Your search keyword '"William B. Klimstra"' showing total 123 results

1. The VLDLR entry receptor is required for the pathogenesis of multiple encephalitic alphaviruses

Author

Sathvik Palakurty, Saravanan Raju, Alan Sariol, Zhenlu Chong, Ngan Wagoner, Hongming Ma, Ofer Zimmerman, Lucas J. Adams, Camille Carmona, Zhuoming Liu, Daved H. Fremont, Sean P.J. Whelan, William B. Klimstra, and Michael S. Diamond

Subjects

CP: Microbiology, CP: Immunology, Biology (General), QH301-705.5

Abstract

Summary: The very-low-density lipoprotein receptor (VLDLR) has been reported as an entry receptor for Semliki Forest (SFV) and Eastern equine encephalitis (EEEV) alphaviruses in cell cultures. However, the role of VLDLR in alphavirus pathogenesis and the extent to which other alphaviruses can engage VLDLR remains unclear. Here, using a surface protein-targeted CRISPR-Cas9 screen, we identify VLDLR as a receptor for Western equine encephalitis virus (WEEV) and demonstrate that it promotes the infection of multiple viruses in the WEE antigenic complex. In vivo studies show that the pathogenicity of WEEV, EEEV, and SFV, but not the distantly related Venezuelan equine encephalitis virus, is markedly diminished in VLDLR-deficient mice and that mice treated with a soluble VLDLR-Fc decoy molecule are protected against disease. Overall, these results expand our understanding of the role of VLDLR in alphavirus pathogenesis and provide a potential path for developing countermeasures against alphaviruses from different antigenic complexes.

Published

2024

2. The low-density lipoprotein receptor promotes infection of multiple encephalitic alphaviruses

Author

Hongming Ma, Lucas J. Adams, Saravanan Raju, Alan Sariol, Natasha M. Kafai, Hana Janova, William B. Klimstra, Daved H. Fremont, and Michael S. Diamond

Subjects

Science

Abstract

Abstract Members of the low-density lipoprotein receptor (LDLR) family, including LDLRAD3, VLDLR, and ApoER2, were recently described as entry factors for different alphaviruses. However, based on studies with gene edited cells and knockout mice, blockade or abrogation of these receptors does not fully inhibit alphavirus infection, indicating the existence of additional uncharacterized entry factors. Here, we perform a CRISPR-Cas9 genome-wide loss-of-function screen in mouse neuronal cells with a chimeric alphavirus expressing the Eastern equine encephalitis virus (EEEV) structural proteins and identify LDLR as a candidate receptor. Expression of LDLR on the surface of neuronal or non-neuronal cells facilitates binding and infection of EEEV, Western equine encephalitis virus, and Semliki Forest virus. Domain mapping and binding studies reveal a low-affinity interaction with LA domain 3 (LA3) that can be enhanced by concatenation of LA3 repeats. Soluble decoy proteins with multiple LA3 repeats inhibit EEEV infection in cell culture and in mice. Our results establish LDLR as a low-affinity receptor for multiple alphaviruses and highlight a possible path for developing inhibitors that could mitigate infection and disease.

Published

2024

3. Post-exposure intranasal IFNα suppresses replication and neuroinvasion of Venezuelan Equine Encephalitis virus within olfactory sensory neurons

Author

Matthew D. Cain, N. Rubin Klein, Xiaoping Jiang, Hamid Salimi, Qingping Wu, Mark J. Miller, William B. Klimstra, and Robyn S. Klein

Subjects

Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background Venezuelan Equine Encephalitis virus (VEEV) may enter the central nervous system (CNS) within olfactory sensory neurons (OSN) that originate in the nasal cavity after intranasal exposure. While it is known that VEEV has evolved several mechanisms to inhibit type I interferon (IFN) signaling within infected cells, whether this inhibits virologic control during neuroinvasion along OSN has not been studied. Methods We utilized an established murine model of intranasal infection with VEEV and a repository of scRNAseq data from IFN-treated OSN to assess the cellular targets and IFN signaling responses after VEEV exposure. Results We found that immature OSN, which express higher levels of the VEEV receptor LDLRAD3 than mature OSN, are the first cells infected by VEEV. Despite rapid VEEV neuroinvasion after intranasal exposure, olfactory neuroepithelium (ONE) and olfactory bulb (OB) IFN responses, as assessed by evaluation of expression of interferon signaling genes (ISG), are delayed for up to 48 h during VEEV neuroinvasion, representing a potential therapeutic window. Indeed, a single intranasal dose of recombinant IFNα triggers early ISG expression in both the nasal cavity and OB. When administered at the time of or early after infection, IFNα treatment delayed onset of sequelae associated with encephalitis and extended survival by several days. VEEV replication after IFN treatment was also transiently suppressed in the ONE, which inhibited subsequent invasion into the CNS. Conclusions Our results demonstrate a critical and promising first evaluation of intranasal IFNα for the treatment of human encephalitic alphavirus exposures.

Published

2024

4. Transchromosomic bovine-derived anti-SARS-CoV-2 polyclonal human antibodies protects hACE2 transgenic hamsters against multiple variants

Author

Theron Gilliland, Matthew Dunn, Yanan Liu, Maria D.H. Alcorn, Yutaka Terada, Shauna Vasilatos, Jeneveve Lundy, Rong Li, Sham Nambulli, Deanna Larson, Paul Duprex, Hua Wu, Thomas Luke, Christoph Bausch, Kristi Egland, Eddie Sullivan, Zhongde Wang, and William B. Klimstra

Subjects

Immunology, Immune response, Virology, Science

Abstract

Summary: Pandemic SARS-CoV-2 has undergone rapid evolution resulting in the emergence of many variants with mutations in the spike protein, some of which appear to evade antibody neutralization, transmit more efficiently, and/or exhibit altered virulence. This raises significant concerns regarding the efficacy of anti-S monoclonal antibody-based therapeutics which have failed against variant SARS-CoV-2 viruses. To address this concern, SAB-185, a human anti-SARS-CoV-2 polyclonal antibody was generated in the DiversitAb platform. SAB-185 exhibited equivalent, robust in vitro neutralization for Munich, Alpha, Beta, Gamma, and Δ144-146 variants and, although diminished, retained PRNT50 and PRNT80 neutralization endpoints for Delta and Omicron variants. Human ACE2 transgenic Syrian hamsters, which exhibit lethal SARS-CoV-2 disease, were protected from mortality after challenge with the Munich, Alpha, Beta, Delta, and Δ144-146 variants and clinical signs after non-lethal Omicron BA.1 infection. This suggests that SAB-185 may be an effective immunotherapy even in the presence of ongoing viral mutation.

Published

2023

5. Human immunoglobulin from transchromosomic bovines hyperimmunized with SARS-CoV-2 spike antigen efficiently neutralizes viral variants

Author

Zhuoming Liu, Hua Wu, Kristi A. Egland, Theron C. Gilliland, Matthew D. Dunn, Thomas C. Luke, Eddie J. Sullivan, William B. Klimstra, Christoph L. Bausch, and Sean P. J. Whelan

Subjects

sars-cov-2, variants, polyclonal antibodies, transchromosomic bovines, Immunologic diseases. Allergy, RC581-607, Therapeutics. Pharmacology, RM1-950

Abstract

Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) variants with amino-acid substitutions and deletions in spike protein (S) can reduce the effectiveness of monoclonal antibodies (mAbs) and may compromise immunity induced by vaccines. We report a polyclonal, fully human, anti-SARS-CoV-2 immunoglobulin produced in transchromosomic bovines (Tc-hIgG-SARS-CoV-2) hyperimmunized with two doses of plasmid DNA encoding the SARS-CoV-2 Wuhan strain S gene, followed by repeated immunization with S protein purified from insect cells. The resulting Tc-hIgG-SARS-CoV-2, termed SAB-185, efficiently neutralizes SARS-CoV-2, and vesicular stomatitis virus (VSV) SARS-CoV-2 chimeras in vitro. Neutralization potency was retained for S variants including S477N, E484K, and N501Y, substitutions present in recent variants of concern. In contrast to the ease of selection of escape variants with mAbs and convalescent human plasma, we were unable to isolate VSV-SARS-CoV-2 mutants resistant to Tc-hIgG-SARS-CoV-2 neutralization. This fully human immunoglobulin that potently inhibits SARS-CoV-2 infection may provide an effective therapeutic to combat COVID-19.

Published

2022

6. Persistence of Severe Acute Respiratory Syndrome Coronavirus 2 in Aerosol Suspensions

Author

Alyssa C. Fears, William B. Klimstra, Paul Duprex, Amy Hartman, Scott C. Weaver, Kenneth S. Plante, Divya Mirchandani, Jessica Ann Plante, Patricia V. Aguilar, Diana Fernández, Aysegul Nalca, Aysegul Totura, David Dyer, Brian Kearney, Matthew Lackemeyer, J. Kyle Bohannon, Reed Johnson, Robert F. Garry, Doug S. Reed, and Chad J. Roy

Subjects

aerosol, coronavirus diseases, 2019 novel coronavirus disease, COVID-19, SARS-CoV-2, severe acute respiratory syndrome coronavirus 2, Medicine, Infectious and parasitic diseases, RC109-216

Abstract

We aerosolized severe acute respiratory syndrome coronavirus 2 and determined that its dynamic aerosol efficiency surpassed those of severe acute respiratory syndrome coronavirus and Middle East respiratory syndrome. Although we performed experiment only once across several laboratories, our findings suggest retained infectivity and virion integrity for up to 16 hours in respirable-sized aerosols.

Published

2020

7. In Vitro and In Vivo Phenotypes of Venezuelan, Eastern and Western Equine Encephalitis Viruses Derived from cDNA Clones of Human Isolates

Author

Christina L. Gardner, Chengqun Sun, Matthew D. Dunn, Theron C. Gilliland, Derek W. Trobaugh, Yutaka Terada, Douglas S. Reed, Amy L. Hartman, and William B. Klimstra

Subjects

cDNA clone, equine, encephalitis, alphavirus, wild type, human isolate, Microbiology, QR1-502

Abstract

The Department of Defense recently began an effort to improve and standardize virus challenge materials and efficacy determination strategies for testing therapeutics and vaccines. This includes stabilization of virus genome sequences in cDNA form where appropriate, use of human-derived virus isolates, and noninvasive strategies for determination of challenge virus replication. Eventually, it is desired that these approaches will satisfy the FDA “Animal Rule” for licensure, which substitutes animal efficacy data when human data are unlikely to be available. To this end, we created and examined the virulence phenotype of cDNA clones of prototypic human infection-derived strains of the alphaviruses, Venezuelan (VEEV INH9813), eastern (EEEV V105) and western (WEEV Fleming) equine encephalitis viruses, and created fluorescent and luminescent reporter expression vectors for evaluation of replication characteristics in vitro and in vivo. Sequences of minimally passaged isolates of each virus were used to synthesize full-length cDNA clones along with a T7 transcription promoter-based bacterial propagation vector. Viruses generated from the cDNA clones were compared with other “wild type” strains derived from cDNA clones and GenBank sequences to identify and eliminate putative tissue culture artifacts accumulated in the cell passaged biological stocks. This was followed by examination of aerosol and subcutaneous infection and disease in mouse models. A mutation that increased heparan sulfate binding was identified in the VEEV INH9813 biological isolate sequence and eliminated from the cDNA clone. Viruses derived from the new human isolate cDNA clones showed similar mouse virulence to existing clone-derived viruses after aerosol or subcutaneous inoculation.

Published

2022

8. Microneedle array delivered recombinant coronavirus vaccines: Immunogenicity and rapid translational development

Author

Eun Kim, Geza Erdos, Shaohua Huang, Thomas W. Kenniston, Stephen C. Balmert, Cara Donahue Carey, V. Stalin Raj, Michael W. Epperly, William B. Klimstra, Bart L. Haagmans, Emrullah Korkmaz, Louis D. Falo, Jr., and Andrea Gambotto

Subjects

Subunit vaccines, Trimerization, Microneedle array, MERS-CoV S1, SARS-CoV-2, COVID-19, Medicine, Medicine (General), R5-920

Abstract

Background: Coronaviruses pose a serious threat to global health as evidenced by Severe Acute Respiratory Syndrome (SARS), Middle East Respiratory Syndrome (MERS), and COVID-19. SARS Coronavirus (SARS-CoV), MERS Coronavirus (MERS-CoV), and the novel coronavirus, previously dubbed 2019-nCoV, and now officially named SARS-CoV-2, are the causative agents of the SARS, MERS, and COVID-19 disease outbreaks, respectively. Safe vaccines that rapidly induce potent and long-lasting virus-specific immune responses against these infectious agents are urgently needed. The coronavirus spike (S) protein, a characteristic structural component of the viral envelope, is considered a key target for vaccines for the prevention of coronavirus infection. Methods: We first generated codon optimized MERS-S1 subunit vaccines fused with a foldon trimerization domain to mimic the native viral structure. In variant constructs, we engineered immune stimulants (RS09 or flagellin, as TLR4 or TLR5 agonists, respectively) into this trimeric design. We comprehensively tested the pre-clinical immunogenicity of MERS-CoV vaccines in mice when delivered subcutaneously by traditional needle injection, or intracutaneously by dissolving microneedle arrays (MNAs) by evaluating virus specific IgG antibodies in the serum of vaccinated mice by ELISA and using virus neutralization assays. Driven by the urgent need for COVID-19 vaccines, we utilized this strategy to rapidly develop MNA SARS-CoV-2 subunit vaccines and tested their pre-clinical immunogenicity in vivo by exploiting our substantial experience with MNA MERS-CoV vaccines. Findings: Here we describe the development of MNA delivered MERS-CoV vaccines and their pre-clinical immunogenicity. Specifically, MNA delivered MERS-S1 subunit vaccines elicited strong and long-lasting antigen-specific antibody responses. Building on our ongoing efforts to develop MERS-CoV vaccines, promising immunogenicity of MNA-delivered MERS-CoV vaccines, and our experience with MNA fabrication and delivery, including clinical trials, we rapidly designed and produced clinically-translatable MNA SARS-CoV-2 subunit vaccines within 4 weeks of the identification of the SARS-CoV-2 S1 sequence. Most importantly, these MNA delivered SARS-CoV-2 S1 subunit vaccines elicited potent antigen-specific antibody responses that were evident beginning 2 weeks after immunization. Interpretation: MNA delivery of coronaviruses-S1 subunit vaccines is a promising immunization strategy against coronavirus infection. Progressive scientific and technological efforts enable quicker responses to emerging pandemics. Our ongoing efforts to develop MNA-MERS-S1 subunit vaccines enabled us to rapidly design and produce MNA SARS-CoV-2 subunit vaccines capable of inducing potent virus-specific antibody responses. Collectively, our results support the clinical development of MNA delivered recombinant protein subunit vaccines against SARS, MERS, COVID-19, and other emerging infectious diseases.

Published

2020

9. Encephalitic Alphaviruses Exploit Caveola-Mediated Transcytosis at the Blood-Brain Barrier for Central Nervous System Entry

Author

Hamid Salimi, Matthew D. Cain, Xiaoping Jiang, Robyn A. Roth, Wandy L. Beatty, Chengqun Sun, William B. Klimstra, Jianghui Hou, and Robyn S. Klein

Subjects

IFNAR, Venezuelan encephalitis virus, western equine encephalitis virus, alphavirus, blood-brain barrier, caveola-mediated transcytosis, Microbiology, QR1-502

Abstract

ABSTRACT Venezuelan and western equine encephalitis viruses (VEEV and WEEV, respectively) invade the central nervous system (CNS) early during infection, via neuronal and hematogenous routes. While viral replication mediates host shutoff, including expression of type I interferons (IFN), few studies have addressed how alphaviruses gain access to the CNS during established infection or the mechanisms of viral crossing at the blood-brain barrier (BBB). Here, we show that hematogenous dissemination of VEEV and WEEV into the CNS occurs via caveolin-1 (Cav-1)-mediated transcytosis (Cav-MT) across an intact BBB, which is impeded by IFN and inhibitors of RhoA GTPase. Use of reporter and nonreplicative strains also demonstrates that IFN signaling mediates viral restriction within cells comprising the neurovascular unit (NVU), differentially rendering brain endothelial cells, pericytes, and astrocytes permissive to viral replication. Transmission and immunoelectron microscopy revealed early events in virus internalization and Cav-1 association within brain endothelial cells. Cav-1-deficient mice exhibit diminished CNS VEEV and WEEV titers during early infection, whereas viral burdens in peripheral tissues remained unchanged. Our findings show that alphaviruses exploit Cav-MT to enter the CNS and that IFN differentially restricts this process at the BBB. IMPORTANCE VEEV, WEEV, and eastern equine encephalitis virus (EEEV) are emerging infectious diseases in the Americas, and they have caused several major outbreaks in the human and horse population during the past few decades. Shortly after infection, these viruses can infect the CNS, resulting in severe long-term neurological deficits or death. Neuroinvasion has been associated with virus entry into the CNS directly from the bloodstream; however, the underlying molecular mechanisms have remained largely unknown. Here, we demonstrate that following peripheral infection alphavirus augments vesicular formation/trafficking at the BBB and utilizes Cav-MT to cross an intact BBB, a process regulated by activators of Rho GTPases within brain endothelium. In vivo examination of early viral entry in Cav-1-deficient mice revealed significantly lower viral burdens in the brain than in similarly infected wild-type animals. These studies identify a potentially targetable pathway to limit neuroinvasion by alphaviruses.

Published

2020

10. Venezuelan Equine Encephalitis Virus nsP3 Phosphorylation Can Be Mediated by IKKβ Kinase Activity and Abrogation of Phosphorylation Inhibits Negative-Strand Synthesis

Author

Allison Bakovic, Nishank Bhalla, Stephanie Kortchak, Chengqun Sun, Weidong Zhou, Aslaa Ahmed, Kenneth Risner, William B. Klimstra, and Aarthi Narayanan

Subjects

Venezuelan equine encephalitis virus, phosphorylation, IKK complex, IKKβ kinase assay, replication-deficient, non-structural protein 3, Microbiology, QR1-502

Abstract

Venezuelan equine encephalitis virus (VEEV), a mosquito transmitted alphavirus of the Togaviridae family, can cause a highly inflammatory and encephalitic disease upon infection. Although a category B select agent, no FDA-approved vaccines or therapeutics against VEEV currently exist. We previously demonstrated NF-κB activation and macromolecular reorganization of the IKK complex upon VEEV infection in vitro, with IKKβ inhibition reducing viral replication. Mass spectrometry and confocal microscopy revealed an interaction between IKKβ and VEEV non-structural protein 3 (nsP3). Here, using western blotting, a cell-free kinase activity assay, and mass spectrometry, we demonstrate that IKKβ kinase activity can directly phosphorylate VEEV nsP3 at sites 204/5, 142, and 134/5. Alanine substitution mutations at sites 204/5, 142, or 134/5 reduced VEEV replication by >30-100,000-fold corresponding to a severe decrease in negative-strand synthesis. Serial passaging rescued viral replication and negative-strand synthesis, and sequencing of revertant viruses revealed reversion to the wild-type TC-83 phosphorylation capable amino acid sequences at nsP3 sites 204/5, 142, and 135. Generation of phosphomimetic mutants using aspartic acid substitutions at site 204/5 resulted in rescue of both viral replication and negative-strand RNA production, whereas phosphomimetic mutant 134/5 rescued viral replication but failed to restore negative-strand RNA levels, and phosphomimetic mutant 142 did not rescue VEEV replication. Together, these data demonstrate that IKKβ can phosphorylate VEEV nsP3 at sites 204/5, 142, and 134/5, and suggest that phosphorylation is essential for negative-strand RNA synthesis at site 204/5, but may be important for infectious particle production at site 134/5.

Published

2020

11. Cryo-EM Structures of Eastern Equine Encephalitis Virus Reveal Mechanisms of Virus Disassembly and Antibody Neutralization

Author

S. Saif Hasan, Chengqun Sun, Arthur S. Kim, Yasunori Watanabe, Chun-Liang Chen, Thomas Klose, Geeta Buda, Max Crispin, Michael S. Diamond, William B. Klimstra, and Michael G. Rossmann

Subjects

Biology (General), QH301-705.5

Abstract

Summary: Alphaviruses are enveloped pathogens that cause arthritis and encephalitis. Here, we report a 4.4-Å cryoelectron microscopy (cryo-EM) structure of eastern equine encephalitis virus (EEEV), an alphavirus that causes fatal encephalitis in humans. Our analysis provides insights into viral entry into host cells. The envelope protein E2 showed a binding site for the cellular attachment factor heparan sulfate. The presence of a cryptic E2 glycan suggests how EEEV escapes surveillance by lectin-expressing myeloid lineage cells, which are sentinels of the immune system. A mechanism for nucleocapsid core release and disassembly upon viral entry was inferred based on pH changes and capsid dissociation from envelope proteins. The EEEV capsid structure showed a viral RNA genome binding site adjacent to a ribosome binding site for viral genome translation following genome release. Using five Fab-EEEV complexes derived from neutralizing antibodies, our investigation provides insights into EEEV host cell interactions and protective epitopes relevant to vaccine design. : Hasan et al. use single-particle cryoelectron microscopy to elucidate the molecular basis of host cell entry of neurovirulent EEEV. They show that the EEEV envelope is primed for intracellular pH sensing and subsequent disassembly. Monoclonal antibodies effectively inhibit EEEV entry by cross-linking the viral envelope. Keywords: alphavirus, cryoelectron microscopy, glycosylation, antibodies, conformational changes, virus entry, virus disassembly

Published

2018

12. The Interferon-Induced Exonuclease ISG20 Exerts Antiviral Activity through Upregulation of Type I Interferon Response Proteins

Author

Christopher M. Weiss, Derek W. Trobaugh, Chengqun Sun, Tiffany M. Lucas, Michael S. Diamond, Kate D. Ryman, and William B. Klimstra

Subjects

alphavirus, host-pathogen interactions, innate immunity, interferon-stimulated gene, virus-host interactions, Microbiology, QR1-502

Abstract

ABSTRACT Type I interferon (IFN)-stimulated genes (ISGs) have critical roles in inhibiting virus replication and dissemination. Despite advances in understanding the molecular basis of ISG restriction, the antiviral mechanisms of many remain unclear. The 20-kDa ISG ISG20 is a nuclear 3′–5′ exonuclease with preference for single-stranded RNA (ssRNA) and has been implicated in the IFN-mediated restriction of several RNA viruses. Although the exonuclease activity of ISG20 has been shown to degrade viral RNA in vitro, evidence has yet to be presented that virus inhibition in cells requires this activity. Here, we utilized a combination of an inducible, ectopic expression system and newly generated Isg20−/− mice to investigate mechanisms and consequences of ISG20-mediated restriction. Ectopically expressed ISG20 localized primarily to Cajal bodies in the nucleus and restricted replication of chikungunya and Venezuelan equine encephalitis viruses. Although restriction by ISG20 was associated with inhibition of translation of infecting genomic RNA, degradation of viral RNAs was not observed. Instead, translation inhibition of viral RNA was associated with ISG20-induced upregulation of over 100 other genes, many of which encode known antiviral effectors. ISG20 modulated the production of IFIT1, an ISG that suppresses translation of alphavirus RNAs. Consistent with this observation, the pathogenicity of IFIT1-sensitive alphaviruses was increased in Isg20−/− mice compared to that of wild-type viruses but not in cells ectopically expressing ISG20. Our findings establish an indirect role for ISG20 in the early restriction of RNA virus replication by regulating expression of other ISGs that inhibit translation and possibly other activities in the replication cycle. IMPORTANCE The host immune responses to infection lead to the production of type I interferon (IFN), and the upregulation of interferon-stimulated genes (ISGs) reduces virus replication and virus dissemination within a host. Ectopic expression of the interferon-induced 20-kDa exonuclease ISG20 suppressed replication of chikungunya virus and Venezuelan equine encephalitis virus, two mosquito-vectored RNA alphaviruses. Since the replication of alphavirus genomes occurs exclusively in the cytoplasm, the mechanism of nucleus-localized ISG20 inhibition of replication is unclear. In this study, we determined that ISG20 acts as a master regulator of over 100 genes, many of which are ISGs. Specifically, ISG20 upregulated IFIT1 genes and inhibited translation of the alphavirus genome. Furthermore, IFIT1-sensitive alphavirus replication was increased in Isg20−/− mice compared to the replication of wild-type viruses but not in cells ectopically expressing ISG20. We propose that ISG20 acts as an indirect regulator of RNA virus replication in the cytoplasm through the upregulation of many other ISGs.

Published

2018

13. The Efficacy of the Interferon Alpha/Beta Response versus Arboviruses Is Temperature Dependent

Author

Whitney C. Lane, Matthew D. Dunn, Christina L. Gardner, L. K. Metthew Lam, Alan M. Watson, Amy L. Hartman, Kate D. Ryman, and William B. Klimstra

Subjects

alphavirus, arbovirus, chikungunya virus, interferons, temperature, Microbiology, QR1-502

Abstract

ABSTRACT Interferon alpha/beta (IFN-α/β) is a critical mediator of protection against most viruses, with host survival frequently impossible in its absence. Many studies have investigated the pathways involved in the induction of IFN-α/β after virus infection and the resultant upregulation of antiviral IFN-stimulated genes (ISGs) through IFN-α/β receptor complex signaling. However, other than examining the effects of genetic deletion of induction or effector pathway components, little is known regarding the functionality of these responses in intact hosts and whether host genetic or environmental factors might influence their potency. Here, we demonstrate that the IFN-α/β response against multiple arthropod-vectored viruses, which replicate over a wide temperature range, is extremely sensitive to fluctuations in temperature, exhibiting reduced antiviral efficacy at subnormal cellular temperatures and increased efficacy at supranormal temperatures. The effect involves both IFN-α/β and ISG upregulation pathways with a major aspect of altered potency reflecting highly temperature-dependent transcription of IFN response genes that leads to altered IFN-α/β and ISG protein levels. Discordantly, signaling steps prior to transcription that were examined showed the opposite effect from gene transcription, with potentiation at low temperature and inhibition at high temperature. Finally, we demonstrate that by lowering the temperature of mice, chikungunya arbovirus replication and disease are exacerbated in an IFN-α/β-dependent manner. This finding raises the potential for use of hyperthermia as a therapeutic modality for viral infections and in other contexts such as antitumor therapy. The increased IFN-α/β efficacy at high temperatures may also reflect an innate immune-relevant aspect of the febrile response. IMPORTANCE The interferon alpha/beta (IFN-α/β) response is a first-line innate defense against arthropod-borne viruses (arboviruses). Arboviruses, such as chikungunya virus (CHIKV), can infect cells and replicate across a wide temperature range due to their replication in both mammalian/avian and arthropod hosts. Accordingly, these viruses can cause human disease in tissues regularly exposed to temperatures below the normal mammalian core temperature, 37°C. We questioned whether temperature variation could affect the efficacy of IFN-α/β responses against these viruses and help to explain some aspects of human disease manifestations. We observed that IFN-α/β efficacy was dramatically lower at subnormal temperatures and modestly enhanced at febrile temperatures, with the effects involving altered IFN-α/β response gene transcription but not IFN-α/β pathway signaling. These results provide insight into the functioning of the IFN-α/β response in vivo and suggest that temperature elevation may represent an immune-enhancing therapeutic modality for a wide variety of IFN-α/β-sensitive infections and pathologies.

Published

2018

14. Electrocardiography Abnormalities in Macaques after Infection with Encephalitic Alphaviruses

Author

Henry Ma, Jeneveve D. Lundy, Katherine J. O'Malley, William B. Klimstra, Amy L. Hartman, and and Douglas S. Reed

Subjects

alphavirus, vaccine, arbovirus, animal models, nonhuman primates, electrocardiography, ecg, aerosol, encephalitis, equine, Medicine

Abstract

Eastern (EEEV) and Venezuelan (VEEV) equine encephalitis viruses (EEVs) are related, (+) ssRNA arboviruses that can cause severe, sometimes fatal, encephalitis in humans. EEVs are highly infectious when aerosolized, raising concerns for potential use as biological weapons. No licensed medical countermeasures exist; given the severity/rarity of natural EEV infections, efficacy studies require animal models. Cynomolgus macaques exposed to EEV aerosols develop fever, encephalitis, and other clinical signs similar to humans. Fever is nonspecific for encephalitis in macaques. Electrocardiography (ECG) metrics may predict onset, severity, or outcome of EEV-attributable disease. Macaques were implanted with thermometry/ECG radiotransmitters and exposed to aerosolized EEV. Data was collected continuously, and repeated-measures ANOVA and frequency-spectrum analyses identified differences between courses of illness and between pre-exposure and post-exposure states. EEEV-infected macaques manifested widened QRS-intervals in severely ill subjects post-exposure. Moreover, QT-intervals and RR-intervals decreased during the febrile period. VEEV-infected macaques suffered decreased QT-intervals and RR-intervals with fever onset. Frequency-spectrum analyses revealed differences in the fundamental frequencies of multiple metrics in the post-exposure and febrile periods compared to baseline and confirmed circadian dysfunction. Heart rate variability (HRV) analyses revealed diminished variability post-exposure. These analyses support using ECG data alongside fever and clinical laboratory findings for evaluating medical countermeasure efficacy.

Published

2019

15. Cryo-EM structures of alphavirus conformational intermediates in low pH-triggered prefusion states

Author

Chun-Liang Chen, Thomas Klose, Chengqun Sun, Arthur S. Kim, Geeta Buda, Michael G. Rossmann, Michael S. Diamond, William B. Klimstra, and Richard J. Kuhn

Subjects

Multidisciplinary, Viral Envelope Proteins, Protein Conformation, Protein Stability, Cryoelectron Microscopy, Encephalitis Virus, Eastern Equine, Hydrogen-Ion Concentration, Antiviral Agents

Abstract

Alphaviruses can cause severe human arthritis and encephalitis. During virus infection, structural changes of viral glycoproteins in the acidified endosome trigger virus–host membrane fusion for delivery of the capsid core and RNA genome into the cytosol to initiate virus translation and replication. However, mechanisms by which E1 and E2 glycoproteins rearrange in this process remain unknown. Here, we investigate prefusion cryoelectron microscopy (cryo-EM) structures of eastern equine encephalitis virus (EEEV) under acidic conditions. With models fitted into the low-pH cryo-EM maps, we suggest that E2 dissociates from E1, accompanied by a rotation (∼60°) of the E2-B domain (E2-B) to expose E1 fusion loops. Cryo-EM reconstructions of EEEV bound to a protective antibody at acidic and neutral pH suggest that stabilization of E2-B prevents dissociation of E2 from E1. These findings reveal conformational changes of the glycoprotein spikes in the acidified host endosome. Stabilization of E2-B may provide a strategy for antiviral agent development.

Published

2023

16. LDLRAD3 is a receptor for Venezuelan equine encephalitis virus

Author

Theron C. Gilliland, Larissa B. Thackray, Chengqun Sun, James Brett Case, Aadit P. Shah, William B. Klimstra, James T. Earnest, Christopher A. Nelson, Daved H. Fremont, Michael S. Diamond, Arthur S. Kim, Hongming Ma, Katherine Basore, and Natasha M. Kafai

Subjects

Male, Virus genetics, Virus Attachment, Virulence, Alphavirus, Biology, medicine.disease_cause, Article, Virus, Cell Line, Encephalitis Virus, Venezuelan Equine, Mice, 03 medical and health sciences, medicine, Animals, Humans, 030304 developmental biology, 0303 health sciences, Multidisciplinary, Genetic Complementation Test, 030302 biochemistry & molecular biology, Encephalomyelitis, Venezuelan Equine, Virus Internalization, medicine.disease, biology.organism_classification, Virology, Fusion protein, Mice, Inbred C57BL, Receptors, LDL, Venezuelan equine encephalitis virus, biology.protein, Receptors, Virus, Female, CRISPR-Cas Systems, Antibody, Encephalitis, Protein Binding

Abstract

Venezuelan equine encephalitis virus (VEEV) is a neurotropic alphavirus transmitted by mosquitoes that causes encephalitis and death in humans1. VEEV is a biodefence concern because of its potential for aerosol spread and the current lack of sufficient countermeasures. The host factors that are required for VEEV entry and infection remain poorly characterized. Here, using a genome-wide CRISPR–Cas9-based screen, we identify low-density lipoprotein receptor class A domain-containing 3 (LDLRAD3)—a highly conserved yet poorly characterized member of the scavenger receptor superfamily—as a receptor for VEEV. Gene editing of mouse Ldlrad3 or human LDLRAD3 results in markedly reduced viral infection of neuronal cells, which is restored upon complementation with LDLRAD3. LDLRAD3 binds directly to VEEV particles and enhances virus attachment and internalization into host cells. Genetic studies indicate that domain 1 of LDLRAD3 (LDLRAD3(D1)) is necessary and sufficient to support infection by VEEV, and both anti-LDLRAD3 antibodies and an LDLRAD3(D1)–Fc fusion protein block VEEV infection in cell culture. The pathogenesis of VEEV infection is abrogated in mice with deletions in Ldlrad3, and administration of LDLRAD3(D1)–Fc abolishes disease caused by several subtypes of VEEV, including highly virulent strains. The development of a decoy-receptor fusion protein suggests a strategy for the prevention of severe VEEV infection and associated disease in humans. LDLRAD3 is a receptor for infection with Venezuelan equine encephalitis virus, and in mouse models deletion of Ldlrad3 or treatment with a soluble LDLRAD3 decoy molecule abrogates infection and disease caused by this virus.

Published

2020

17. Persistence of Severe Acute Respiratory Syndrome Coronavirus 2 in Aerosol Suspensions

Author

Divya Mirchandani, Scott C. Weaver, Paul Duprex, Aysegul Nalca, Alyssa C. Fears, Robert F. Garry, Reed F. Johnson, Patricia V. Aguilar, Aysegul Totura, David W. Dyer, Kenneth S. Plante, Diana Fernández, J. Kyle Bohannon, William B. Klimstra, Jessica A. Plante, Chad J. Roy, Matthew G. Lackemeyer, Brian J. Kearney, Amy L. Hartman, and Doug S. Reed

Subjects

Microbiology (medical), Epidemiology, Middle East respiratory syndrome coronavirus, aerosol, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), viruses, 030231 tropical medicine, lcsh:Medicine, macromolecular substances, medicine.disease_cause, complex mixtures, Persistence (computer science), Microbiology, 2019 novel coronavirus disease, lcsh:Infectious and parasitic diseases, 03 medical and health sciences, 0302 clinical medicine, medicine, lcsh:RC109-216, 030212 general & internal medicine, coronavirus diseases, Aerosolization, Infectivity, biology, business.industry, SARS-CoV-2, lcsh:R, COVID-19, respiratory system, biology.organism_classification, medicine.disease, Aerosol, Infectious Diseases, nervous system, Middle East respiratory syndrome, business, Betacoronavirus, severe acute respiratory syndrome coronavirus 2

Abstract

We aerosolized severe acute respiratory syndrome coronavirus 2 and determined that its dynamic aerosol efficiency surpassed those of severe acute respiratory syndrome coronavirus and Middle East respiratory syndrome. Although we performed experiment only once across several laboratories, our findings suggest retained infectivity and virion integrity for up to 16 hours in respirable-sized aerosols.

Published

2020

18. Glycosaminoglycan binding by arboviruses: a cautionary tale

Author

Maria D. H. Alcorn and William B. Klimstra

Subjects

viruses, Virology, virus diseases, Reviews, Animals, Humans, Heparitin Sulfate, Arbovirus Infections, Arboviruses

Abstract

Arboviruses are medically important arthropod-borne viruses that cause a range of diseases in humans from febrile illness to arthritis, encephalitis and hemorrhagic fever. Given their transmission cycles, these viruses face the challenge of replicating in evolutionarily divergent organisms that can include ticks, flies, mosquitoes, birds, rodents, reptiles and primates. Furthermore, their cell attachment receptor utilization may be affected by the opposing needs for generating high and sustained serum viremia in vertebrates such that virus particles are efficiently collected during a hematophagous arthropod blood meal but they must also bind sufficiently to cellular structures on divergent organisms such that productive infection can be initiated and viremia generated. Sulfated polysaccharides of the glycosaminoglycan (GAG) groups, primarily heparan sulfate (HS), have been identified as cell attachment moieties for many arboviruses. Original identification of GAG binding as a phenotype of arboviruses appeared to involve this attribute arising solely as a consequence of adaptation of virus isolates to growth in cell culture. However, more recently, naturally circulating strains of at least one arbovirus, eastern equine encephalitis, have been shown to bind HS efficiently and the GAG binding phenotype continues to be associated with arbovirus infection in published studies. If GAGs are attachment receptors for many naturally circulating arboviruses, this could lead to development of broad-spectrum antiviral therapies through blocking of the virus–GAG interaction. This review summarizes the available data for GAG/HS binding as a phenotype of naturally circulating arbovirus strains emphasizing the importance of avoiding tissue culture amplification and artifactual phenotypes during their isolation.

Published

2022

19. Neutralizing antibodies protect mice against Venezuelan equine encephalitis virus aerosol challenge

Author

Natasha M. Kafai, Lauren E. Williamson, Elad Binshtein, Soila Sukupolvi-Petty, Christina L. Gardner, Jaclyn Liu, Samantha Mackin, Arthur S. Kim, Nurgun Kose, Robert H. Carnahan, Ana Jung, Lindsay Droit, Douglas S. Reed, Scott A. Handley, William B. Klimstra, James E. Crowe, and Michael S. Diamond

Subjects

Aerosols, Encephalitis Virus, Venezuelan Equine, Mice, Immunology, Cryoelectron Microscopy, Immunology and Allergy, Animals, Antibodies, Monoclonal, Encephalomyelitis, Venezuelan Equine, Viral Vaccines, Horses, Antibodies, Viral, Antibodies, Neutralizing

Abstract

Venezuelan equine encephalitis virus (VEEV) remains a risk for epidemic emergence or use as an aerosolized bioweapon. To develop possible countermeasures, we isolated VEEV-specific neutralizing monoclonal antibodies (mAbs) from mice and a human immunized with attenuated VEEV strains. Functional assays and epitope mapping established that potently inhibitory anti-VEEV mAbs bind distinct antigenic sites in the A or B domains of the E2 glycoprotein and block multiple steps in the viral replication cycle including attachment, fusion, and egress. A 3.2-Å cryo-electron microscopy reconstruction of VEEV virus-like particles bound by a human Fab suggests that antibody engagement of the B domain may result in cross-linking of neighboring spikes to prevent conformational requirements for viral fusion. Prophylaxis or postexposure therapy with these mAbs protected mice against lethal aerosol challenge with VEEV. Our study defines functional and structural mechanisms of mAb protection and suggests that multiple antigenic determinants on VEEV can be targeted for vaccine or antibody-based therapeutic development.

Published

2021

20. Long-term persistence of viral RNA and inflammation in the CNS of macaques exposed to aerosolized Venezuelan equine encephalitis virus

Author

Katherine J. O’Malley, Joseph R. Albe, Matthew D. Dunn, Emily L. Cottle, Cynthia M. McMillen, Ivona Pandrea, Henry Ma, Noah Salama, William B. Klimstra, Tobias Teichert, Stacey Barrick, Theron Gilliland, Jeneveve D. Lundy, Douglas S. Reed, Devin A. Boyles, Christina L. Gardner, and Amy L. Hartman

Subjects

Central Nervous System, Chemokine, Immunology, Clone (cell biology), Alphavirus, medicine.disease_cause, Arbovirus, Microbiology, Virus, Encephalitis Virus, Venezuelan Equine, Virology, medicine, Genetics, Animals, Horses, Molecular Biology, Inflammation, biology, business.industry, Encephalomyelitis, Venezuelan Equine, medicine.disease, biology.organism_classification, Macaca fascicularis, Viral replication, Venezuelan equine encephalitis virus, biology.protein, RNA, Viral, Parasitology, business, Encephalitis

Abstract

Venezuelan equine encephalitis virus (VEEV) is a positively-stranded RNA arbovirus of the genus Alphavirus that causes encephalitis in humans. Cynomolgus macaques are a relevant model of the human disease caused by VEEV and are useful in exploring pathogenic mechanisms and the host response to VEEV infection. Macaques were exposed to small-particle aerosols containing virus derived from an infectious clone of VEEV strain INH-9813, a subtype IC strain isolated from a human infection. VEEV-exposed macaques developed a biphasic fever after infection similar to that seen in humans. Maximum temperature deviation correlated with the inhaled dose, but fever duration did not. Neurological signs, suggestive of virus penetration into the CNS, were predominantly seen in the second febrile period. Electroencephalography data indicated a statistically significant decrease in all power bands and circadian index during the second febrile period that returned to normal after fever resolved. Intracranial pressure increased late in the second febrile period. On day 6 post-infection macaques had high levels of MCP-1 and IP-10 chemokines in the CNS, as well as a marked increase of T lymphocytes and activated microglia. More than four weeks after infection, viral genomic RNA was found in the brain, cerebrospinal fluid and cervical lymph nodes. Pro-inflammatory cytokines & chemokines, infiltrating leukocytes and pathological changes were seen in the CNS tissues of macaques euthanized at these times. These data are consistent with persistence of virus replication and/or genomic RNA and potentially, inflammatory sequelae in the central nervous system after resolution of acute VEEV disease.

Published

2021

21. Protection of human ACE2 transgenic Syrian hamsters from SARS CoV-2 variants by human polyclonal IgG from hyper-immunized transchromosomic bovines

Author

Yutaka Terada, Maria Alcorn, Kristi A Egland, Theron Gilliland, Deanna Larson, Zhongde Wang, Shauna N. Vasilatos, Jeneveve D. Lundy, Eddie Sullivan, Thomas C. Luke, Rong Li, Christoph L Bausch, Zachary Ryckman, William B. Klimstra, Hua Wu, Emily L. Cottle, Matthew D. Dunn, and Yanan Liu

Subjects

biology, medicine.drug_class, Hamster, Monoclonal antibody, Virology, Article, Neutralization, Virus, Hyperimmunization, Ectodomain, biology.protein, medicine, Vero cell, Antibody

Abstract

Pandemic SARS CoV-2 has been undergoing rapid evolution during spread throughout the world resulting in the emergence of many Spike protein variants, some of which appear to either evade antibody neutralization, transmit more efficiently, or potentially exhibit increased virulence. This raises significant concerns regarding the long-term efficacy of protection elicited after primary infection and/or from vaccines derived from single virus Spike (S) genotypes, as well as the efficacy of anti-S monoclonal antibody based therapeutics. Here, we used fully human polyclonal human IgG (SAB-185), derived from hyperimmunization of transchromosomic bovines with DNA plasmids encoding the SARS-CoV-2 Wa-1 strain S protein or purified ectodomain of S protein, to examine the neutralizing capacity of SAB-185 in vitro and the protective efficacy of passive SAB-185 antibody (Ab) transfer in vivo. The Ab preparation was tested for neutralization against five variant SARS-CoV-2 strains: Munich (Spike D614G), UK (B.1.1.7), Brazil (P.1) and SA (B.1.3.5) variants, and a variant isolated from a chronically infected immunocompromised patient (Spike Δ144-146). For the in vivo studies, we used a new human ACE2 (hACE2) transgenic Syrian hamster model that exhibits lethality after SARS-Cov-2 challenge and the Munich, UK, SA and Δ144-146 variants. SAB-185 neutralized each of the SARS-CoV-2 strains equivalently on Vero E6 cells, however, a control convalescent human serum sample was less effective at neutralizing the SA variant. In the hamster model, prophylactic SAB-185 treatment protected the hamsters from fatal disease and minimized clinical signs of infection. These results suggest that SAB-185 may be an effective treatment for patients infected with SARS CoV-2 variants.

Published

2021

22. Human immunoglobulin from transchromosomic bovines hyperimmunized with SARS-CoV-2 spike antigen efficiently neutralizes viral variants

Author

Eddie Sullivan, Zhuoming Liu, Christoph L Bausch, Kristi A Egland, Theron C. Gilliland, Thomas C. Luke, Sean P. J. Whelan, Hua Wu, Matthew D. Dunn, and William B. Klimstra

Subjects

transchromosomic bovines, medicine.drug_class, viruses, Immunology, Monoclonal antibody, Antibodies, Viral, Neutralization, Antigen, Immunity, Neutralization Tests, medicine, Immunology and Allergy, Animals, Humans, polyclonal antibodies, skin and connective tissue diseases, Gene, Pharmacology, variants, biology, SARS-CoV-2, fungi, virus diseases, Antibodies, Monoclonal, COVID-19, biology.organism_classification, Virology, Antibodies, Neutralizing, body regions, Polyclonal antibodies, Vesicular stomatitis virus, Immunoglobulin G, Spike Glycoprotein, Coronavirus, biology.protein, Cattle, Antibody, Research Article, Research Paper

Abstract

Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) variants with amino-acid substitutions and deletions in spike protein (S) can reduce the effectiveness of monoclonal antibodies (mAbs) and may compromise immunity induced by vaccines. We report a polyclonal, fully human, anti-SARS-CoV-2 immunoglobulin produced in transchromosomic bovines (Tc-hIgG-SARS-CoV-2) hyperimmunized with two doses of plasmid DNA encoding the SARS-CoV-2 Wuhan strain S gene, followed by repeated immunization with S protein purified from insect cells. The resulting Tc-hIgG-SARS-CoV-2, termed SAB-185, efficiently neutralizes SARS-CoV-2, and vesicular stomatitis virus (VSV) SARS-CoV-2 chimerasin vitro. Neutralization potency was retained for S variants including S477N, E484K, and N501Y, substitutions present in recent variants of concern. In contrast to the ease of selection of escape variants with mAbs and convalescent human plasma, we were unable to isolate VSV-SARS-CoV-2 mutants resistant to Tc-hIgG-SARS-CoV-2 neutralization. This fully human immunoglobulin that potently inhibits SARS-CoV-2 infection may provide an effective therapeutic to combat COVID-19.

Published

2021

23. SARS-CoV-2 growth, furin-cleavage-site adaptation and neutralization using serum from acutely infected hospitalized COVID-19 patients

Author

Chengqun Sun, Sham Nambulli, Cynthia M. McMillen, Amy L. Hartman, Natasha L. Tilston-Lunel, Linda J. Rennick, W. Paul Duprex, James Boslett, Matthew D. Dunn, William B. Klimstra, Theron Gilliland, Anita K. McElroy, Alan Wells, Sarah E Wheeler, and Douglas S. Reed

Subjects

0301 basic medicine, clinical isolates, viruses, 030106 microbiology, adaptation, Virus Replication, Cleavage (embryo), Article, Virus, 03 medical and health sciences, Antigen, Neutralization Tests, Virology, Chlorocebus aethiops, Animals, Humans, Neutralizing antibody, Vero Cells, Furin, chemistry.chemical_classification, biology, Sequence Analysis, RNA, Animal, SARS-CoV-2, Genetic Variation, COVID-19, Viral Load, neutralization, Adaptation, Physiological, Antibodies, Neutralizing, In vitro, Immunoglobulin A, Hospitalization, 030104 developmental biology, chemistry, Immunoglobulin G, Host-Pathogen Interactions, Proteolysis, Vero cell, biology.protein, RNA, Viral, Positive-strand RNA Viruses, furin cleavage, Antibody, Glycoprotein, Research Article

Abstract

Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), the causative agent of coronavirus disease 2019 (COVID-19), emerged at the end of 2019 and by mid-June 2020 the virus had spread to at least 215 countries, caused more than 8 000 000 confirmed infections and over 450 000 deaths, and overwhelmed healthcare systems worldwide. Like severe acute respiratory syndrome coronavirus (SARS-CoV), which emerged in 2002 and caused a similar disease, SARS-CoV-2 is a betacoronavirus. Both viruses use human angiotensin-converting enzyme 2 (hACE2) as a receptor to enter cells. However, the SARS-CoV-2 spike (S) glycoprotein has a novel insertion that generates a putative furin cleavage signal and this has been postulated to expand the host range. Two low-passage (P) strains of SARS-CoV-2 (Wash1 : P4 and Munich : P1) were cultured twice in Vero E6 cells and characterized virologically. Sanger and MinION sequencing demonstrated significant deletions in the furin cleavage signal of Wash1 : P6 and minor variants in the Munich : P3 strain. Cleavage of the S glycoprotein in SARS-CoV-2-infected Vero E6 cell lysates was inefficient even when an intact furin cleavage signal was present. Indirect immunofluorescence demonstrated that the S glycoprotein reached the cell surface. Since the S protein is a major antigenic target for the development of neutralizing antibodies, we investigated the development of neutralizing antibody titres in serial serum samples obtained from COVID-19 human patients. These were comparable regardless of the presence of an intact or deleted furin cleavage signal. These studies illustrate the need to characterize virus stocks meticulously prior to performing either in vitro or in vivo pathogenesis studies.

Published

2020

24. Animal models for COVID-19

Author

Marco Cavaleri, Geraldine A. Hamilton, Lisa E. Gralinski, Juergen A. Richt, Emmie de Wit, Barney S. Graham, Michael Schotsaert, Matthew B. Frieman, Chien Te K. Tseng, Sander Herfst, Angela L. Rasmussen, Chad J. Roy, Koert J. Stittelaar, Amy L. Hartman, César Muñoz-Fontela, Anita K. McElroy, Suzanne J.F. Kaptein, Joana Rocha-Pereira, Júlia Vergara-Alert, Douglas S. Reed, Johan Neyts, Pauline Maisonnasse, Darryl Falzarano, Mark G. Lewis, Ian Crozier, Nadia Oreshkova, Kate Guilfoyle, Simon G. P. Funnell, Kai Dallmeier, W. Paul Duprex, Vincent J. Munster, Courtney L. Finch, Wen-Chun Liu, Joaquim Segalés, Pierre Stéphane Gsell, Martin Beer, Seshadri S. Vasan, Barry Rockx, William B. Klimstra, Hendrik Jan Thibaut, Ana Maria Henao-Restrepo, Bart L. Haagmans, Stanley Perlman, Roger Le Grand, Ivana Knezevic, Randy A. Albrecht, Ralph S. Baric, Trevor Brasel, Leen Delang, Jens H. Kuhn, Erik D. Dohm, Chuan Qin, Francisco J. Salguero, Leon de Waal, Philip R. Krause, A. Ximena Riveros-Balta, Thomas F. Rogers, William E. Dowling, Adolfo García-Sastre, Miles W. Carroll, Hanne Leth Andersen, Dan H. Barouch, Jasper Fuk-Woo Chan, Estefanía Rodríguez, Internal Medicine, Virology, Producció Animal, and Sanitat Animal

Subjects

0301 basic medicine, PATHOGENESIS, medicine.disease_cause, Mice, 0302 clinical medicine, RESPIRATORY SYNDROME CORONAVIRUS, Pandemic, INFECTION, Coronavirus, Multidisciplinary, biology, Respiratory infection, MOUSE MODEL, Virology & Molecular Biology, Multidisciplinary Sciences, Science & Technology - Other Topics, Coronavirus Infections, Primates, medicine.medical_specialty, COVID-19 Vaccines, Coronavirus disease 2019 (COVID-19), Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Pneumonia, Viral, SARS-COV-2, Article, Betacoronavirus, 03 medical and health sciences, Immunity, MERS, medicine, Animals, Humans, Life Science, Intensive care medicine, Pandemics, SARS, Science & Technology, Mesocricetus, SARS-CoV-2, business.industry, Ferrets, COVID-19, Viral Vaccines, biology.organism_classification, medicine.disease, EFFICACY, Virologie & Moleculaire Biologie, Disease Models, Animal, Pneumonia, MICE, 030104 developmental biology, business, RESERVOIRS, 030217 neurology & neurosurgery

Abstract

Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is the aetiological agent of coronavirus disease 2019 (COVID-19), an emerging respiratory infection caused by the introduction of a novel coronavirus into humans late in 2019 (first detected in Hubei province, China). As of 18 September 2020, SARS-CoV-2 has spread to 215 countries, has infected more than 30 million people and has caused more than 950,000 deaths. As humans do not have pre-existing immunity to SARS-CoV-2, there is an urgent need to develop therapeutic agents and vaccines to mitigate the current pandemic and to prevent the re-emergence of COVID-19. In February 2020, the World Health Organization (WHO) assembled an international panel to develop animal models for COVID-19 to accelerate the testing of vaccines and therapeutic agents. Here we summarize the findings to date and provides relevant information for preclinical testing of vaccine candidates and therapeutic agents for COVID-19. ispartof: NATURE vol:586 issue:7830 pages:509-515 ispartof: location:England status: published

Published

2020

25. SARS-CoV-2 infection of African green monkeys results in mild respiratory disease discernible by PET/CT imaging and shedding of infectious virus from both respiratory and gastrointestinal tracts

Author

JoAnne L. Flynn, Natasha L. Tilston-Lunel, Matthew S. Hartman, Matthew D. Dunn, Amy L. Hartman, Madeline M. Schwarz, Charles A. Scanga, Reagan C. Walker, Edwin Klein, Cynthia M. McMillen, Theron Gilliland, William B. Klimstra, Jaime A Tomko, Sham Nambulli, Mengying Xia, Douglas S. Reed, Emily L. Cottle, Emily L. Olsen, Katherine J. O’Malley, Anita K. McElroy, Joseph R. Albe, W. Paul Duprex, L. James Frye, and Alexander G. White

Subjects

RNA viruses, Viral Diseases, Pulmonology, Vaccine evaluation, Coronaviruses, viruses, Diagnostic Radiology, Medical Conditions, Positron Emission Tomography Computed Tomography, Chlorocebus aethiops, Gastrointestinal Infections, Respiratory system, Biology (General), Materials, Tomography, Lung, Pathology and laboratory medicine, Subclinical infection, 0303 health sciences, Radiology and Imaging, 030302 biochemistry & molecular biology, Respiratory disease, Medical microbiology, Pulmonary Imaging, Virus Shedding, Infectious Diseases, medicine.anatomical_structure, Viruses, Physical Sciences, SARS CoV 2, Pathogens, Coronavirus Infections, Viral load, Research Article, SARS coronavirus, Imaging Techniques, QH301-705.5, Materials Science, Pneumonia, Viral, Immunology, Neuroimaging, Gastroenterology and Hepatology, Research and Analysis Methods, Microbiology, Respiratory Disorders, Betacoronavirus, 03 medical and health sciences, Diagnostic Medicine, Virology, Genetics, medicine, Animals, Viral shedding, Pandemics, Molecular Biology, 030304 developmental biology, Medicine and health sciences, Aerosols, Biology and life sciences, SARS-CoV-2, business.industry, Organisms, Viral pathogens, COVID-19, Covid 19, RC581-607, medicine.disease, Microbial pathogens, Computed Axial Tomography, Gastrointestinal Tract, Mixtures, Respiratory Infections, Parasitology, African Green Monkey, Immunologic diseases. Allergy, business, Positron Emission Tomography, Neuroscience

Abstract

Vaccines are urgently needed to combat the global coronavirus disease 2019 (COVID-19) pandemic, and testing of candidate vaccines in an appropriate non-human primate (NHP) model is a critical step in the process. Infection of African green monkeys (AGM) with a low passage human isolate of SARS-CoV-2 by aerosol or mucosal exposure resulted in mild clinical infection with a transient decrease in lung tidal volume. Imaging with human clinical-grade 18F-fluoro-2-deoxy-D-glucose positron emission tomography (18F-FDG PET) co-registered with computed tomography (CT) revealed pulmonary lesions at 4 days post-infection (dpi) that resolved over time. Infectious virus was shed from both respiratory and gastrointestinal (GI) tracts in all animals in a biphasic manner, first between 2–7 dpi followed by a recrudescence at 14–21 dpi. Viral RNA (vRNA) was found throughout both respiratory and gastrointestinal systems at necropsy with higher levels of vRNA found within the GI tract tissues. All animals seroconverted simultaneously for IgM and IgG, which has also been documented in human COVID-19 cases. Young AGM represent an species to study mild/subclinical COVID-19 disease and with possible insights into live virus shedding. Future vaccine evaluation can be performed in AGM with correlates of efficacy being lung lesions by PET/CT, virus shedding, and tissue viral load., Author summary SARS-CoV-2 infection can result in asymptomatic, mild or severe disease in humans. Vaccines against SARS-CoV-2 are paramount for combating COVID-19 disease and curtailing the pandemic. Large animal models are critical for early vaccine testing before human clinical trials. Here, we found that infection of African green monkeys (AGM) with SARS-CoV-2 resulted in mild disease yet lesions were detectable by PET/CT imaging of the lungs. Shedding of infectious virus from both respiratory and gastrointestinal tracts was also documented. This study provides a detailed account of the pathogenesis of a low-passage SARS-CoV-2 isolate in the AGM model and suggests that AGM can be used for preclinical evaluation of candidate vaccines and therapeutic interventions.

Published

2020

26. Human Antibodies Protect against Aerosolized Eastern Equine Encephalitis Virus Infection

Author

Rachel E. Sutton, Rachel S. Nargi, Robert H. Carnahan, William B. Klimstra, Lauren E. Williamson, Elad Binshtein, Erica Armstrong, Theron Gilliland, Lauren M. Walker, Arthur S. Kim, James E. Crowe, Clarissa L Durie, Michael S. Diamond, Nurgun Kose, Pramod Kumar Yadav, Julie M. Fox, Melanie D. Ohi, and Robin G. Bombardi

Subjects

Adult, Encephalomyelitis, Equine, Models, Molecular, medicine.drug_class, Eastern equine encephalitis virus, Virulence, Biology, Monoclonal antibody, medicine.disease_cause, Antibodies, Viral, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Epitopes, Mice, 0302 clinical medicine, Protein Domains, Neutralization Tests, medicine, Animals, Humans, Antigens, Viral, Aerosolization, 030304 developmental biology, Glycoproteins, Aerosols, 0303 health sciences, Cryoelectron Microscopy, Virion, Antibodies, Monoclonal, Virus Internalization, medicine.disease, Virology, Antibodies, Neutralizing, Recombinant Proteins, Disease Models, Animal, Mutagenesis, Monoclonal, biology.protein, Encephalitis Virus, Eastern Equine, Female, Sindbis Virus, Antibody, 030217 neurology & neurosurgery, Encephalitis, Protein Binding

Abstract

Eastern equine encephalitis virus (EEEV) is one of the most virulent viruses endemic to North America. No licensed vaccines or antiviral therapeutics are available to combat this infection, which has recently shown an increase in human cases. Here, we characterize human monoclonal antibodies (mAbs) isolated from a survivor of natural EEEV infection with potent (

Published

2020

27. SARS-CoV-2 infection of African green monkeys results in mild respiratory disease discernible by PET/CT imaging and prolonged shedding of infectious virus from both respiratory and gastrointestinal tracts

Author

Theron Gilliland, Lonnie Frye, Charles A. Scanga, Mengying Xia, Matthew D. Dunn, Emily L. Olsen, Shamkumar Nambulli, Matthew S. Hartman, Anita K. McElroy, Amy L. Hartman, Alexander G. White, Madeline M. Schwarz, Douglas S. Reed, Jaime A Tomko, JoAnne L. Flynn, Reagan C. Walker, Natasha L. Tilston-Lunel, Cynthia M. McMillen, William B. Klimstra, Edwin Klein, Emily L. Cottle, Joseph R. Albe, Katherine J. O’Malley, and W. Paul Duprex

Subjects

Lung, medicine.diagnostic_test, business.industry, Respiratory disease, Disease, medicine.disease, Virology, medicine.anatomical_structure, Positron emission tomography, medicine, African Green Monkey, Viral shedding, Respiratory system, business, Subclinical infection

Abstract

Vaccines are urgently needed to combat the global coronavirus disease 2019 (COVID-19) pandemic, and testing of candidate vaccines in an appropriate non-human primate (NHP) model is a critical step in the process. Infection of African green monkeys (AGM) with a low passage human isolate of SARS-CoV-2 by aerosol or mucosal exposure resulted in mild clinical infection with a transient decrease in lung tidal volume. Imaging with human clinical-grade18F-fluoro-2-deoxy-D-glucose positron emission tomography (18F-FDG PET) co-registered with computed tomography (CT) revealed pulmonary lesions at 4 days post-infection (dpi) that resolved over time. Infectious virus was shed from both respiratory and gastrointestinal (GI) tracts in all animals in a biphasic manner, first between 2-7 dpi followed by a recrudescence at 14-21 dpi. Viral RNA (vRNA) was found throughout both respiratory and gastrointestinal systems at necropsy with higher levels of vRNA found within the GI tract tissues. All animals seroconverted simultaneously for IgM and IgG, which has also been documented in human COVID-19 cases. Young AGM represent an excellent species to study mild/subclinical COVID-19 disease and have shed light on unknown aspects of long-term virus shedding. They are ideally suited for preclinical evaluation of candidate vaccines and therapeutic interventions.One Sentence SummarySubclinical infection of African green monkeys infected with SARS-CoV-2 results in prolonged shedding of infectious virus from both respiratory and gastrointestinal tracts.

Published

2020

28. Comparative dynamic aerosol efficiencies of three emergent coronaviruses and the unusual persistence of SARS-CoV-2 in aerosol suspensions

Author

Allison L. Totura, Douglas S. Reed, Alyssa C. Fears, Ken C. Plante, Scott C. Weaver, Aysegul Nalca, Robert F. Garry, J. Kyle Bohannon, Diana Fernández, William B. Klimstra, David N Dyer, Amy L. Hartman, Chad J. Roy, Divya Mirchandani, Reed F. Johnson, Matthew G. Lackemeyer, Brian J. Kearney, Patricia V. Aguilar, Paul Duprex, and Jessica A. Plante

Subjects

aerosol, viruses, Expedited, Middle Eastern Respiratory Syndrome, 010501 environmental sciences, medicine.disease_cause, 01 natural sciences, Persistence (computer science), MERS-CoV, Persistence of Severe Acute Respiratory Syndrome Coronavirus 2 in Aerosol Suspensions, Coronavirus, Infectivity, 0303 health sciences, education.field_of_study, respiratory diseases, Dispatch, virus diseases, SARS-CoV, respiratory system, 3. Good health, Coronavirus Infections, severe acute respiratory syndrome coronavirus 2, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Population, Pneumonia, Viral, macromolecular substances, Biology, complex mixtures, Article, 2019 novel coronavirus disease, 03 medical and health sciences, Betacoronavirus, Suspensions, medicine, Disease Transmission, Infectious, Humans, coronavirus diseases, education, Zoonotic pathogen, Pandemics, 030304 developmental biology, 0105 earth and related environmental sciences, Aerosols, severe acute respiratory syndrome coronavirus, SARS-CoV-2, COVID-19, biochemical phenomena, metabolism, and nutrition, Virology, respiratory tract diseases, Aerosol, zoonoses, nervous system, Middle East respiratory syndrome coronavirus

Abstract

The emergent coronavirus, designated severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2), is a zoonotic pathogen that has demonstrated remarkable transmissibility in the human population and is the etiological agent of a current global pandemic called COVID-191. We measured the dynamic (short-term) aerosol efficiencies of SARS-CoV-2 and compared the efficiencies with two other emerging coronaviruses, SARS-CoV (emerged in 2002) and Middle Eastern respiratory syndrome CoV (MERS-CoV; emerged starting in 2012). We also quantified the long-term persistence of SARS-CoV-2 and its ability to maintain infectivity when suspended in aerosols for up to 16 hours.

Published

2020

29. Applications of minimally invasive multimodal telemetry for continuous monitoring of brain function and intracranial pressure in macaques with acute viral encephalitis

Author

Amy L. Hartman, William B. Klimstra, Douglas S. Reed, Katherine J. O’Malley, Anita M. Trichel, Henry Ma, Emily L. Cottle, Tobias Teichert, and Jeneveve D. Lundy

Subjects

0301 basic medicine, Male, RNA viruses, Eastern Equine Encephalitis Virus, Intracranial Pressure, Medical Implants, Eastern equine encephalitis virus, Physiology, Fevers, Electroencephalography, Monkeys, medicine.disease_cause, Pathology and Laboratory Medicine, Macaque, Severity of Illness Index, 0302 clinical medicine, Infectious Diseases of the Nervous System, Medicine and Health Sciences, Telemetry, Encephalitis, Viral, Intracranial pressure, Mammals, Clinical Neurophysiology, Brain Mapping, Multidisciplinary, biology, medicine.diagnostic_test, Brain, Eukaryota, Circadian Rhythm, Electrophysiology, Circadian Rhythms, Bioassays and Physiological Analysis, Infectious Diseases, Brain Electrophysiology, Neurology, Medical Microbiology, Viral Pathogens, Vertebrates, Viruses, Medicine, Encephalitis, Engineering and Technology, Female, Pathogens, Research Article, Biotechnology, Primates, Imaging Techniques, Science, Alphaviruses, Neurophysiology, Neuroimaging, Bioengineering, Alphavirus, Research and Analysis Methods, Microbiology, Virus, Togaviruses, 03 medical and health sciences, Signs and Symptoms, Diagnostic Medicine, biology.animal, Old World monkeys, medicine, Animals, Circadian rhythm, Alphavirus infection, Microbial Pathogens, Biology and life sciences, business.industry, Alphavirus Infections, Electrophysiological Techniques, Organisms, medicine.disease, Disease Models, Animal, 030104 developmental biology, Venezuelan equine encephalitis virus, Immunology, Amniotes, Macaca, Medical Devices and Equipment, Clinical Medicine, business, Chronobiology, 030217 neurology & neurosurgery, Biomarkers, Neuroscience

Abstract

Alphaviruses such as Venezuelan equine encephalitis virus (VEEV) and Eastern equine encephalitis virus (EEEV) are arboviruses that can cause severe zoonotic disease in humans. Both VEEV and EEEV are highly infectious when aerosolized and can be used as biological weapons. Vaccines and therapeutics are urgently needed, but efficacy determination requires animal models. The cynomolgus macaque (Macaca fascicularis) provides a relevant model of human disease, but questions remain whether vaccines or therapeutics can mitigate CNS infection or disease in this model. The documentation of alphavirus encephalitis in animals relies on traditional physiological biomarkers and behavioral/neurological observations by veterinary staff; quantitative measurements such as electroencephalography (EEG) and intracranial pressure (ICP) can recapitulate underlying encephalitic processes. We detail a telemetry implantation method suitable for continuous monitoring of both EEG and ICP in awake macaques, as well as methods for collection and analysis of such data. We sought to evaluate whether changes in EEG/ICP suggestive of CNS penetration by virus would be seen after aerosol exposure of naïve macaques to VEEV IC INH9813 or EEEV V105 strains compared to mock-infection in a cohort of twelve adult cynomolgus macaques. Data collection ran continuously from at least four days preceding aerosol exposure and up to 50 days thereafter. EEG signals were processed into frequency spectrum bands (delta: [0.4 – 4Hz); theta: [4 – 8Hz); alpha: [8-12Hz); beta: [12-30] Hz) and assessed for viral encephalitis-associated changes against robust background circadian variation while ICP data was assessed for signal fidelity, circadian variability, and for meaningful differences during encephalitis. Results indicated differences in delta, alpha, and beta band magnitude in infected macaques, disrupted circadian rhythm, and proportional increases in ICP in response to alphavirus infection. This novel enhancement of the cynomolgus macaque model offers utility for timely determination of onset, severity, and resolution of encephalitic disease and for the evaluation of vaccine and therapeutic candidates.

Published

2020

30. Cryo-EM structure of eastern equine encephalitis virus in complex with heparan sulfate analogues

Author

Chengqun Sun, Yingyuan Sun, William B. Klimstra, Geeta Buda, Michael G. Rossmann, Chun-Liang Chen, Thomas Klose, and S. Saif Hasan

Subjects

Encephalomyelitis, Equine, Cryo-electron microscopy, Eastern equine encephalitis virus, Virus Attachment, Alphavirus, medicine.disease_cause, Antiviral Agents, Cell Line, 03 medical and health sciences, chemistry.chemical_compound, Structure-Activity Relationship, Viral envelope, Viral Envelope Proteins, Viral entry, medicine, Animals, Humans, Binding site, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Multidisciplinary, Binding Sites, biology, Mesocricetus, Molecular Structure, Heparin, 030302 biochemistry & molecular biology, Chondroitin Sulfates, Cryoelectron Microscopy, Heparan sulfate, biology.organism_classification, Virology, chemistry, PNAS Plus, Drug Design, Encephalitis Virus, Eastern Equine, Glycoprotein, Heparan Sulfate Proteoglycans

Abstract

Eastern equine encephalitis virus (EEEV), a mosquito-borne icosahedral alphavirus found mainly in North America, causes human and equine neurotropic infections. EEEV neurovirulence is influenced by the interaction of the viral envelope protein E2 with heparan sulfate (HS) proteoglycans from the host’s plasma membrane during virus entry. Here, we present a 5.8-Å cryoelectron microscopy (cryo-EM) structure of EEEV complexed with the HS analog heparin. “Peripheral” HS binding sites were found to be associated with the base of each of the E2 glycoproteins that form the 60 quasi-threefold spikes (q3) and the 20 sites associated with the icosahedral threefold axes (i3). In addition, there is one HS site at the vertex of each q3 and i3 spike (the “axial” sites). Both the axial and peripheral sites are surrounded by basic residues, suggesting an electrostatic mechanism for HS binding. These residues are highly conserved among EEEV strains, and therefore a change in these residues might be linked to EEEV neurovirulence.

Published

2020

31. Protective antibodies against Eastern equine encephalitis virus bind to epitopes in domains A and B of the E2 glycoprotein

Author

Arthur S. Kim, S. Kyle Austin, Derek W. Trobaugh, Mark K. Slifka, Lauren E. Williamson, Daved H. Fremont, Michael S. Diamond, Adam Zuiani, Douglas S. Reed, Chengqun Sun, Christina L. Gardner, James E. Crowe, William B. Klimstra, and Katherine Basore

Subjects

Microbiology (medical), Encephalomyelitis, Equine, Eastern equine encephalitis virus, medicine.drug_class, Immunology, Alphavirus, medicine.disease_cause, Monoclonal antibody, Antibodies, Viral, Applied Microbiology and Biotechnology, Microbiology, Epitope, Neutralization, Article, 03 medical and health sciences, Epitopes, Mice, Protein Domains, Viral Envelope Proteins, Cricetinae, Chlorocebus aethiops, Genetics, medicine, Animals, Humans, Vero Cells, 030304 developmental biology, 0303 health sciences, biology, 030306 microbiology, Antibodies, Monoclonal, Cell Biology, biology.organism_classification, Virology, Antibodies, Neutralizing, 3. Good health, Epitope mapping, HEK293 Cells, Vero cell, biology.protein, Encephalitis Virus, Eastern Equine, Female, Antibody, Epitope Mapping

Abstract

Eastern equine encephalitis virus (EEEV) is a mosquito-transmitted alphavirus with a high case mortality rate in humans. EEEV is a biodefence concern because of its potential for aerosol spread and the lack of existing countermeasures. Here, we identify a panel of 18 neutralizing murine monoclonal antibodies (mAbs) against the EEEV E2 glycoprotein, several of which have 'elite' activity with 50 and 99% effective inhibitory concentrations (EC50 and EC99) of less than 10 and 100 ng ml-1, respectively. Alanine-scanning mutagenesis and neutralization escape mapping analysis revealed epitopes for these mAbs in domains A or B of the E2 glycoprotein. A majority of the neutralizing mAbs blocked infection at a post-attachment stage, with several inhibiting viral membrane fusion. Administration of one dose of anti-EEEV mAb protected mice from lethal subcutaneous or aerosol challenge. These experiments define the mechanistic basis for neutralization by protective anti-EEEV mAbs and suggest a path forward for treatment and vaccine design.

Published

2018

32. Mxra8 is a receptor for multiple arthritogenic alphaviruses

Author

Subhajit Poddar, Rong Zhang, Hueylie Lin, Daved H. Fremont, Rachel H. Fong, Arthur S. Kim, William B. Klimstra, Julie M. Fox, James E. Crowe, Katherine Basore, Benjamin J. Doranz, Rebecca Rimkunas, Michael S. Diamond, and Sharmila Nair

Subjects

Male, 0301 basic medicine, medicine.drug_class, viruses, Information Storage and Retrieval, Immunoglobulins, Mutagenesis (molecular biology technique), Alphavirus, Receptors, Fc, Monoclonal antibody, medicine.disease_cause, Article, Virus, Mice, 03 medical and health sciences, Chondrocytes, medicine, Animals, Humans, O'nyong-nyong Virus, Chikungunya, Antibodies, Blocking, Muscle, Skeletal, Receptor, Vaccines, Osteoblasts, Multidisciplinary, biology, Cell adhesion molecule, Publications, Membrane Proteins, virus diseases, 3T3 Cells, Fibroblasts, biology.organism_classification, Fusion protein, Virology, 3. Good health, 030104 developmental biology, Receptors, Virus, CRISPR-Cas Systems, Chikungunya virus

Abstract

Arthritogenic alphaviruses comprise a group of enveloped RNA viruses that are transmitted to humans by mosquitoes and cause debilitating acute and chronic musculoskeletal disease 1 . The host factors required for alphavirus entry remain poorly characterized 2 . Here we use a genome-wide CRISPR–Cas9-based screen to identify the cell adhesion molecule Mxra8 as an entry mediator for multiple emerging arthritogenic alphaviruses, including chikungunya, Ross River, Mayaro and O’nyong nyong viruses. Gene editing of mouse Mxra8 or human MXRA8 resulted in reduced levels of viral infection of cells and, reciprocally, ectopic expression of these genes resulted in increased infection. Mxra8 bound directly to chikungunya virus particles and enhanced virus attachment and internalization into cells. Consistent with these findings, Mxra8–Fc fusion protein or anti-Mxra8 monoclonal antibodies blocked chikungunya virus infection in multiple cell types, including primary human synovial fibroblasts, osteoblasts, chondrocytes and skeletal muscle cells. Mutagenesis experiments suggest that Mxra8 binds to a surface-exposed region across the A and B domains of chikungunya virus E2 protein, which are a speculated site of attachment. Finally, administration of the Mxra8–Fc protein or anti-Mxra8 blocking antibodies to mice reduced chikungunya and O’nyong nyong virus infection as well as associated foot swelling. Pharmacological targeting of Mxra8 could form a strategy for mitigating infection and disease by multiple arthritogenic alphaviruses. The cell adhesion molecule Mxra8 is identified as a receptor for multiple arthritogenic alphaviruses such as chikungunya virus, and anti-Mxra8 monoclonal antibodies are shown to reduce rates of chikungunya virus infection in mice and a range of human cells.

Published

2018

33. Therapeutic alphavirus cross-reactive E1 human antibodies inhibit viral egress

Author

Jens Meiler, Robert H. Carnahan, Nurgun Kose, Erica Armstrong, Joseph X. Reidy, Kevin L. Schey, Rachel E. Sutton, James E. Crowe, Kristen M. Reeder, Minh H. Tran, Lauren E. Williamson, Rachel S. Nargi, Benjamin J. Doranz, Edgar Davidson, Arthur S. Kim, William B. Klimstra, W. Hayes McDonald, Andrew Trivette, Mallorie E. Fouch, Michael S. Diamond, Vicky Roy, Kevin W. Bailey, Emma S. Winkler, Galit Alter, Christopher Gainza, Justin G. Julander, Jessica Rodriguez, and Clara T. Schoeder

Subjects

Encephalomyelitis, Equine, Male, Eastern equine encephalitis virus, medicine.drug_class, viruses, Alphavirus, Receptors, Fc, Cross Reactions, Antibodies, Viral, medicine.disease_cause, Monoclonal antibody, Models, Biological, Article, General Biochemistry, Genetics and Molecular Biology, Epitope, Cell Line, Viral Proteins, Immunity, medicine, Animals, Humans, Horses, Antigens, Viral, Virus Release, chemistry.chemical_classification, biology, Temperature, Virion, Antibodies, Monoclonal, Hydrogen-Ion Concentration, Virus Internalization, biology.organism_classification, Antibodies, Neutralizing, Virology, Mice, Inbred C57BL, Epitope mapping, chemistry, biology.protein, Encephalitis Virus, Eastern Equine, RNA, Viral, Female, Joints, Antibody, Glycoprotein, Chikungunya virus, Epitope Mapping, Protein Binding

Abstract

Summary Alphaviruses cause severe arthritogenic or encephalitic disease. The E1 structural glycoprotein is highly conserved in these viruses and mediates viral fusion with host cells. However, the role of antibody responses to the E1 protein in immunity is poorly understood. We isolated E1-specific human monoclonal antibodies (mAbs) with diverse patterns of recognition for alphaviruses (ranging from Eastern equine encephalitis virus [EEEV]-specific to alphavirus cross-reactive) from survivors of natural EEEV infection. Antibody binding patterns and epitope mapping experiments identified differences in E1 reactivity based on exposure of epitopes on the glycoprotein through pH-dependent mechanisms or presentation on the cell surface prior to virus egress. Therapeutic efficacy in vivo of these mAbs corresponded with potency of virus egress inhibition in vitro and did not require Fc-mediated effector functions for treatment against subcutaneous EEEV challenge. These studies reveal the molecular basis for broad and protective antibody responses to alphavirus E1 proteins.

Published

2021

34. Pan-protective anti-alphavirus human antibodies target a conserved E1 protein epitope

Author

Natasha M. Kafai, Lo Vang, Lauren E. Williamson, Michael S. Diamond, Prashant N. Jethva, Michael L. Gross, Arthur S. Kim, William B. Klimstra, Paulina Kaplonek, Jose A. Quiroz, Daved H. Fremont, Aadit P. Shah, Matthias Mack, Emma S. Winkler, Jonathan R. Lai, Benjamin J. Doranz, Galit Alter, Emily L. Cottle, James E. Crowe, Ryan J. Malonis, Theron C. Gilliland, Edgar Davidson, Rachel H. Fong, and James T. Earnest

Subjects

Male, medicine.drug_class, viruses, medicine.medical_treatment, Alphavirus, Antibodies, Viral, Monoclonal antibody, medicine.disease_cause, Models, Biological, Monocytes, Article, General Biochemistry, Genetics and Molecular Biology, Epitope, Epitopes, Viral Proteins, Immunity, Chlorocebus aethiops, medicine, Animals, Humans, Amino Acid Sequence, Chikungunya, Vero Cells, Conserved Sequence, Virus Release, biology, Alphavirus Infections, Antibodies, Monoclonal, virus diseases, Immunotherapy, medicine.disease, biology.organism_classification, Virology, Mice, Inbred C57BL, biology.protein, Chikungunya Fever, Antibody, Chikungunya virus, Epitope Mapping, Encephalitis

Abstract

Alphaviruses are emerging, mosquito-transmitted pathogens that cause musculoskeletal and neurological disease in humans. Although neutralizing antibodies that inhibit individual alphaviruses have been described, broadly reactive antibodies that protect against both arthritogenic and encephalitic alphaviruses have not been reported. Here, we identify DC2.112 and DC2.315, two pan-protective yet poorly neutralizing human monoclonal antibodies (mAbs) that avidly bind to viral antigen on the surface of cells infected with arthritogenic and encephalitic alphaviruses. These mAbs engage a conserved epitope in domain II of the E1 protein proximal to and within the fusion peptide. Treatment with DC2.112 or DC2.315 protects mice against infection by both arthritogenic (chikungunya and Mayaro) and encephalitic (Venezuelan, Eastern, and Western equine encephalitis) alphaviruses through multiple mechanisms, including inhibition of viral egress and monocyte-dependent Fc effector functions. These findings define a conserved epitope recognized by weakly neutralizing yet protective antibodies that could be targeted for pan-alphavirus immunotherapy and vaccine design.

Published

2021

35. The expression level of C19MC miRNAs in early pregnancy and in response to viral infection

Author

Jacob C. Larkin, Christina L. Gardner, Anna Binstock, Tina Dumont, Jean-Francois Mouillet, Joseph S. Sanfilippo, Fabiola Balmir, Carolyn B. Coyne, Avaraham Bayer, William B. Klimstra, Simcha Yagel, Dana G. Wolf, and Yoel Sadovsky

Subjects

0301 basic medicine, Amniotic fluid, Primary Cell Culture, Mice, Transgenic, Fertilization in Vitro, Article, 03 medical and health sciences, Pregnancy, microRNA, Togaviridae, medicine, Animals, Humans, Gene silencing, Embryo Implantation, Longitudinal Studies, Prospective Studies, Pregnancy Complications, Infectious, biology, Obstetrics and Gynecology, Trophoblast, Vesiculovirus, Amniotic Fluid, biology.organism_classification, medicine.disease, MicroRNAs, 030104 developmental biology, medicine.anatomical_structure, Reproductive Medicine, Viral replication, Vesicular stomatitis virus, Cytomegalovirus Infections, Immunology, Female, Chromosomes, Human, Pair 19, Developmental Biology

Abstract

Introduction We have previously shown that miRNAs produced from the Chromosome 19 MiRNA Cluster (C19MC), which are expressed almost exclusively in primate trophoblasts and are released into the maternal circulation, reduce viral replication in non-placental cells and can modulate migratory behavior of extravillous trophoblast. We sought to define the expression pattern of C19MC miRNA in early pregnancy and in response to viral infection in vitro and in vivo . Methods We prospectively followed women undergoing in vitro fertilization (IVF) and determined their blood level of C19MC miRNA using RT-qPCR. To examine the effect of viral exposure on C19MC miRNAs expression, we used three systems: (1) a transgenic mouse overexpressing the C19MC cluster and exposed to Togaviridae during pregnancy, (2) cultured primary human trophoblasts exposed to Vesicular Stomatitis Virus in vitro , and (3) amniotic fluid from women exposed to cytomegalovirus during pregnancy. Results In 27 IVF pregnancies, C19MC miRNAs were detected as early as 2 weeks after implantation, and their levels increased thereafter. There was no change in C19MC miRNA expression levels in the mouse placenta in response to viral exposure. Similarly, Vesicular Stomatitis Virus infection of primary human trophoblast did not selectively increase C19MC miRNA expression. C19MC miRNA expression in the amniotic fluid was not affected by vertical transmission of cytomegalovirus. Discussion The expression of C19MC miRNAs in maternal circulation very early in pregnancy suggests a role in the establishment of the maternal-fetal interface. The levels of C19MC miRNA are not influenced by diverse types of viral infection.

Published

2017

36. Alphaviruses suppress host immunity by preventing myeloid cell replication and antagonizing innate immune responses

Author

William B. Klimstra and Derek W. Trobaugh

Subjects

0301 basic medicine, Myeloid, viruses, Alphavirus, Adaptive Immunity, Article, Virus, 03 medical and health sciences, Immune system, Immunity, Virology, medicine, Animals, Humans, Myeloid Cells, Cell Proliferation, Immune Evasion, Innate immune system, 030102 biochemistry & molecular biology, biology, biochemical phenomena, metabolism, and nutrition, Acquired immune system, biology.organism_classification, Immunity, Innate, 030104 developmental biology, medicine.anatomical_structure, Viral replication, Host-Pathogen Interactions, Immunology

Abstract

Alphaviruses are medically important mosquito-borne viruses that cause a range of diseases in humans from febrile illness to arthritis or encephalitis. The innate immune response functions to suppress virus replication through upregulation of antiviral molecules and contributes to development of the adaptive immune response. Myeloid cells act as master regulators of virus infection by initiating both the innate and adaptive immune responses. Alphaviruses are capable of antagonizing individual components of these responses to increase replicative fitness in vivo. However, recently, studies have demonstrated that some alphaviruses avoid myeloid cell replication altogether to achieve a similar effect. In this review, we summarize how alphaviruses evade myeloid cell infection and individual inductive mechanisms, thereby limiting the activation of the innate immune response.

Published

2017

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

Author

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

Subjects

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

Abstract

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

Published

2019

38. Encephalitic alphaviruses exploit caveolae-mediated transcytosis at the blood-brain barrier for CNS entry

Author

Robyn Roth, William B. Klimstra, Jianghui Hou, Wandy L. Beatty, Robyn S. Klein, Matthew D. Cain, Chengqun Sun, Xiaoping Jiang, and Hamid Salimi

Subjects

education.field_of_study, biology, Immunoelectron microscopy, viruses, Population, Alphavirus, Blood–brain barrier, biology.organism_classification, Virology, Virus, medicine.anatomical_structure, Transcytosis, Viral replication, Viral entry, medicine, cardiovascular system, education

Abstract

Venezuelan and Western equine encephalitis viruses (VEEV and WEEV) invade the CNS early during infection, via neuronal and hematogenous routes (1, 2). While viral replication mediates host-shut off, including expression of type I interferons (IFN) (3, 4), few studies have addressed how alphaviruses gain access to the CNS during established infection or the mechanisms of viral crossing at the blood-brain barrier (BBB). Here, we show that hematogenous dissemination of VEEV and WEEV into the CNS occurs via caveolin (Cav)-1-mediated transcytosis (Cav-MT) across an intact BBB, which is impeded by IFN and inhibitors of RhoA GTPase. Use of reporter and non-replicative strains also demonstrates that IFN signaling mediates viral restriction within cells comprising the neurovascular unit (NVU), differentially rendering brain endothelial cells, pericytes and astrocytes permissive to viral replication. Transmission and immunoelectron microscopy revealed early events in virus internalization and Cav-1-association within brain endothelial cells. Cav-1-deficient mice exhibit diminished CNS VEEV and WEEV titers during early infection, whereas viral burdens in peripheral tissues remained unchanged. Our findings show that alphaviruses exploit Cav-MT to enter the CNS, and that IFN differentially restricts this process at the BBB.ImportanceVEEV, WEEV and EEEV are emerging infectious diseases in the Americas, and they have caused several major outbreaks in the human and horse population during the past few decades. Shortly after infection, these viruses can infect the CNS, resulting in severe long-term neurological deficits or death. Neuroinvasion has been associated with virus entry into the CNS directly from the blood-stream, however the underlying molecular mechanisms have remained largely unknown. Here we demonstrate that following peripheral infection alphavirus augments vesicular formation/trafficking at the BBB and utilizes Cav-MT to cross an intact BBB, a process regulated by activators of Rho GTPAses within brain endothelium.In vivoexamination of early viral entry in Cav-1-deficient mice revealed significantly lower viral burdens than in similarly infected wild-type animals. These studies identify a potentially targetable pathway to limit neuroinvasion by alphaviruses.

Published

2019

39. Electrocardiography Abnormalities in Macaques after Infection with Encephalitic Alphaviruses

Author

Amy L. Hartman, Henry Ma, Katherine J. O’Malley, Jeneveve D. Lundy, William B. Klimstra, and Douglas S. Reed

Subjects

0301 basic medicine, Microbiology (medical), aerosol, viruses, nonhuman primates, electrocardiography, ecg, encephalitis, 030106 microbiology, lcsh:Medicine, Disease, Alphavirus, Arbovirus, Article, 03 medical and health sciences, vaccine, Immunology and Allergy, alphavirus, Medicine, Heart rate variability, Circadian rhythm, Molecular Biology, Equine Encephalitis, equine, General Immunology and Microbiology, medicine.diagnostic_test, biology, business.industry, fungi, lcsh:R, virus diseases, medicine.disease, biology.organism_classification, animal models, virology, 030104 developmental biology, Infectious Diseases, arbovirus, Immunology, business, Electrocardiography, Encephalitis

Abstract

Eastern (EEEV) and Venezuelan (VEEV) equine encephalitis viruses (EEVs) are related, (+) ssRNA arboviruses that can cause severe, sometimes fatal, encephalitis in humans. EEVs are highly infectious when aerosolized, raising concerns for potential use as biological weapons. No licensed medical countermeasures exist, given the severity/rarity of natural EEV infections, efficacy studies require animal models. Cynomolgus macaques exposed to EEV aerosols develop fever, encephalitis, and other clinical signs similar to humans. Fever is nonspecific for encephalitis in macaques. Electrocardiography (ECG) metrics may predict onset, severity, or outcome of EEV-attributable disease. Macaques were implanted with thermometry/ECG radiotransmitters and exposed to aerosolized EEV. Data was collected continuously, and repeated-measures ANOVA and frequency-spectrum analyses identified differences between courses of illness and between pre-exposure and post-exposure states. EEEV-infected macaques manifested widened QRS-intervals in severely ill subjects post-exposure. Moreover, QT-intervals and RR-intervals decreased during the febrile period. VEEV-infected macaques suffered decreased QT-intervals and RR-intervals with fever onset. Frequency-spectrum analyses revealed differences in the fundamental frequencies of multiple metrics in the post-exposure and febrile periods compared to baseline and confirmed circadian dysfunction. Heart rate variability (HRV) analyses revealed diminished variability post-exposure. These analyses support using ECG data alongside fever and clinical laboratory findings for evaluating medical countermeasure efficacy.

Published

2019

40. A Vibrating Mesh Nebulizer as an Alternative to the Collison Three-Jet Nebulizer for Infectious Disease Aerobiology

Author

Jennifer D. Bowling, Katherine J. O’Malley, Douglas S. Reed, William B. Klimstra, and Amy L. Hartman

Subjects

Microbiological Techniques, Indoor bioaerosol, Applied Microbiology and Biotechnology, complex mixtures, 03 medical and health sciences, medicine, Methods, Particle Size, Aerosolization, Francisella tularensis, 030304 developmental biology, Aerosols, 0303 health sciences, Ecology, biology, 030306 microbiology, business.industry, Nebulizers and Vaporizers, Respiratory infection, respiratory system, biology.organism_classification, Aerosol, Nebulizer, medicine.anatomical_structure, Infectious disease (medical specialty), Immunology, business, Food Science, Biotechnology, Respiratory tract

Abstract

Experimental infection of animals with aerosols containing pathogenic agents is essential for an understanding of the natural history and pathogenesis of infectious disease as well as evaluation of potential treatments. We evaluated whether the Aeroneb nebulizer, a vibrating mesh nebulizer, would serve as an alternative to the Collison nebulizer, the “gold standard” for generating infectious bioaerosols. While the Collison possesses desirable properties that have contributed to its longevity in infectious disease aerobiology, concerns have lingered about the liquid volume and concentration of the infectious agent required to cause disease and the damage that jet nebulization causes to the agent. Fluorescein salt was added to the nebulizer contents to assess pathogen loss during aerosolization. Relative to fluorescein salt, loss of influenza virus during aerosolization was worse with the Collison than with the Aeroneb. Four other viruses also had superior aerosol performance with the Aeroneb. The Aeroneb did not improve the aerosol performance for a vegetative bacterium, Francisella tularensis. Environmental parameters collected during the aerosol challenges indicated that the Aeroneb generated a higher relative humidity in exposure chambers while not affecting other environmental parameters. The aerosol mass median aerodynamic diameter (MMAD) was generally larger and more disperse for aerosols generated by the Aeroneb than what is seen with the Collison, but ≥80% of particles were within the range that would reach the lower respiratory tract and alveolar regions. The improved aerosol performance and generated particle size range suggest that for viral pathogens, the Aeroneb is a suitable alternative to the Collison three-jet nebulizer for use in experimental infection of animals. IMPORTANCE Respiratory infection by pathogens via aerosol remains a major concern for both natural disease transmission as well as intentional release of biological weapons. Critical to understanding the disease course and pathogenesis of inhaled pathogens are studies in animal models conducted under tightly controlled experimental settings, including the inhaled dose. The route of administration, particle size, and dose can affect disease progression and outcome. Damage to or loss of pathogens during aerosolization could increase the dose required to cause disease and could stimulate innate immune responses, altering outcome. Aerosol generators that reduce pathogen loss would be ideal. This study compares two aerosol generators to determine which is superior for animal studies. Aerosol research methods and equipment need to be well characterized to optimize the development of animal models for respiratory pathogens, including bioterrorism agents. This information will be critical for pivotal efficacy studies in animals to evaluate potential vaccines or treatments against these agents.

Published

2019

41. Approach to Strain Selection and the Propagation of Viral Stocks for Venezuelan Equine Encephalitis Virus Vaccine Efficacy Testing under the Animal Rule

Author

Farooq Nasar, William B. Klimstra, Lucy A. Ward, Scott C. Weaver, Andrew M. Glenn, Carol L. K. Sabourin, Pamela J. Glass, Christopher S. Badorrek, and Janice M. Rusnak

Subjects

0301 basic medicine, Venezuelan equine encephalitis virus, lcsh:QR1-502, Guidelines as Topic, Alphavirus, virus stock propagation, medicine.disease_cause, Virus, lcsh:Microbiology, Article, Animal Rule, Encephalitis Virus, Venezuelan Equine, strain selection, 03 medical and health sciences, 0302 clinical medicine, Virology, vaccine, medicine, Animals, Humans, 030212 general & internal medicine, Epizootic, Selection (genetic algorithm), biology, Immunization Programs, Viral Vaccine, Strain (biology), Encephalomyelitis, Venezuelan Equine, Viral Vaccines, medicine.disease, biology.organism_classification, Vaccine efficacy, cDNA cloned virus, Disease Models, Animal, 030104 developmental biology, Infectious Diseases

Abstract

Licensure of a vaccine to protect against aerosolized Venezuelan equine encephalitis virus (VEEV) requires use of the U.S. Food and Drug Administration (FDA) Animal Rule to assess vaccine efficacy as human studies are not feasible or ethical. An approach to selecting VEEV challenge strains for use under the Animal Rule was developed, taking into account Department of Defense (DOD) vaccine requirements, FDA Animal Rule guidelines, strain availability, and lessons learned from the generation of filovirus challenge agents within the Filovirus Animal Nonclinical Group (FANG). Initial down-selection to VEEV IAB and IC epizootic varieties was based on the DOD objective for vaccine protection in a bioterrorism event. The subsequent down-selection of VEEV IAB and IC isolates was based on isolate availability, origin, virulence, culture and animal passage history, known disease progression in animal models, relevancy to human disease, and ability to generate sufficient challenge material. Methods for the propagation of viral stocks (use of uncloned (wild-type), plaque-cloned, versus cDNA-cloned virus) to minimize variability in the potency of the resulting challenge materials were also reviewed. The presented processes for VEEV strain selection and the propagation of viral stocks may serve as a template for animal model development product testing under the Animal Rule to other viral vaccine programs. This manuscript is based on the culmination of work presented at the &ldquo, Alphavirus Workshop&rdquo, organized and hosted by the Joint Vaccine Acquisition Program (JVAP) on 15 December 2014 at Fort Detrick, Maryland, USA.

Published

2019

42. Cooperativity between the 3’ untranslated region microRNA binding sites is critical for the virulence of eastern equine encephalitis virus

Author

Christina L. Gardner, Chengqun Sun, Derek W. Trobaugh, Nishank Bhalla, William B. Klimstra, and Matthew D. Dunn

Subjects

Untranslated region, RNA viruses, Eastern Equine Encephalitis Virus, Eastern equine encephalitis virus, medicine.disease_cause, Pathology and Laboratory Medicine, Virus Replication, Biochemistry, Mice, 0302 clinical medicine, L Cells, Untranslated Regions, Animal Cells, Aedes, Cricetinae, Medicine and Health Sciences, Biology (General), 3' Untranslated Regions, 0303 health sciences, Mice, Inbred C3H, Western equine encephalitis virus, Virulence, Messenger RNA, 030302 biochemistry & molecular biology, Microbial Mutation, 3. Good health, Nucleic acids, Medical Microbiology, Viral Pathogens, Viruses, Female, Pathogens, Cellular Types, Research Article, Cell Binding, Encephalomyelitis, Equine, Cell Physiology, 3' Utr, QH301-705.5, Alphaviruses, Immunology, MiRNA binding, Bone Marrow Cells, Biology, Microbiology, Virus, Encephalitis Virus, Western Equine, Cell Line, Togaviruses, 03 medical and health sciences, Virology, medicine, Genetics, Animals, Non-coding RNA, Molecular Biology, Microbial Pathogens, 030304 developmental biology, Natural antisense transcripts, Binding Sites, Western Equine Encephalitis Virus, Organisms, Biology and Life Sciences, RNA virus, Cell Biology, RC581-607, biology.organism_classification, Viral Replication, Immunity, Innate, Gene regulation, Mice, Inbred C57BL, MicroRNAs, RAW 264.7 Cells, Viral replication, RNA, Encephalitis Virus, Eastern Equine, Parasitology, Gene expression, Immunologic diseases. Allergy, 030217 neurology & neurosurgery

Abstract

Eastern equine encephalitis virus (EEEV), a mosquito-borne RNA virus, is one of the most acutely virulent viruses endemic to the Americas, causing between 30% and 70% mortality in symptomatic human cases. A major factor in the virulence of EEEV is the presence of four binding sites for the hematopoietic cell-specific microRNA, miR-142-3p, in the 3’ untranslated region (3’ UTR) of the virus. Three of the sites are “canonical” with all 7 seed sequence residues complimentary to miR-142-3p while one is “non-canonical” and has a seed sequence mismatch. Interaction of the EEEV genome with miR-142-3p limits virus replication in myeloid cells and suppresses the systemic innate immune response, greatly exacerbating EEEV neurovirulence. The presence of the miRNA binding sequences is also required for efficient EEEV replication in mosquitoes and, therefore, essential for transmission of the virus. In the current studies, we have examined the role of each binding site by point mutagenesis of the seed sequences in all combinations of sites followed by infection of mammalian myeloid cells, mosquito cells and mice. The resulting data indicate that both canonical and non-canonical sites contribute to cell infection and animal virulence, however, surprisingly, all sites are rapidly deleted from EEEV genomes shortly after infection of myeloid cells or mice. Finally, we show that the virulence of a related encephalitis virus, western equine encephalitis virus, is also dependent upon miR-142-3p binding sites., Author summary Eastern equine encephalitis virus (EEEV) is one of the most acutely virulent mosquito-borne viruses in the Americas. A major determinant of EEEV virulence is a mammalian microRNA (miRNA) that is primarily expressed in hematopoietic cells, miR-142-3p. Like miRNA suppression of host mRNA, miR-142-3p binds to the 3’ untranslated region (UTR) of the EEEV genome only in myeloid cells suppressing virus replication and the induction of the innate immune response. In this study, we used point mutations in all four miR-142-3p binding sites in the EEEV 3’ UTR to understand the mechanism behind this miRNA suppression. We observed that decreasing the number of miR-142-3p binding sites leads to virus escape and ultimately attenuation in vivo. Furthermore, another virus, western equine encephalitis virus, also encodes miR-142-3p binding sites that contribute to virulence in vivo. These results provide insight into the mechanism of how cell-specific miRNAs can mediate suppression of virus replication.

Published

2019

43. A vibrating mesh nebulizer as an alternative to the Collison 3-jet nebulizer for infectious disease aerobiology

Author

Amy L. Hartman, Jennifer D. Bowling, William B. Klimstra, Katherine J. O’Malley, and Douglas S. Reed

Subjects

0303 health sciences, medicine.medical_specialty, 030306 microbiology, business.industry, Indoor bioaerosol, Aerobiology, 3. Good health, Microbiology, Aerosol, 03 medical and health sciences, Nebulizer, Infectious disease (medical specialty), medicine, Exposure chamber, business, Vibrating mesh nebulizer, Aerosolization, 030304 developmental biology

Abstract

Experimental infection of animals via inhalation containing pathogenic agents is essential to understanding the natural history and pathogenesis of infectious disease as well as evaluation of potential medical countermeasures. We evaluated whether the Aeroneb, a vibrating mesh nebulizer, would serve as an alternative to the Collison, the ‘gold standard’ for generating infectious bioaerosols. While the Collison possesses desirable properties that have contributed to its longevity in infectious disease aerobiology, concerns have lingered about the volume and concentration of agent required to cause disease and the damage that jet nebulization causes to the agent. For viruses, the ratio of aerosol concentration to nebulizer concentration (spray factor, SF), the Aeroneb was superior to the Collison for four different viruses in a nonhuman primate head-only exposure chamber. Aerosol concentration of influenza was higher relative to fluorescein for the Aeroneb compared to the Collison, suggesting that the Aeroneb was less harsh to viral pathogens than the Collison when generating aerosols. The Aeroneb did not improve the aerosol SF for a vegetative bacterium,Francisella tularensis.Environmental parameters collected during the aerosols indicated that the Aeroneb generated a higher relative humidity in exposure chambers while not affecting other environmental parameters. Aerosol mass median aerodynamic diameter was generally larger and more disperse for aerosols generated by the Aeroneb than what is seen with the Collison but ≥80% were within the range that would reach the lower respiratory tract and alveolar regions. These data suggest that for viral pathogens, the Aeroneb is a suitable alternative to the Collison 3-jet nebulizer.ImportanceThe threat of aerosolization is often not the natural method of transmission. While selection of an appropriate animal model is vital for these types of experiments, other confounding factors can be controlled through a thorough understanding of experimental design and the effects that different parameters can have on disease outcome. Route of administration, particle size, and dose are all factors which can affect disease progression and need to be controlled. Aerosol research methods and equipment need to be well characterized to optimize the development of animal models for bioterrorism agents.

Published

2019

44. Physiological and immunological changes in the brain associated with lethal eastern equine encephalitis virus in macaques

Author

Tobias Teichert, Theron Gilliland, Joseph R. Albe, William B. Klimstra, Henry Ma, Douglas S. Reed, Devin A. Boyles, Amy L. Hartman, Cynthia M. McMillen, Ivona Pandrea, Jeneveve D. Lundy, Emily L. Cottle, Christina L. Gardner, Matthew D. Dunn, Noah Salama, Aaron W. Walters, and Katherine J. O’Malley

Subjects

Male, Eastern equine encephalitis virus, Monkeys, Pathology and Laboratory Medicine, Medical Conditions, 0302 clinical medicine, Infectious Diseases of the Nervous System, Biology (General), Mammals, Innate Immune System, 0303 health sciences, Microglia, Eukaryota, Brain, Bioassays and Physiological Analysis, Neurology, Medical Microbiology, Viral Pathogens, Physical Sciences, Cytokines, Macaque, Encephalitis, Primates, Imaging Techniques, QH301-705.5, Alphaviruses, Materials Science, Immunology, Neurophysiology, Viremia, Microbiology, 03 medical and health sciences, Signs and Symptoms, biology.animal, Genetics, Microbial Pathogens, Molecular Biology, Organisms, Molecular Development, medicine.disease, Macaca fascicularis, Mixtures, Encephalitis Virus, Eastern Equine, Parasitology, Clinical Medicine, Immunologic diseases. Allergy, Biomarkers, 030217 neurology & neurosurgery, Neuroscience, Developmental Biology, Central Nervous System, RNA viruses, Eastern Equine Encephalitis Virus, Chemokine, Physiology, Fevers, medicine.disease_cause, Nervous System, Immune Physiology, Medicine and Health Sciences, Encephalitis, Viral, Materials, Clinical Neurophysiology, Brain Mapping, biology, Electroencephalography, Electrophysiology, Infectious Diseases, medicine.anatomical_structure, Brain Electrophysiology, Vertebrates, Viruses, Female, Anatomy, Pathogens, Research Article, Fever, Neuroimaging, Research and Analysis Methods, Virus, Togaviruses, Virology, Old World monkeys, medicine, Animals, 030304 developmental biology, Aerosols, Biology and life sciences, business.industry, Viral encephalitis, Electrophysiological Techniques, RC581-607, Disease Models, Animal, Immune System, Amniotes, biology.protein, business, Zoology

Abstract

Aerosol exposure to eastern equine encephalitis virus (EEEV) can trigger a lethal viral encephalitis in cynomolgus macaques which resembles severe human disease. Biomarkers indicative of central nervous system (CNS) infection by the virus and lethal outcome of disease would be useful in evaluating potential medical countermeasures, especially for therapeutic compounds. To meet requirements of the Animal Rule, a better understanding of the pathophysiology of EEEV-mediated disease in cynomolgus macaques is needed. In this study, macaques given a lethal dose of clone-derived EEEV strain V105 developed a fever between 2–3 days post infection (dpi) and succumbed to the disease by 6 dpi. At the peak of the febrile phase, there was a significant increase in the delta electroencephalography (EEG) power band associated with deep sleep as well as a sharp rise in intracranial pressure (ICP). Viremia peaked early after infection and was largely absent by the onset of fever. Granulocytosis and elevated plasma levels of IP-10 were found early after infection. At necropsy, there was a one hundred- to one thousand-fold increase in expression of traumatic brain injury genes (LIF, MMP-9) as well as inflammatory cytokines and chemokines (IFN-γ, IP-10, MCP-1, IL-8, IL-6) in the brain tissues. Phenotypic analysis of leukocytes entering the brain identified cells as primarily lymphoid (T, B, NK cells) with lower levels of infiltrating macrophages and activated microglia. Massive amounts of infectious virus were found in the brains of lethally-infected macaques. While no infectious virus was found in surviving macaques, quantitative PCR did find evidence of viral genomes in the brains of several survivors. These data are consistent with an overwhelming viral infection in the CNS coupled with a tremendous inflammatory response to the infection that may contribute to the disease outcome. Physiological monitoring of EEG and ICP represent novel methods for assessing efficacy of vaccines or therapeutics in the cynomolgus macaque model of EEEV encephalitis., Author summary Eastern equine encephalitis virus (EEEV) is a mosquito-transmitted virus that can cause highly lethal encephalitis in a subset of infected humans. Due to being highly virulent and infectious by aerosol, a need exists to develop vaccines or therapeutics to prevent lethal disease, and FDA approval of such an intervention would likely require use of the FDA’s Animal Rule. To further characterize the cynomolgus macaque model of EEEV after aerosol exposure, we conducted a detailed analysis of the pathological progression of encephalitis in these animals. Physiological condition of the animals was assessed after infection using electroencephalography (EEG) and intracranial pressure (ICP) along with immunological characterization of the inflammatory cells in the brain. We found overwhelming virus infection of the CNS in fatal infections coupled with a strong CNS inflammatory response. Novel findings by EEG and ICP will guide comprehensive studies evaluating the efficacy of medical countermeasures.

Published

2021

45. Venezuelan Equine Encephalitis Virus nsP3 Phosphorylation Can Be Mediated by IKKβ Kinase Activity and Abrogation of Phosphorylation Inhibits Negative-Strand Synthesis

Author

Stephanie Kortchak, Aarthi Narayanan, Aslaa Ahmed, Allison Bakovic, Weidong Zhou, Kenneth Risner, Chengqun Sun, William B. Klimstra, and Nishank Bhalla

Subjects

0301 basic medicine, Venezuelan equine encephalitis virus, viruses, lcsh:QR1-502, Viral Nonstructural Proteins, Virus Replication, medicine.disease_cause, lcsh:Microbiology, Encephalitis Virus, Venezuelan Equine, chemistry.chemical_compound, Aedes, Chlorocebus aethiops, IKK complex, negative-strand, Phosphomimetics, biology, phosphorylation, NF-kappa B, Encephalomyelitis, Venezuelan Equine, sequencing, I-kappa B Kinase, Infectious Diseases, Phosphorylation, phosphomimetics, 030106 microbiology, Alphavirus, Antiviral Agents, Article, Cell Line, non-structural protein 3, 03 medical and health sciences, Virology, medicine, Animals, Humans, Kinase activity, Vero Cells, RNA, IKKβ kinase assay, replication-deficient, mutations, biology.organism_classification, revertants, 030104 developmental biology, chemistry, Viral replication, Mutation, Togaviridae

Abstract

Venezuelan equine encephalitis virus (VEEV), a mosquito transmitted alphavirus of the Togaviridae family, can cause a highly inflammatory and encephalitic disease upon infection. Although a category B select agent, no FDA-approved vaccines or therapeutics against VEEV currently exist. We previously demonstrated NF-&kappa, B activation and macromolecular reorganization of the IKK complex upon VEEV infection in vitro, with IKK&beta, inhibition reducing viral replication. Mass spectrometry and confocal microscopy revealed an interaction between IKK&beta, and VEEV non-structural protein 3 (nsP3). Here, using western blotting, a cell-free kinase activity assay, and mass spectrometry, we demonstrate that IKK&beta, kinase activity can directly phosphorylate VEEV nsP3 at sites 204/5, 142, and 134/5. Alanine substitution mutations at sites 204/5, 142, or 134/5 reduced VEEV replication by &gt, 30-100,000-fold corresponding to a severe decrease in negative-strand synthesis. Serial passaging rescued viral replication and negative-strand synthesis, and sequencing of revertant viruses revealed reversion to the wild-type TC-83 phosphorylation capable amino acid sequences at nsP3 sites 204/5, 142, and 135. Generation of phosphomimetic mutants using aspartic acid substitutions at site 204/5 resulted in rescue of both viral replication and negative-strand RNA production, whereas phosphomimetic mutant 134/5 rescued viral replication but failed to restore negative-strand RNA levels, and phosphomimetic mutant 142 did not rescue VEEV replication. Together, these data demonstrate that IKK&beta, can phosphorylate VEEV nsP3 at sites 204/5, 142, and 134/5, and suggest that phosphorylation is essential for negative-strand RNA synthesis at site 204/5, but may be important for infectious particle production at site 134/5.

Published

2020

46. Neutralizing monoclonal antibodies against Venezuelan equine encephalitis virus envelope glycoprotein E2 protect from lethal encephalitis

Author

Natasha M. Kafai, Soila Sukupolvi, Christina L. Gardner, William B. Klimstra, and Michael S. Diamond

Subjects

Immunology, Immunology and Allergy

Abstract

Venezuelan equine encephalitis virus (VEEV) is a mosquito-borne New World alphavirus responsible for severe morbidity and mortality in humans and equines. The development of therapeutics against VEEV is critical due to its potential for outbreak and aerosolization as a bioterrorist agent. However, effective and widely accessible antiviral agents for VEEV do not exist. Humoral immunity is an important defense against many alphavirus infections, and we thus generated a panel of 17 highly neutralizing murine VEEV-specific monoclonal antibodies (mAbs) using the VEEV vaccine TC-83 and attenuated chimeric SINV-VEEV Trinidad donkey (TRD) subtype IAB. Nine of these mAbs demonstrate 50% effective inhibitory concentrations (EC50) values below 100 ng/ml when tested against enzootic subtype ID and epizootic VEEV subtypes IAB and IC virion envelope glycoproteins. To define specific viral epitopes important for mAb binding, mapping studies including competition assays, HDX, alanine-scanning mutagenesis, and viral escape mutants are ongoing. Preliminary data suggests the epitopes for these mAbs are found in both the A and B domains of the surface virion envelope 2 glycoprotein. Additionally, several of these mAbs confer prophylactic and therapeutic protection in mice aerosol challenged with virulent TRD VEEV. Mechanism of action studies are underway to define the steps in the virus life cycle (viral attachment, entry, fusion, and egress) at which our most potent protective antibodies act. Identification of specific epitopes targeted by these protective mAbs will better inform the development of targeted immunotherapeutics and vaccines against VEEV and related encephalitic alphaviruses.

Published

2020

47. Microneedle array delivered recombinant coronavirus vaccines: Immunogenicity and rapid translational development

Author

Bart L. Haagmans, Stephen C. Balmert, Louis D. Falo, William B. Klimstra, Emrullah Korkmaz, Thomas W. Kenniston, Geza Erdos, Andrea Gambotto, V. Stalin Raj, Michael W. Epperly, Cara Donahue Carey, Shaohua Huang, Eun Kim, and Virology

Subjects

0301 basic medicine, Research paper, Time Factors, viruses, lcsh:Medicine, Antibodies, Viral, medicine.disease_cause, Mice, 0302 clinical medicine, Coronavirus, lcsh:R5-920, Mice, Inbred BALB C, biology, Immunogenicity, virus diseases, General Medicine, Specific Pathogen-Free Organisms, 030220 oncology & carcinogenesis, Spike Glycoprotein, Coronavirus, Vaccines, Subunit, Trimerization, Middle East Respiratory Syndrome Coronavirus, Female, Antibody, lcsh:Medicine (General), Coronavirus Infections, COVID-19 Vaccines, Middle East respiratory syndrome coronavirus, Injections, Subcutaneous, Recombinant Fusion Proteins, Immunization, Secondary, Microneedle array, General Biochemistry, Genetics and Molecular Biology, Virus, Betacoronavirus, 03 medical and health sciences, Immune system, SDG 3 - Good Health and Well-being, Adjuvants, Immunologic, MERS-CoV S1, medicine, Animals, SARS-CoV-2, business.industry, lcsh:R, Subunit vaccines, COVID-19, Viral Vaccines, medicine.disease, Virology, Mice, Inbred C57BL, 030104 developmental biology, Immunization, Immunoglobulin G, biology.protein, Middle East respiratory syndrome, business

Abstract

Background Coronaviruses pose a serious threat to global health as evidenced by Severe Acute Respiratory Syndrome (SARS), Middle East Respiratory Syndrome (MERS), and COVID-19. SARS Coronavirus (SARS-CoV), MERS Coronavirus (MERS-CoV), and the novel coronavirus, previously dubbed 2019-nCoV, and now officially named SARS-CoV-2, are the causative agents of the SARS, MERS, and COVID-19 disease outbreaks, respectively. Safe vaccines that rapidly induce potent and long-lasting virus-specific immune responses against these infectious agents are urgently needed. The coronavirus spike (S) protein, a characteristic structural component of the viral envelope, is considered a key target for vaccines for the prevention of coronavirus infection. Methods We first generated codon optimized MERS-S1 subunit vaccines fused with a foldon trimerization domain to mimic the native viral structure. In variant constructs, we engineered immune stimulants (RS09 or flagellin, as TLR4 or TLR5 agonists, respectively) into this trimeric design. We comprehensively tested the pre-clinical immunogenicity of MERS-CoV vaccines in mice when delivered subcutaneously by traditional needle injection, or intracutaneously by dissolving microneedle arrays (MNAs) by evaluating virus specific IgG antibodies in the serum of vaccinated mice by ELISA and using virus neutralization assays. Driven by the urgent need for COVID-19 vaccines, we utilized this strategy to rapidly develop MNA SARS-CoV-2 subunit vaccines and tested their pre-clinical immunogenicity in vivo by exploiting our substantial experience with MNA MERS-CoV vaccines. Findings Here we describe the development of MNA delivered MERS-CoV vaccines and their pre-clinical immunogenicity. Specifically, MNA delivered MERS-S1 subunit vaccines elicited strong and long-lasting antigen-specific antibody responses. Building on our ongoing efforts to develop MERS-CoV vaccines, promising immunogenicity of MNA-delivered MERS-CoV vaccines, and our experience with MNA fabrication and delivery, including clinical trials, we rapidly designed and produced clinically-translatable MNA SARS-CoV-2 subunit vaccines within 4 weeks of the identification of the SARS-CoV-2 S1 sequence. Most importantly, these MNA delivered SARS-CoV-2 S1 subunit vaccines elicited potent antigen-specific antibody responses that were evident beginning 2 weeks after immunization. Interpretation MNA delivery of coronaviruses-S1 subunit vaccines is a promising immunization strategy against coronavirus infection. Progressive scientific and technological efforts enable quicker responses to emerging pandemics. Our ongoing efforts to develop MNA-MERS-S1 subunit vaccines enabled us to rapidly design and produce MNA SARS-CoV-2 subunit vaccines capable of inducing potent virus-specific antibody responses. Collectively, our results support the clinical development of MNA delivered recombinant protein subunit vaccines against SARS, MERS, COVID-19, and other emerging infectious diseases.

Published

2020

48. Vascular permeability in the brain is a late pathogenic event during Rift Valley fever virus encephalitis in rats

Author

Michael R. Kujawa, Amy L. Hartman, William B. Klimstra, Joseph R. Albe, Douglas S. Reed, and Aaron W. Walters

Subjects

Time Factors, Rift Valley Fever, Central nervous system, Gene Expression, Vascular permeability, Biology, Blood–brain barrier, Virus Replication, Virus, Article, Capillary Permeability, 03 medical and health sciences, Virology, medicine, Animals, Encephalitis, Viral, Rift Valley fever, 030304 developmental biology, 0303 health sciences, Viral encephalitis, 030302 biochemistry & molecular biology, Brain, medicine.disease, Rift Valley fever virus, Rats, Disease Models, Animal, medicine.anatomical_structure, Viral replication, Matrix Metalloproteinase 9, Rats, Inbred Lew, Female, Encephalitis

Abstract

Rift Valley fever virus (RVFV) is a zoonotic disease of livestock that causes several clinical outcomes in people including febrile disease, hemorrhagic fever, and/or encephalitis. After aerosol infection with RVFV, Lewis rats develop lethal encephalitic disease, and we use this as a model for studying disease mechanisms of RVFV infection in the brain. Permeability of the brain vasculature in relation to virus invasion and replication is not known. Here, we found that vascular permeability in the brain occurred late in the course of infection and corresponded temporally to expression of matrix metalloproteinase-9 (MMP-9). Virus replication was ongoing within the central nervous system for several days prior to detectable vascular leakage. Based on this study, vascular permeability was not required for entry of RVFV into the brain of rats. Prevention of vascular leakage late in infection may be an important component for prevention of lethal neurological disease in the rat model.

Published

2018

49. The Interferon-Induced Exonuclease ISG20 Exerts Antiviral Activity through Upregulation of Type I Interferon Response Proteins

Author

Kate D. Ryman, William B. Klimstra, Derek W. Trobaugh, Michael S. Diamond, Chengqun Sun, Christopher Weiss, and Tiffany M. Lucas

Subjects

0301 basic medicine, Exonucleases, Male, viruses, lcsh:QR1-502, interferon-stimulated gene, medicine.disease_cause, Virus Replication, lcsh:Microbiology, Encephalitis Virus, Venezuelan Equine, Mice, Interferon, alphavirus, innate immunity, Mice, Knockout, virus diseases, RNA-Binding Proteins, QR1-502, Up-Regulation, Host-Pathogen Interactions, Interferon Type I, RNA, Viral, Female, Chikungunya virus, medicine.drug, Alphavirus, Biology, Microbiology, Virus, Cell Line, 03 medical and health sciences, medicine, Animals, Molecular Biology, Gene, virus-host interactions, Adaptor Proteins, Signal Transducing, 030102 biochemistry & molecular biology, RNA, RNA virus, biology.organism_classification, Virology, Immunity, Innate, Mice, Inbred C57BL, 030104 developmental biology, Viral replication, Microscopy, Fluorescence, Venezuelan equine encephalitis virus, Exoribonucleases, Carrier Proteins

Abstract

Type I interferon (IFN)-stimulated genes (ISGs) have critical roles in inhibiting virus replication and dissemination. Despite advances in understanding the molecular basis of ISG restriction, the antiviral mechanisms of many remain unclear. The 20-kDa ISG ISG20 is a nuclear 3′–5′ exonuclease with preference for single-stranded RNA (ssRNA) and has been implicated in the IFN-mediated restriction of several RNA viruses. Although the exonuclease activity of ISG20 has been shown to degrade viral RNA in vitro, evidence has yet to be presented that virus inhibition in cells requires this activity. Here, we utilized a combination of an inducible, ectopic expression system and newly generated Isg20−/− mice to investigate mechanisms and consequences of ISG20-mediated restriction. Ectopically expressed ISG20 localized primarily to Cajal bodies in the nucleus and restricted replication of chikungunya and Venezuelan equine encephalitis viruses. Although restriction by ISG20 was associated with inhibition of translation of infecting genomic RNA, degradation of viral RNAs was not observed. Instead, translation inhibition of viral RNA was associated with ISG20-induced upregulation of over 100 other genes, many of which encode known antiviral effectors. ISG20 modulated the production of IFIT1, an ISG that suppresses translation of alphavirus RNAs. Consistent with this observation, the pathogenicity of IFIT1-sensitive alphaviruses was increased in Isg20−/− mice compared to that of wild-type viruses but not in cells ectopically expressing ISG20. Our findings establish an indirect role for ISG20 in the early restriction of RNA virus replication by regulating expression of other ISGs that inhibit translation and possibly other activities in the replication cycle. IMPORTANCE The host immune responses to infection lead to the production of type I interferon (IFN), and the upregulation of interferon-stimulated genes (ISGs) reduces virus replication and virus dissemination within a host. Ectopic expression of the interferon-induced 20-kDa exonuclease ISG20 suppressed replication of chikungunya virus and Venezuelan equine encephalitis virus, two mosquito-vectored RNA alphaviruses. Since the replication of alphavirus genomes occurs exclusively in the cytoplasm, the mechanism of nucleus-localized ISG20 inhibition of replication is unclear. In this study, we determined that ISG20 acts as a master regulator of over 100 genes, many of which are ISGs. Specifically, ISG20 upregulated IFIT1 genes and inhibited translation of the alphavirus genome. Furthermore, IFIT1-sensitive alphavirus replication was increased in Isg20−/− mice compared to the replication of wild-type viruses but not in cells ectopically expressing ISG20. We propose that ISG20 acts as an indirect regulator of RNA virus replication in the cytoplasm through the upregulation of many other ISGs.

Published

2018

50. Gamma-interferon exerts a critical early restriction on replication and dissemination of yellow fever virus vaccine strain 17D-204

Author

Kate D. Ryman, William B. Klimstra, Alan M. Watson, and L. K. Metthew Lam

Subjects

lcsh:Immunologic diseases. Allergy, 0301 basic medicine, 030106 microbiology, Immunology, Context (language use), Biology, lcsh:RC254-282, Article, Virus, 03 medical and health sciences, Immunity, medicine, Pharmacology (medical), Vector (molecular biology), Pharmacology, Attenuated vaccine, Viral Vaccine, Yellow fever, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, Virology, 3. Good health, 030104 developmental biology, Infectious Diseases, Viral replication, lcsh:RC581-607

Abstract

Live attenuated viruses are historically among the most effective viral vaccines. Development of a safe vaccine requires the virus to be less virulent, a phenotype that is historically arrived by empirical evaluation often leaving the mechanisms of attenuation unknown. The yellow fever virus 17D live attenuated vaccine strain has been developed as a delivery vector for heterologous antigens; however, the mechanisms of attenuation remain elusive. The successful and safe progress of 17D as a vaccine vector and the development of live attenuated vaccines (LAVs) to related flaviviruses requires an understanding of the molecular mechanisms leading to attenuation. Using subcutaneous infection of interferon-deficient mouse models of wild type yellow fever virus (WT YFV) pathogenesis and 17D-mediated immunity, we found that, in the absence of type I IFN (IFN-α/β), type II interferon (IFN-γ) restricted 17D replication, but not that of WT YFV, by 1–2 days post-infection. In this context, IFN-γ responses protected 17D-infected animals from mortality, largely restricted the virus to lymphoid organs, and eliminated viscerotropic disease signs such as steatosis in the liver and inflammatory cell infiltration into the spleen. However, WT YFV caused a disseminated infection, gross liver pathology, and rapid death of the animals. In vitro, IFN-γ treatment of myeloid cells suppressed the replication of 17D significantly more than that of WT YFV, suggesting a direct differential effect on 17D virus replication. Together these data indicate that an important mechanism of 17D attenuation in vivo is increased sensitivity to IFN-γ stimulated responses elicited early after infection., Yellow fever: What makes vaccines safe? The interferon gamma protein may play a key role in preventing yellow fever vaccine 17D from causing virus-like disease in recipients. The highly effective 17D vaccine is a less virulent form of the virus, but can induce severe disease in rare cases. A research group from the University of Pittsburgh, led by William Klimstra, investigated the impact of the vaccine on mice, as the mechanism by which hosts defend against its disease-causing potential is not fully understood. They found that interferon gamma restricted the replication and spread of the attenuated virus (the vaccine) but not its natural form. This study helps to inform efforts to improve the safety of the 17D vaccine, as well as the other vaccines that use it as a template for prophylaxis against other pathogens.

Published

2018