJ, Sooda A, Heath SL, Mallal S, Goepfert P, Kalams SA, and Gaudieri S

Subjects

Adult, Cross Reactions immunology, Epitopes, T-Lymphocyte immunology, Female, Humans, Male, Middle Aged, Adaptation, Physiological immunology, CD8-Positive T-Lymphocytes immunology, HIV immunology, HIV Infections immunology

Abstract

Loss of T cell immunogenicity due to mutations in virally encoded epitopes is a well-described adaptation strategy to limit host anti-viral immunity. Another described, but less understood, adaptation strategy involves the selection of mutations within epitopes that retain immune recognition, suggesting a benefit for the virus despite continued immune pressure (termed non-classical adaptation). To understand this adaptation strategy, we utilized a single cell transcriptomic approach to identify features of the HIV-specific CD8 + T cell responses targeting non-adapted (NAE) and adapted (AE) forms of epitopes containing a non-classical adaptation. T cell receptor (TCR) repertoire and transcriptome were obtained from antigen-specific CD8 + T cells of chronic (n=7) and acute (n=4) HIV-infected subjects identified by either HLA class I tetramers or upregulation of activation markers following peptide stimulation. CD8 + T cells were predominantly dual tetramer + , confirming a large proportion of cross-reactive TCR clonotypes capable of recognizing the NAE and AE form. However, single-reactive CD8 + T cells were identified in acute HIV-infected subjects only, providing the potential for the selection of T cell clones over time. The transcriptomic profile of CD8 + T cells was dependent on the autologous virus: subjects whose virus encoded the NAE form of the epitope (and who transitioned to the AE form at a later timepoint) exhibited an 'effective' immune response, as indicated by expression of transcripts associated with polyfunctionality, cytotoxicity and apoptosis (largely driven by the genes GZMB, IFNɣ, CCL3, CCL4 and CCL5). These data suggest that viral adaptation at a single amino acid residue can provide an alternative strategy for viral survival by modulating the transcriptome of CD8 + T cells and potentially selecting for less effective T cell clones from the acute to chronic phase., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Currenti, Law, Qin, John, Pilkinton, Bansal, Leary, Ram, Chopra, Gangula, Yue, Warren, Barnett, Alves, McDonnell, Sooda, Heath, Mallal, Goepfert, Kalams and Gaudieri.)

Published

2021

23. Antiviral Immune Response and the Route of Infection in Drosophila melanogaster

Author

Maria-Carla Saleh, Juan A Mondotte, Virus et Interférence ARN - Viruses and RNA Interference, Institut Pasteur [Paris] (IP)-Centre National de la Recherche Scientifique (CNRS), This work was supported by the European Research Council (FP7/2013-2019 ERC CoG 615220) and the French Government's Investissement d’Avenir program, Laboratoire d’Excellence Integrative Biology of Emerging Infectious Diseases (Grant ANR-10-LABX-62-IBEID) to M.C.S. J.A.M. was supported by AXA Research fund., We apologize to all of our colleagues whose work has not been cited due to space constraints. We thank Vanesa Mongelli and Elizabeth Jaworski for fruitful discussions and help with editing. Chloé Baron for artwork, ANR-10-LABX-0062,IBEID,Integrative Biology of Emerging Infectious Diseases(2010), European Project: 615220,EC:FP7:ERC,ERC-2013-CoG,RNAIMMUNITY(2015), and Institut Pasteur [Paris]-Centre National de la Recherche Scientifique (CNRS)

Subjects

0301 basic medicine, MESH: Signal Transduction, MESH: Drosophila Proteins, 030106 microbiology, ved/biology.organism_classification_rank.species, MESH: RNA Interference, Biology, Antiviral immunity, [SDV.IMM.II]Life Sciences [q-bio]/Immunology/Innate immunity, Virus, MESH: Drosophila melanogaster, 03 medical and health sciences, Immune system, Modes of infection, MESH: Dicistroviridae, MESH: Animals, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Model organism, Pathogen, Viral tropism, Innate immune system, ved/biology, Insect control, fungi, MESH: Host-Pathogen Interactions, Antiviral responses, biology.organism_classification, Virology, 3. Good health, Insects, 030104 developmental biology, Drosophila melanogaster, Drosophila C virus, [SDV.MP.VIR]Life Sciences [q-bio]/Microbiology and Parasitology/Virology, Tissue tropism, [SDV.IMM]Life Sciences [q-bio]/Immunology, Host–viral interactions, MESH: Immunity, Innate, MESH: Disease Models, Animal, MESH: Viral Tropism

Abstract

International audience; The use of Drosophila as a model organism has made an important contribution to our understanding of the function and regulation of innate immunity in insects. Indeed, insects can discriminate between different types of pathogens and mount specific and effective responses. Strikingly, the same pathogen can trigger a different immune response in the same organism, depending solely on the route of infection by which the pathogen is delivered. In this review, we recapitulate what is known about antiviral responses in Drosophila, and how they are triggered depending on the route and the mode used for the virus to infect its host.

Published

2018

24. Human DDX3X Unwinds Japanese Encephalitis and Zika Viral 5′ Terminal Regions.

Author

Nelson, Corey, Mrozowich, Tyler, Gemmill, Darren L., Park, Sean M., and Patel, Trushar R.

Subjects

*JAPANESE B encephalitis, *JAPANESE encephalitis viruses, *VIRAL encephalitis, *ZIKA virus, *PROTEIN-protein interactions, *ZIKA virus infections

Abstract

Flavivirus genus includes many deadly viruses such as the Japanese encephalitis virus (JEV) and Zika virus (ZIKV). The 5′ terminal regions (TR) of flaviviruses interact with human proteins and such interactions are critical for viral replication. One of the human proteins identified to interact with the 5′ TR of JEV is the DEAD-box helicase, DDX3X. In this study, we in vitro transcribed the 5′ TR of JEV and demonstrated its direct interaction with recombinant DDX3X (Kd of 1.66 ± 0.21 µM) using microscale thermophoresis (MST). Due to the proposed structural similarities of 5′ and 3′ TRs of flaviviruses, we investigated if the ZIKV 5′ TR could also interact with human DDX3X. Our MST studies suggested that DDX3X recognizes ZIKV 5′ TR with a Kd of 7.05 ± 0.75 µM. Next, we performed helicase assays that suggested that the binding of DDX3X leads to the unwinding of JEV and ZIKV 5′ TRs. Overall, our data indicate, for the first time, that DDX3X can directly bind and unwind in vitro transcribed flaviviral TRs. In summary, our work indicates that DDX3X could be further explored as a therapeutic target to inhibit Flaviviral replication [ABSTRACT FROM AUTHOR]

Published

2021

25. Human DDX17 Unwinds Rift Valley Fever Virus Non-Coding RNAs.

Author

Nelson, Corey R., Mrozowich, Tyler, Park, Sean M., D'souza, Simmone, Henrickson, Amy, Vigar, Justin R. J., Wieden, Hans-Joachim, Owens, Raymond J., Demeler, Borries, and Patel, Trushar R.

Subjects

*RIFT Valley fever, *NON-coding RNA, *RNA viruses, *SMALL-angle X-ray scattering, *RNA helicase

Abstract

Rift Valley fever virus (RVFV) is a mosquito-transmitted virus from the Bunyaviridae family that causes high rates of mortality and morbidity in humans and ruminant animals. Previous studies indicated that DEAD-box helicase 17 (DDX17) restricts RVFV replication by recognizing two primary non-coding RNAs in the S-segment of the genome: the intergenic region (IGR) and 5′ non-coding region (NCR). However, we lack molecular insights into the direct binding of DDX17 with RVFV non-coding RNAs and information on the unwinding of both non-coding RNAs by DDX17. Therefore, we performed an extensive biophysical analysis of the DDX17 helicase domain (DDX17135–555) and RVFV non-coding RNAs, IGR and 5' NCR. The homogeneity studies using analytical ultracentrifugation indicated that DDX17135–555, IGR, and 5' NCR are pure. Next, we performed small-angle X-ray scattering (SAXS) experiments, which suggested that DDX17 and both RNAs are homogenous as well. SAXS analysis also demonstrated that DDX17 is globular to an extent, whereas the RNAs adopt an extended conformation in solution. Subsequently, microscale thermophoresis (MST) experiments were performed to investigate the direct binding of DDX17 to the non-coding RNAs. The MST experiments demonstrated that DDX17 binds with the IGR and 5' NCR with a dissociation constant of 5.77 ± 0.15 µM and 9.85 ± 0.11 µM, respectively. As DDX17135–555 is an RNA helicase, we next determined if it could unwind IGR and NCR. We developed a helicase assay using MST and fluorescently-labeled oligos, which suggested DDX17135–555 can unwind both RNAs. Overall, our study provides direct evidence of DDX17135–555 interacting with and unwinding RVFV non-coding regions. [ABSTRACT FROM AUTHOR]

Published

2021

26. Human DDX17 Unwinds Rift Valley Fever Virus Non-Coding RNAs.

Author

Nelson CR, Mrozowich T, Park SM, D'souza S, Henrickson A, Vigar JRJ, Wieden HJ, Owens RJ, Demeler B, and Patel TR

Subjects

Adenosine Triphosphate, Animals, DEAD-box RNA Helicases chemistry, Humans, Models, Molecular, Protein Binding, Protein Conformation, Protein Interaction Domains and Motifs, RNA-Binding Proteins chemistry, RNA-Binding Proteins metabolism, Structure-Activity Relationship, DEAD-box RNA Helicases metabolism, Host-Pathogen Interactions, RNA, Untranslated, RNA, Viral, Rift Valley Fever metabolism, Rift Valley Fever virology, Rift Valley fever virus genetics

Abstract

Rift Valley fever virus (RVFV) is a mosquito-transmitted virus from the Bunyaviridae family that causes high rates of mortality and morbidity in humans and ruminant animals. Previous studies indicated that DEAD-box helicase 17 (DDX17) restricts RVFV replication by recognizing two primary non-coding RNAs in the S-segment of the genome: the intergenic region (IGR) and 5' non-coding region (NCR). However, we lack molecular insights into the direct binding of DDX17 with RVFV non-coding RNAs and information on the unwinding of both non-coding RNAs by DDX17. Therefore, we performed an extensive biophysical analysis of the DDX17 helicase domain (DDX17 135-555 ) and RVFV non-coding RNAs, IGR and 5' NCR. The homogeneity studies using analytical ultracentrifugation indicated that DDX17 135-555 , IGR, and 5' NCR are pure. Next, we performed small-angle X-ray scattering (SAXS) experiments, which suggested that DDX17 and both RNAs are homogenous as well. SAXS analysis also demonstrated that DDX17 is globular to an extent, whereas the RNAs adopt an extended conformation in solution. Subsequently, microscale thermophoresis (MST) experiments were performed to investigate the direct binding of DDX17 to the non-coding RNAs. The MST experiments demonstrated that DDX17 binds with the IGR and 5' NCR with a dissociation constant of 5.77 ± 0.15 µM and 9.85 ± 0.11 µM, respectively. As DDX17 135-555 is an RNA helicase, we next determined if it could unwind IGR and NCR. We developed a helicase assay using MST and fluorescently-labeled oligos, which suggested DDX17 135-555 can unwind both RNAs. Overall, our study provides direct evidence of DDX17 135-555 interacting with and unwinding RVFV non-coding regions.

Published

2020

27. Host Transcription Factors in Hepatitis B Virus RNA Synthesis.

Author

Turton KL, Meier-Stephenson V, Badmalia MD, Coffin CS, and Patel TR

Subjects

Animals, Genome, Viral, Hepatitis B virology, Hepatitis B virus physiology, Humans, Mice, Transcription Factors metabolism, Virus Replication, DNA, Circular genetics, Hepatitis B virus genetics, Host Microbial Interactions genetics, RNA, Viral biosynthesis, Transcription Factors genetics

Abstract

The hepatitis B virus (HBV) chronically infects over 250 million people worldwide and is one of the leading causes of liver cancer and hepatocellular carcinoma. HBV persistence is due in part to the highly stable HBV minichromosome or HBV covalently closed circular DNA (cccDNA) that resides in the nucleus. As HBV replication requires the help of host transcription factors to replicate, focusing on host protein-HBV genome interactions may reveal insights into new drug targets against cccDNA. The structural details on such complexes, however, remain poorly defined. In this review, the current literature regarding host transcription factors' interactions with HBV cccDNA is discussed., Competing Interests: The authors declare no conflicts of interest.

Published

2020