Your search keyword '"Jason E, Comer"' showing total 63 results

1. Comparison of Routes of Administration, Frequency, and Duration of Favipiravir Treatment in Mouse and Guinea Pig Models of Ebola Virus Disease

Author

Dylan M. Johnson, Terry Juelich, Lihong Zhang, Jennifer K. Smith, Birte K. Kalveram, David Perez, Jeanon Smith, Michael R. Grimes, Tania Garron, Maricela Torres, Shane Massey, Trevor Brasel, David W. C. Beasley, Alex N. Freiberg, and Jason E. Comer

Subjects

filovirus, Ebola virus, favipiravir, T-705, EBOV, animal model, Microbiology, QR1-502

Abstract

Favipiravir is a ribonucleoside analogue that has been explored as a therapeutic for the treatment of Ebola Virus Disease (EVD). Promising data from rodent models has informed nonhuman primate trials, as well as evaluation in patients during the 2013–2016 West African EVD outbreak of favipiravir treatment. However, mixed results from these studies hindered regulatory approval of favipiravir for the indication of EVD. This study examined the influence of route of administration, duration of treatment, and treatment schedule of favipiravir in immune competent mouse and guinea pig models using rodent-adapted Zaire ebolavirus (EBOV). A dose of 300 mg/kg/day of favipiravir with an 8-day treatment was found to be fully effective at preventing lethal EVD-like disease in BALB/c mice regardless of route of administration (oral, intraperitoneal, or subcutaneous) or whether it was provided as a once-daily dose or a twice-daily split dose. Preclinical data generated in guinea pigs demonstrates that an 8-day treatment of 300 mg/kg/day of favipiravir reduces mortality following EBOV challenge regardless of route of treatment or duration of treatments for 8, 11, or 15 days. This work supports the future translational development of favipiravir as an EVD therapeutic.

Published

2024

2. Natural history of nonhuman primates after conjunctival exposure to Ebola virus

Author

Robert W. Cross, Abhishek N. Prasad, Courtney B. Woolsey, Krystle N. Agans, Viktoriya Borisevich, Natalie S. Dobias, Jason E. Comer, Daniel J. Deer, Joan B. Geisbert, Angela L. Rasmussen, Walter Ian Lipkin, Karla A. Fenton, and Thomas W. Geisbert

Subjects

Medicine, Science

Abstract

Abstract Transmission of Ebola virus (EBOV) primarily occurs via contact exposure of mucosal surfaces with infected body fluids. Historically, nonhuman primate (NHP) challenge studies have employed intramuscular (i.m.) or small particle aerosol exposure, which are largely lethal routes of infection, but mimic worst-case scenarios such as a needlestick or intentional release, respectively. When exposed by more likely routes of natural infection, limited NHP studies have shown delayed onset of disease and reduced mortality. Here, we performed a series of systematic natural history studies in cynomolgus macaques with a range of conjunctival exposure doses. Challenge with 10,000 plaque forming units (PFU) of EBOV was uniformly lethal, whereas 5/6 subjects survived lower dose challenges (100 or 500 PFU). Conjunctival challenge resulted in a protracted time-to death compared to i.m. Asymptomatic infection was observed in survivors with limited detection of EBOV replication. Inconsistent seropositivity in survivors may suggest physical or natural immunological barriers are sufficient to prevent widespread viral dissemination.

Published

2023

3. Pathogenic and Apathogenic Strains of Lymphocytic Choriomeningitis Virus Have Distinct Entry and Innate Immune Activation Pathways

Author

Dylan M. Johnson, Nittaya Khakhum, Min Wang, Nikole L. Warner, Jenny D. Jokinen, Jason E. Comer, and Igor S. Lukashevich

Subjects

lymphocytic choriomeningitis virus, toll-like receptors, intracellular trafficking, Microbiology, QR1-502

Abstract

Lymphocytic choriomeningitis virus (LCMV) and Lassa virus (LASV) share many genetic and biological features including subtle differences between pathogenic and apathogenic strains. Despite remarkable genetic similarity, the viscerotropic WE strain of LCMV causes a fatal LASV fever-like hepatitis in non-human primates (NHPs) while the mouse-adapted Armstrong (ARM) strain of LCMV is deeply attenuated in NHPs and can vaccinate against LCMV-WE challenge. Here, we demonstrate that internalization of WE is more sensitive to the depletion of membrane cholesterol than ARM infection while ARM infection is more reliant on endosomal acidification. LCMV-ARM induces robust NF-κB and interferon response factor (IRF) activation while LCMV-WE seems to avoid early innate sensing and failed to induce strong NF-κB and IRF responses in dual-reporter monocyte and epithelial cells. Toll-like receptor 2 (TLR-2) signaling appears to play a critical role in NF-κB activation and the silencing of TLR-2 shuts down IL-6 production in ARM but not in WE-infected cells. Pathogenic LCMV-WE infection is poorly recognized in early endosomes and failed to induce TLR-2/Mal-dependent pro-inflammatory cytokines. Following infection, Interleukin-1 receptor-associated kinase 1 (IRAK-1) expression is diminished in LCMV-ARM- but not LCMV-WE-infected cells, which indicates it is likely involved in the LCMV-ARM NF-κB activation. By confocal microscopy, ARM and WE strains have similar intracellular trafficking although LCMV-ARM infection appears to coincide with greater co-localization of early endosome marker EEA1 with TLR-2. Both strains co-localize with Rab-7, a late endosome marker, but the interaction with LCMV-WE seems to be more prolonged. These findings suggest that LCMV-ARM’s intracellular trafficking pathway may facilitate interaction with innate immune sensors, which promotes the induction of effective innate and adaptive immune responses.

Published

2024

4. 373 Identification of potential targets for immunotherapy in a cynomolgus macaque model of Ebola virus disease

Author

Timothy Wanninger, Omar A. Saldarriaga, Daniel E. Millian, Jason E. Comer, Kamil Khanipov, George Golovko, Slobodan Paessler, and Heather L. Stevenson

Subjects

Medicine

Abstract

OBJECTIVES/GOALS: Ebola virus infection causes severe disease and liver injury in humans. Macrophages contribute to inflammatory signaling and are prevalent in the liver. We assessed the activation status, including therapeutic target expression, of hepatic macrophages. METHODS/STUDY POPULATION: We compared formalin-fixed, paraffin-embedded liver tissue from terminal Ebola virus-infected and uninfected control cynomolgus macaques, a gold-standard model for human disease. We characterized region-specific protein and whole transcriptome expression in these tissues using GeoMx Digital Spatial Profiling. Macrophage (CD68+) and leukocyte (CD45+) accumulation in liver tissue was quantified by immunofluorescence image analysis using digital pathology software. RESULTS/ANTICIPATED RESULTS: Macrophage-specific (CD68+) regions in the liver of Ebola virus-infected macaques demonstrated a shift towards an inflammatory gene expression profile, as compared to those from healthy control tissue. These regions showed differential expression of monocyte/macrophage differentiation, antigen presentation, and T cell activation gene sets, which were associated with decreased MHC-II allele expression. Moreover, macrophage-specific regions in the infected macaques showed enriched expression of genes or proteins associated with known immunomodulatory therapeutics, including S100A9, IDO1, and CTLA-4. DISCUSSION/SIGNIFICANCE: These data demonstrate that hepatic macrophages express an inflammatory phenotype, that their ability to present antigens to the adaptive immune system may be impaired, and that they express therapeutically targetable markers for immunomodulation of these cells during Ebola virus infection.

Published

2023

5. Natural History of Marburg Virus Infection to Support Medical Countermeasure Development

Author

Jason E. Comer, Trevor Brasel, Shane Massey, David W. Beasley, Chris M. Cirimotich, Daniel C. Sanford, Ying-Liang Chou, Nancy A. Niemuth, Joseph Novak, Carol L. Sabourin, Michael Merchlinsky, James P. Long, Eric J. Stavale, and Daniel N. Wolfe

Subjects

Marburg virus, MARV, filovirus, natural history study, virus, macaques, Microbiology, QR1-502

Abstract

The Biomedical Advanced Research and Development Authority, part of the Administration for Strategic Preparedness and Response within the U.S. Department of Health and Human Services, recognizes that the evaluation of medical countermeasures under the Animal Rule requires well-characterized and reproducible animal models that are likely to be predictive of clinical benefit. Marburg virus (MARV), one of two members of the genus Marburgvirus, is characterized by a hemorrhagic fever and a high case fatality rate for which there are no licensed vaccines or therapeutics available. This natural history study consisted of twelve cynomolgus macaques challenged with 1000 PFU of MARV Angola and observed for body weight, temperature, viremia, hematology, clinical chemistry, and coagulation at multiple time points. All animals succumbed to disease within 8 days and exhibited signs consistent with those observed in human cases, including viremia, fever, systemic inflammation, coagulopathy, and lymphocytolysis, among others. Additionally, this study determined the time from exposure to onset of disease manifestations and the time course, frequency, and magnitude of the manifestations. This study will be instrumental in the design and development of medical countermeasures to Marburg virus disease.

Published

2022

6. The Fc-mediated effector functions of a potent SARS-CoV-2 neutralizing antibody, SC31, isolated from an early convalescent COVID-19 patient, are essential for the optimal therapeutic efficacy of the antibody.

Author

Conrad E Z Chan, Shirley G K Seah, De Hoe Chye, Shane Massey, Maricela Torres, Angeline P C Lim, Steven K K Wong, Jacklyn J Y Neo, Pui San Wong, Jie Hui Lim, Gary S L Loh, Dongling Wang, Jerome D Boyd-Kirkup, Siyu Guan, Dipti Thakkar, Guo Hui Teo, Kiren Purushotorman, Paul E Hutchinson, Barnaby E Young, Jenny G Low, Paul A MacAry, Hannes Hentze, Venkateshan S Prativadibhayankara, Kantharaj Ethirajulu, Jason E Comer, Chien-Te K Tseng, Alan D T Barrett, Piers J Ingram, Trevor Brasel, and Brendon John Hanson

Subjects

Medicine, Science

Abstract

Although SARS-CoV-2-neutralizing antibodies are promising therapeutics against COVID-19, little is known about their mechanism(s) of action or effective dosing windows. We report the generation and development of SC31, a potent SARS-CoV-2 neutralizing antibody, isolated from a convalescent patient. Antibody-mediated neutralization occurs via an epitope within the receptor-binding domain of the SARS-CoV-2 Spike protein. SC31 exhibited potent anti-SARS-CoV-2 activities in multiple animal models. In SARS-CoV-2 infected K18-human ACE2 transgenic mice, treatment with SC31 greatly reduced viral loads and attenuated pro-inflammatory responses linked to the severity of COVID-19. Importantly, a comparison of the efficacies of SC31 and its Fc-null LALA variant revealed that the optimal therapeutic efficacy of SC31 requires Fc-mediated effector functions that promote IFNγ-driven anti-viral immune responses, in addition to its neutralization ability. A dose-dependent efficacy of SC31 was observed down to 5mg/kg when administered before viral-induced lung inflammatory responses. In addition, antibody-dependent enhancement was not observed even when infected mice were treated with SC31 at sub-therapeutic doses. In SARS-CoV-2-infected hamsters, SC31 treatment significantly prevented weight loss, reduced viral loads, and attenuated the histopathology of the lungs. In rhesus macaques, the therapeutic potential of SC31 was evidenced through the reduction of viral loads in both upper and lower respiratory tracts to undetectable levels. Together, the results of our preclinical studies demonstrated the therapeutic efficacy of SC31 in three different models and its potential as a COVID-19 therapeutic candidate.

Published

2021

7. Natural history of disease in cynomolgus monkeys exposed to Ebola virus Kikwit strain demonstrates the reliability of this non-human primate model for Ebola virus disease.

Author

Nancy A Niemuth, Dawn Fallacara, Cheryl A Triplett, Sanjay M Tamrakar, Alisha Rajbhandari, Clint Florence, Lucy Ward, Anthony Griffiths, Ricardo Carrion, Yenny Goez-Gazi, Kendra J Alfson, Hilary M Staples, Trevor Brasel, Jason E Comer, Shane Massey, Jeanon Smith, Andrew Kocsis, Jake Lowry, Sara C Johnston, Aysegul Nalca, Arthur J Goff, Amy C Shurtleff, Margaret L Pitt, John Trefry, and Michael P Fay

Subjects

Medicine, Science

Abstract

Filoviruses (Family Filoviridae genera Ebolavirus and Marburgvirus) are negative-stranded RNA viruses that cause severe health effects in humans and non-human primates, including death. Except in outbreak settings, vaccines and other medical countermeasures against Ebola virus (EBOV) will require testing under the FDA Animal Rule. Multiple vaccine candidates have been evaluated using cynomolgus monkeys (CM) exposed to EBOV Kikwit strain. To the best of our knowledge, however, animal model development data supporting the use of CM in vaccine research have not been submitted to the FDA. This study describes a large CM database (122 CM, 62 female and 60 male, age 2 to 9 years) and demonstrates the consistency of the CM model through time to death models and descriptive statistics. CMs were exposed to EBOV doses of 0.1 to 100,000 PFU in 33 studies conducted at three Animal Biosafety Level 4 facilities, by three exposure routes. Time to death was modeled using Cox proportional hazards models with a frailty term that incorporated study-to-study variability. Despite significant differences attributed to exposure variables, all CMs exposed to the 100 to 1,000 pfu doses commonly used in vaccine studies died or met euthanasia criteria within 21 days of exposure, median 7 days, 93% between 5 and 12 days of exposure. Moderate clinical signs were observed 4 to 5 days after exposure and preceded death or euthanasia by approximately one day. Viremia was detected within a few days of infection. Hematology indices were indicative of viremia and the propensity for hemorrhage with progression of Ebola viremia. Changes associated with coagulation parameters and platelets were consistent with coagulation disruption. Changes in leukocyte profiles were indicative of an acute inflammatory response. Increased liver enzymes were observed shortly after exposure. Taken together, these factors suggest that the cynomolgus monkey is a reliable animal model for human disease.

Published

2021

8. STAT-1 Knockout Mice as a Model for Wild-Type Sudan Virus (SUDV)

Author

Olivier Escaffre, Terry L. Juelich, Natasha Neef, Shane Massey, Jeanon Smith, Trevor Brasel, Jennifer K. Smith, Birte Kalveram, Lihong Zhang, David Perez, Tetsuro Ikegami, Alexander N. Freiberg, and Jason E. Comer

Subjects

ebolavirus, filovirus, SUDV, STAT-1 knockout mice, animal model, Microbiology, QR1-502

Abstract

Currently there is no FDA-licensed vaccine or therapeutic against Sudan ebolavirus (SUDV) infections. The largest ever reported 2014–2016 West Africa outbreak, as well as the 2021 outbreak in the Democratic Republic of Congo, highlight the critical need for countermeasures against filovirus infections. A well-characterized small animal model that is susceptible to wild-type filoviruses would greatly add to the screening of antivirals and vaccines. Here, we infected signal transducer and activator of transcription-1 knock out (STAT-1 KO) mice with five different wildtype filoviruses to determine susceptibility. SUDV and Marburg virus (MARV) were the most virulent, and caused 100% or 80% lethality, respectively. Zaire ebolavirus (EBOV), Bundibugyo ebolavirus (BDBV), and Taï Forest ebolavirus (TAFV) caused 40%, 20%, and no mortality, respectively. Further characterization of SUDV in STAT-1 KO mice demonstrated lethality down to 3.1 × 101 pfu. Viral genomic material was detectable in serum as early as 1 to 2 days post-challenge. The onset of viremia was closely followed by significant changes in total white blood cells and proportion of neutrophils and lymphocytes, as well as by an influx of neutrophils in the liver and spleen. Concomitant significant fluctuations in blood glucose, albumin, globulin, and alanine aminotransferase were also noted, altogether consistent with other models of filovirus infection. Finally, favipiravir treatment fully protected STAT-1 KO mice from lethal SUDV challenge, suggesting that this may be an appropriate small animal model to screen anti-SUDV countermeasures.

Published

2021

9. Repurposing the antimalarial pyronaridine tetraphosphate to protect against Ebola virus infection.

Author

Thomas R Lane, Christopher Massey, Jason E Comer, Manu Anantpadma, Joel S Freundlich, Robert A Davey, Peter B Madrid, and Sean Ekins

Subjects

Arctic medicine. Tropical medicine, RC955-962, Public aspects of medicine, RA1-1270

Abstract

Recent outbreaks of the Ebola virus (EBOV) have focused attention on the dire need for antivirals to treat these patients. We identified pyronaridine tetraphosphate as a potential candidate as it is an approved drug in the European Union which is currently used in combination with artesunate as a treatment for malaria (EC50 between 420 nM-1.14 μM against EBOV in HeLa cells). Range-finding studies in mice directed us to a single 75 mg/kg i.p. dose 1 hr after infection which resulted in 100% survival and statistically significantly reduced viremia at study day 3 from a lethal challenge with mouse-adapted EBOV (maEBOV). Further, an EBOV window study suggested we could dose pyronaridine 2 or 24 hrs post-exposure to result in similar efficacy. Analysis of cytokine and chemokine panels suggests that pyronaridine may act as an immunomodulator during an EBOV infection. Our studies with pyronaridine clearly demonstrate potential utility for its repurposing as an antiviral against EBOV and merits further study in larger animal models with the added benefit of already being used as a treatment against malaria.

Published

2019

10. Characterization of Ebola Virus Mucosal Challenge Routes in Cynomolgus Macaques

Author

Dylan M. Johnson, Trevor Brasel, Shane Massey, Jeanon Smith, Tania Garron, Shannon Wallace, Xiaoying Yu, David W. Beasley, and Jason E. Comer

Subjects

Virology, Insect Science, Immunology, Microbiology

Abstract

This study is the first to examine the Kikwit strain of EBOV, the most commonly used strain, in the gold-standard macaque model of infection. Additionally, this is the first description of the detection of virus in the vitreous fluid, an immune privileged site that has been proposed as a viral reservoir, following conjunctival challenge.

Published

2023

11. Pathogenesis of aerosolized Ebola virus variant Makona in nonhuman primates

Author

Abhishek N Prasad, Karla A Fenton, Krystle N Agans, Viktoriya Borisevich, Courtney Woolsey, Jason E Comer, Natalie S Dobias, Jennifer E Peel, Daniel J Deer, Joan B Geisbert, William S Lawrence, Robert W Cross, and Thomas W Geisbert

Subjects

Infectious Diseases, Immunology and Allergy

Abstract

Background The primary route of infection by Ebola virus (EBOV) and other pathogenic filoviruses in humans is through contact of contaminated body fluids with mucosal surfaces. Despite this, filoviruses hold capacity for delivery by both large and small particle artificial aerosols, and thus present potential for intentional misuse. Previous studies have shown that high doses of EBOV (≥ 1000 PFU) delivered by small particle aerosol cause uniform lethality in nonhuman primates (NHP) while only a few small studies have assessed lower doses in NHPs. Methods To further characterize the pathogenesis of EBOV infection via the small particle aerosol route, we challenged cohorts of cynomolgus monkeys with low doses (10 PFU, 1 PFU, 0.1 PFU) of EBOV variant Makona, which may help to define risks associated with small particle aerosol exposures. Results Despite using challenge doses several orders of magnitude lower than previously published studies, infection via this route was uniformly lethal across all cohorts; however, the time to death was delayed in a dose-dependent manner between aerosol-challenged cohorts, as well as in comparison to animals challenged via the intramuscular route. Here, we describe the observed clinical and pathological details including serum biomarkers, viral burden, and histopathological changes leading to death. Conclusions Our observations in this model highlight the striking susceptibility of NHPs, and by extension, likely humans, via small particle aerosol exposure to EBOV and emphasize the need for further development of rapid diagnostics and potent postexposure prophylactics in the event of intentional release via deployment of an aerosol-producing device.

Published

2023

12. A Synthetic Peptide CTL Vaccine Targeting Nucleocapsid Confers Protection from SARS-CoV-2 Challenge in Rhesus Macaques

Author

Paul E. Harris, Trevor Brasel, Christopher Massey, C. V. Herst, Scott Burkholz, Peter Lloyd, Tikoes Blankenberg, Thomas M. Bey, Richard Carback, Thomas Hodge, Serban Ciotlos, Lu Wang, Jason E. Comer, and Reid M. Rubsamen

Subjects

SARS-CoV-2, animal model, macaque, vaccine, MHC class I peptide, T cell, Medicine

Abstract

Background: Persistent transmission of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) has given rise to a COVID-19 pandemic. Several vaccines, conceived in 2020, that evoke protective spike antibody responses are being deployed in mass public health vaccination programs. Recent data suggests, however, that as sequence variation in the spike genome accumulates, some vaccines may lose efficacy. Methods: Using a macaque model of SARS-CoV-2 infection, we tested the efficacy of a peptide-based vaccine targeting MHC class I epitopes on the SARS-CoV-2 nucleocapsid protein. We administered biodegradable microspheres with synthetic peptides and adjuvants to rhesus macaques. Unvaccinated control and vaccinated macaques were challenged with 1 × 108 TCID50 units of SARS-CoV-2, followed by assessment of clinical symptoms and viral load, chest radiographs, and sampling of peripheral blood and bronchoalveolar lavage (BAL) fluid for downstream analysis. Results: Vaccinated animals were free of pneumonia-like infiltrates characteristic of SARS-CoV-2 infection and presented with lower viral loads relative to controls. Gene expression in cells collected from BAL samples of vaccinated macaques revealed a unique signature associated with enhanced development of adaptive immune responses relative to control macaques. Conclusions: We demonstrate that a room temperature stable peptide vaccine based on known immunogenic HLA class I bound CTL epitopes from the nucleocapsid protein can provide protection against SARS-CoV-2 infection in nonhuman primates.

Published

2021

13. Cell-Type Apoptosis in Lung during SARS-CoV-2 Infection

Author

Yakun Liu, Tania M. Garron, Qing Chang, Zhengchen Su, Changcheng Zhou, Yuan Qiu, Eric C. Gong, Junying Zheng, Y. Whitney Yin, Thomas Ksiazek, Trevor Brasel, Yang Jin, Paul Boor, Jason E. Comer, and Bin Gong

Subjects

SARS-CoV-2, apoptosis, lung, human, non-human primate, co-culture, Medicine

Abstract

The SARS-CoV-2 pandemic has inspired renewed interest in understanding the fundamental pathology of acute respiratory distress syndrome (ARDS) following infection. However, the pathogenesis of ARDS following SRAS-CoV-2 infection remains largely unknown. In the present study, we examined apoptosis in postmortem lung sections from COVID-19 patients and in lung tissues from a non-human primate model of SARS-CoV-2 infection, in a cell-type manner, including type 1 and 2 alveolar cells and vascular endothelial cells (ECs), macrophages, and T cells. Multiple-target immunofluorescence assays and Western blotting suggest both intrinsic and extrinsic apoptotic pathways are activated during SARS-CoV-2 infection. Furthermore, we observed that SARS-CoV-2 fails to induce apoptosis in human bronchial epithelial cells (i.e., BEAS2B cells) and primary human umbilical vein endothelial cells (HUVECs), which are refractory to SARS-CoV-2 infection. However, infection of co-cultured Vero cells and HUVECs or Vero cells and BEAS2B cells with SARS-CoV-2 induced apoptosis in both Vero cells and HUVECs/BEAS2B cells but did not alter the permissiveness of HUVECs or BEAS2B cells to the virus. Post-exposure treatment of the co-culture of Vero cells and HUVECs with a novel non-cyclic nucleotide small molecule EPAC1-specific activator reduced apoptosis in HUVECs. These findings may help to delineate a novel insight into the pathogenesis of ARDS following SARS-CoV-2 infection.

Published

2021

14. Mucosal Challenge Ferret Models of Ebola Virus Disease

Author

Trevor Brasel, Jason E. Comer, Shane Massey, Jeanon Smith, Jennifer Smith, Matthew Hyde, Andrew Kocsis, Melicia Gainey, Nancy Niemuth, Cheryl Triplett, and Thomas Rudge

Subjects

Ebola virus, ferret, mucosal challenge, Medicine

Abstract

Recent studies have shown the domestic ferret (Mustela putorius furo) to be a promising small animal model for the study of Ebola virus (EBOV) disease and medical countermeasure evaluation. To date, most studies have focused on traditional challenge routes, predominantly intramuscular and intranasal administration. Here, we present results from a non-clinical pathogenicity study examining oronasal, oral, and ocular mucosal challenge routes in ferrets. Animals were challenged with 1, 10, or 100 plaque forming units EBOV followed by monitoring of disease progression and biosampling. Ferrets administered virus via oronasal and oral routes met euthanasia criteria due to advanced disease 5–10 days post-challenge. Conversely, all ferrets dosed via the ocular route survived until the scheduled study termination 28-day post-challenge. In animals that succumbed to disease, a dose/route response was not observed; increases in disease severity, febrile responses, serum and tissue viral load, alterations in clinical pathology, and gross/histopathology findings were similar between subjects. Disease progression in ferrets challenged via ocular administration was unremarkable throughout the study period. Results from this study further support the ferret as a model for EBOV disease following oral and nasal mucosa exposure.

Published

2021

15. Physiological Responses to Multiple Low-Doses of Bacillus anthracis Spores in the Rabbit Model of Inhalation Anthrax

Author

Sarah C. Taft, Tonya L. Nichols, Stephanie A. Hines, Roy E. Barnewall, Gregory V. Stark, and Jason E. Comer

Subjects

Bacillus anthracis, anthrax, low-dose, multiple dose, dose-response, physiological response, Medicine

Abstract

Bacillus anthracis spores that are re-aerosolized from surface deposits after initial contamination present significant health risks for personnel involved in decontamination. To model repeated exposure to low dose B. anthracis spores, three groups of seven rabbits were challenged with multiple low-doses of B. anthracis spores 5 days a week for 3 weeks. Mortality, body temperature, heart and respiration rates, hematology, C-reactive protein, bacteremia, and serum protective antigen were monitored for 21 days post-exposure after the last of multiple doses. All rabbits exposed to a mean daily dose of 2.91 × 102 colony forming units (CFU) survived and showed minimal physiological changes attributable to exposure. One of seven rabbits receiving a mean daily dose of 1.22 × 103 CFU died and four of seven receiving a mean daily dose of 1.17 × 104 CFU died. The LD50 was calculated to be 8.1 × 103 CFU of accumulated dose. Rabbits that succumbed to the higher dose exhibited bacteremia and increases above baseline in heart rate, respiration rate, and body temperature. Two rabbits in the mean daily dose group of 1.17 × 104 CFU exhibited clinical signs of inhalation anthrax yet survived. This study provides a description of lethality, pathophysiology, and pathology in a controlled multiple low-dose inhalation exposure study of B. anthracis in the rabbit model. The data suggest that the accumulated dose is important in survival outcome and that a subset of rabbits may show clinical signs of disease but fully recover without therapeutic intervention

Published

2020

16. Teixobactin Provides Protection against Inhalation Anthrax in the Rabbit Model

Author

William S. Lawrence, Jennifer E. Peel, Satheesh K. Sivasubramani, Wallace B. Baze, Elbert B. Whorton, David W. C. Beasley, Jason E. Comer, Dallas E. Hughes, Losee L. Ling, and Johnny W. Peterson

Subjects

Bacillus anthracis, anthrax, inhalation, infection, antibiotic, rabbit model, Medicine

Abstract

The use of antibiotics is a vital means of treating infections caused by the bacteria Bacillus (B.) anthracis. Importantly, with the potential future use of multidrug-resistant strains of B. anthracis as bioweapons, new antibiotics are needed as alternative therapeutics. In this blinded study, we assessed the protective efficacy of teixobactin, a recently discovered antibiotic, against inhalation anthrax infection in the adult rabbit model. New Zealand White rabbits were infected with a lethal dose of B. anthracis Ames spores via the inhalation route, and blood samples were collected at various times to assess antigenemia, bacteremia, tissue bacterial load, and antibody production. Treatments were administered upon detection of B. anthracis protective antigen in the animals’ sera. For comparison, a fully protective dose of levofloxacin was used as a positive control. Rabbits treated with teixobactin showed 100% survival following infection, and the bacteremia was completely resolved by 24–48 h post-treatment. In addition, the bacterial/spore loads in tissues of the animals treated with teixobactin were either zero or dramatically less relative to that of the negative control animals. Moreover, microscopic evaluation of the tissues revealed decreased pathology following treatment with teixobactin. Overall, these results show that teixobactin was protective against inhalation anthrax infection in the rabbit model, and they indicate the potential of teixobactin as a therapeutic for the disease.

Published

2020

17. Physiological Responses to a Single Low-Dose of Bacillus anthracis Spores in the Rabbit Model of Inhalational Anthrax

Author

Sarah C. Taft, Tonya L. Nichols, Stephanie A. Hines, Roy E. Barnewall, Gregory V. Stark, and Jason E. Comer

Subjects

Bacillus anthracis, anthrax, low-dose, dose–response, physiological response, Medicine

Abstract

Credible dose–response relationships are needed to more accurately assess the risk posed by exposure to low-level Bacillus anthracis contamination during or following a release. To begin to fill this knowledge gap, New Zealand White rabbits were implanted with D70-PCT telemetry transmitters and subsequently aerosol challenged with average inhaled doses of 2.86 × 102 to 2.75 × 105 colony forming units (CFU) of B. anthracis spores. Rabbits exposed to a single inhaled dose at or above 2.54 × 104 CFU succumbed with dose-dependent time to death. Death was associated with increases above baseline in heart rate, respiration rate, and body temperature and all rabbits that died exhibited bacteremia at some point prior to death. Rabbits that inhaled doses of 2.06 × 103 CFU or lower survived to the end of the study and showed no or minimal adverse changes in the measured physiological responses in response to the challenge. Moreover, no bacteremia nor toxemia were observed in rabbits that survived to the end of the study. Overall, the data indicate that challenge doses of B. anthracis below the level sufficient to establish systemic infection do not produce observable physiological responses; however, doses that triggered a response resulted in death.

Published

2020

18. The Prophylactic and Therapeutic Efficacy of the Broadly Active Antiviral RibonucleosideN4-Hydroxycytidine (EIDD-1931) in a Mouse Model of Lethal Ebola Virus Infection

Author

Gregory R. Bluemling, Shuli Mao, Michael G. Natchus, Wendy Painter, Sabue Mulangu, Mark Lockwood, Abel De La Rosa, Trevor Brasel, Jason E. Comer, Alexander N. Freiberg, Alexander A. Kolykhalov, and George R. Painter

Abstract

The unprecedented magnitude of the 2013-2016 Ebola virus (EBOV) epidemic in West Africa resulted in over 11,000 deaths and spurred an international public health emergency. A second outbreak in 2018-2020 in DRC resulted in an additional >3400 cases and nearly 2300 deaths (WHO Disease Outbreak News: Update 26 June, 2020). These large outbreaks across geographically diverse regions highlight the need for the development of effective oral therapeutic agents that can be easily distributed for self-administration to populations with active disease or at risk of infection. Herein, we report the in vivo efficacy ofN4-hydroxycytidine (EIDD-1931), a broadly active ribonucleoside analog and the active metabolite of the prodrug EIDD-2801 (molnupiravir), in murine models of lethal EBOV infection. Twice daily oral dosing with EIDD-1931 at 200 mg/kg for 7 days, initiated either with a prophylactic dose 2 hours before infection, or as therapeutic treatment starting 6 hours post-infection, resulted in 92-100% survival of mice challenged with lethal doses of EBOV, reduced clinical signs of Ebola virus disease (EVD), reduced serum virus titers, and facilitated weight loss recovery. These results support further investigation of molnupiravir as a potential therapeutic or prophylactic treatment for EVD.

Published

2022

19. The prophylactic and therapeutic efficacy of the broadly active antiviral ribonucleoside N

Author

Gregory R, Bluemling, Shuli, Mao, Michael G, Natchus, Wendy, Painter, Sabue, Mulangu, Mark, Lockwood, Abel, De La Rosa, Trevor, Brasel, Jason E, Comer, Alexander N, Freiberg, Alexander A, Kolykhalov, and George R, Painter

Abstract

The unprecedented magnitude of the 2013-2016 Ebola virus (EBOV) epidemic in West Africa resulted in over 11 000 deaths and spurred an international public health emergency. A second outbreak in 2018-2020 in DRC resulted in an additional3400 cases and nearly 2300 deaths (WHO, 2020). These large outbreaks across geographically diverse regions highlight the need for the development of effective oral therapeutic agents that can be easily distributed for self-administration to populations with active disease or at risk of infection. Herein, we report the in vivo efficacy of N

Published

2022

20. Filovirus Virulence in Interferon α/β and γ Double Knockout Mice, and Treatment with Favipiravir

Author

Jason E. Comer, Olivier Escaffre, Natasha Neef, Trevor Brasel, Terry L. Juelich, Jennifer K. Smith, Jeanon Smith, Birte Kalveram, David D. Perez, Shane Massey, Lihong Zhang, and Alexander N. Freiberg

Subjects

filovirus, Ebola virus, mouse, interferon receptor knockout, Microbiology, QR1-502

Abstract

The 2014 Ebolavirus outbreak in West Africa highlighted the need for vaccines and therapeutics to prevent and treat filovirus infections. A well-characterized small animal model that is susceptible to wild-type filoviruses would facilitate the screening of anti-filovirus agents. To that end, we characterized knockout mice lacking α/β and γ interferon receptors (IFNAGR KO) as a model for wild-type filovirus infection. Intraperitoneal challenge of IFNAGR KO mice with several known human pathogenic species from the genus Ebolavirus and Marburgvirus, except Bundibugyo ebolavirus and Taï Forest ebolavirus, caused variable mortality rate. Further characterization of the prototype Ebola virus Kikwit isolate infection in this KO mouse model showed 100% lethality down to a dilution equivalent to 1.0 × 10−1 pfu with all deaths occurring between 7 and 9 days post-challenge. Viral RNA was detectable in serum after challenge with 1.0 × 102 pfu as early as one day after infection. Changes in hematology and serum chemistry became pronounced as the disease progressed and mirrored the histological changes in the spleen and liver that were also consistent with those described for patients with Ebola virus disease. In a proof-of-principle study, treatment of Ebola virus infected IFNAGR KO mice with favipiravir resulted in 83% protection. Taken together, the data suggest that IFNAGR KO mice may be a useful model for early screening of anti-filovirus medical countermeasures.

Published

2019

21. Venezuelan equine encephalitis vaccine with rearranged genome resists reversion and protects non-human primates from viremia after aerosol challenge

Author

H. William S. Lawrence, Kenneth S. Plante, Divya Mirchandani, Alexander Tibbens, Eryu Wang, Jason E. Comer, Igor S. Lukashevich, Jennifer E. Peel, Tek N. Lamichhane, Irina Tretyakova, Peter Pushko, Shannan L. Rossi, Scott C. Weaver, and Sif Gudjohnsen

Subjects

viruses, 030231 tropical medicine, Population, Viremia, Biology, Antibodies, Viral, medicine.disease_cause, Virus, DNA vaccination, Encephalitis Virus, Venezuelan Equine, 03 medical and health sciences, 0302 clinical medicine, Chlorocebus aethiops, medicine, Animals, 030212 general & internal medicine, education, Vero Cells, Aerosols, education.field_of_study, Attenuated vaccine, General Veterinary, General Immunology and Microbiology, Immunogenicity, Public Health, Environmental and Occupational Health, Encephalomyelitis, Venezuelan Equine, Viral Vaccines, medicine.disease, Antibodies, Neutralizing, Virology, Vaccination, Infectious Diseases, Venezuelan equine encephalitis virus, Macaca, Molecular Medicine

Abstract

Live-attenuated V4020 vaccine for Venezuelan equine encephalitis virus (VEEV) containing attenuating rearrangement of the virus structural genes was evaluated in a non-human primate model for immunogenicity and protective efficacy against aerosol challenge with wild-type VEEV. The genomic RNA of V4020 vaccine virus was encoded in the pMG4020 plasmid under control of the CMV promoter and contained the capsid gene downstream from the glycoprotein genes. It also included attenuating mutations from the VEE TC83 vaccine, with E2-120Arg substitution genetically engineered to prevent reversion mutations. The population of V4020 vaccine virus derived from pMG4020-transfected Vero cells was characterized by next generation sequencing (NGS) and indicated no detectable genetic reversions. Cynomolgus macaques were vaccinated with V4020 vaccine virus. After one or two vaccinations including by intramuscular route, high levels of virus-neutralizing antibodies were confirmed with no viremia or apparent adverse reactions to vaccinations. The protective effect of vaccination was evaluated using an aerosol challenge with VEEV. After challenge, macaques had no detectable viremia, demonstrating a protective effect of vaccination with live V4020 VEEV vaccine.

Published

2020

22. Evaluation of molnupiravir (EIDD-2801) efficacy against SARS-CoV-2 in the rhesus macaque model

Author

Dylan M. Johnson, Trevor Brasel, Shane Massey, Tania Garron, Michael Grimes, Jeanon Smith, Maricela Torres, Shannon Wallace, Alejandro Villasante-Tezanos, David W. Beasley, and Jason E. Comer

Subjects

Pharmacology, Virology

Abstract

Molnupiravir (EIDD-2801) is a prodrug of a ribonucleoside analogue that is currently being used under a US FDA emergency use authorization for the treatment of mild to moderate COVID-19. We evaluated molnupiravir for efficacy as an oral treatment in the rhesus macaque model of SARS-CoV-2 infection. Twenty non-human primates (NHPs) were challenged with SARS-CoV-2 and treated with 75 mg/kg (n = 8) or 250 mg/kg (n = 8) of molnupiravir twice daily by oral gavage for 7 days. The NHPs were observed for 14 days post-challenge and monitored for clinical signs of disease. After challenge, all groups showed a trend toward increased respiration rates. Treatment with molnupiravir significantly reduced viral RNA levels in bronchoalveolar lavage (BAL) samples at Days 7 and 10. Considering the mild to moderate nature of SARS-CoV-2 infection in the rhesus macaque model, this study highlights the importance of monitoring the viral load in the lung as an indicator of pharmaceutical efficacy for COVID-19 treatments. Additionally, this study provides evidence of the efficacy of molnupiravir which supplements the current ongoing clinical trials of this drug.

Published

2023

23. The prophylactic and therapeutic efficacy of the broadly active antiviral ribonucleoside N-Hydroxycytidine (EIDD-1931) in a mouse model of lethal Ebola virus infection

Author

Gregory R. Bluemling, Shuli Mao, Michael G. Natchus, Wendy Painter, Sabue Mulangu, Mark Lockwood, Abel De La Rosa, Trevor Brasel, Jason E. Comer, Alexander N. Freiberg, Alexander A. Kolykhalov, and George R. Painter

Subjects

Pharmacology, Virology

Published

2023

24. STAT-1 Knockout Mice as a Model for Wild-Type Sudan Virus (SUDV)

Author

David Perez, Olivier Escaffre, Jeanon N. Smith, Lihong Zhang, Alexander N. Freiberg, Terry L. Juelich, Tetsuro Ikegami, Natasha Neef, Trevor Brasel, Shane Massey, Birte Kalveram, Jennifer K. Smith, and Jason E. Comer

Subjects

Male, 0301 basic medicine, Zaire ebolavirus, filovirus, SUDV, 030106 microbiology, Sudan ebolavirus, Spleen, Viremia, Favipiravir, Antibodies, Viral, medicine.disease_cause, Antiviral Agents, Microbiology, Article, Virus, Mice, Viral Proteins, 03 medical and health sciences, Virology, medicine, Animals, ebolavirus, Mice, Knockout, Ebolavirus, STAT-1 knockout mice, biology, animal model, Hemorrhagic Fever, Ebola, biology.organism_classification, medicine.disease, Amides, QR1-502, Bundibugyo ebolavirus, Disease Models, Animal, STAT1 Transcription Factor, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, Pyrazines, Female

Abstract

Currently there is no FDA-licensed vaccine or therapeutic against Sudan ebolavirus (SUDV) infections. The largest ever reported 2014–2016 West Africa outbreak, as well as the 2021 outbreak in the Democratic Republic of Congo, highlight the critical need for countermeasures against filovirus infections. A well-characterized small animal model that is susceptible to wild-type filoviruses would greatly add to the screening of antivirals and vaccines. Here, we infected signal transducer and activator of transcription-1 knock out (STAT-1 KO) mice with five different wildtype filoviruses to determine susceptibility. SUDV and Marburg virus (MARV) were the most virulent, and caused 100% or 80% lethality, respectively. Zaire ebolavirus (EBOV), Bundibugyo ebolavirus (BDBV), and Taï Forest ebolavirus (TAFV) caused 40%, 20%, and no mortality, respectively. Further characterization of SUDV in STAT-1 KO mice demonstrated lethality down to 3.1 × 101 pfu. Viral genomic material was detectable in serum as early as 1 to 2 days post-challenge. The onset of viremia was closely followed by significant changes in total white blood cells and proportion of neutrophils and lymphocytes, as well as by an influx of neutrophils in the liver and spleen. Concomitant significant fluctuations in blood glucose, albumin, globulin, and alanine aminotransferase were also noted, altogether consistent with other models of filovirus infection. Finally, favipiravir treatment fully protected STAT-1 KO mice from lethal SUDV challenge, suggesting that this may be an appropriate small animal model to screen anti-SUDV countermeasures.

Published

2021

25. Natural history of disease in cynomolgus monkeys exposed to Ebola virus Kikwit strain demonstrates the reliability of this non-human primate model for Ebola virus disease

Author

Lucy A Ward, Aysegul Nalca, Ricardo Carrion, Trevor Brasel, Arthur J. Goff, Hilary M. Staples, Alisha Rajbhandari, Margaret L. Pitt, Andrew Kocsis, John Trefry, Anthony Griffiths, Jason E. Comer, Cheryl A. Triplett, Nancy A. Niemuth, Clint Florence, Kendra J. Alfson, Dawn Fallacara, Amy C. Shurtleff, Shane Massey, Jake Lowry, Michael P. Fay, Sanjay M. Tamrakar, Yenny Goez-Gazi, Jeanon N. Smith, and Sara C. Johnston

Subjects

0301 basic medicine, RNA viruses, Male, Physiology, Filoviridae, medicine.disease_cause, Pathology and Laboratory Medicine, Body Temperature, Disease Outbreaks, 0302 clinical medicine, Medical Conditions, Mathematical and Statistical Techniques, Medicine and Health Sciences, Medicine, 030212 general & internal medicine, Vaccines, Multidisciplinary, biology, Statistics, Animal Models, Viral Load, Metaanalysis, Ebolavirus, Body Fluids, Infectious Diseases, Blood, Physiological Parameters, Experimental Organism Systems, Medical Microbiology, Filoviruses, Viral Pathogens, Viruses, Physical Sciences, Female, Pathogens, Anatomy, Ebola Virus, Viral load, Research Article, Infectious Disease Control, Science, Viremia, Research and Analysis Methods, Natural history of disease, Microbiology, 03 medical and health sciences, Virology, Animals, Statistical Methods, Microbial Pathogens, Ebola virus, Biology and life sciences, business.industry, Hemorrhagic Fever Viruses, Euthanasia, Organisms, Outbreak, Reproducibility of Results, Hemorrhagic Fever, Ebola, biology.organism_classification, Marburgvirus, medicine.disease, Blood Counts, Disease Models, Animal, Macaca fascicularis, 030104 developmental biology, Animal Studies, business, Viral Transmission and Infection, Mathematics

Abstract

Filoviruses (Family Filoviridae genera Ebolavirus and Marburgvirus) are negative-stranded RNA viruses that cause severe health effects in humans and non-human primates, including death. Except in outbreak settings, vaccines and other medical countermeasures against Ebola virus (EBOV) will require testing under the FDA Animal Rule. Multiple vaccine candidates have been evaluated using cynomolgus monkeys (CM) exposed to EBOV Kikwit strain. To the best of our knowledge, however, animal model development data supporting the use of CM in vaccine research have not been submitted to the FDA. This study describes a large CM database (122 CM, 62 female and 60 male, age 2 to 9 years) and demonstrates the consistency of the CM model through time to death models and descriptive statistics. CMs were exposed to EBOV doses of 0.1 to 100,000 PFU in 33 studies conducted at three Animal Biosafety Level 4 facilities, by three exposure routes. Time to death was modeled using Cox proportional hazards models with a frailty term that incorporated study-to-study variability. Despite significant differences attributed to exposure variables, all CMs exposed to the 100 to 1,000 pfu doses commonly used in vaccine studies died or met euthanasia criteria within 21 days of exposure, median 7 days, 93% between 5 and 12 days of exposure. Moderate clinical signs were observed 4 to 5 days after exposure and preceded death or euthanasia by approximately one day. Viremia was detected within a few days of infection. Hematology indices were indicative of viremia and the propensity for hemorrhage with progression of Ebola viremia. Changes associated with coagulation parameters and platelets were consistent with coagulation disruption. Changes in leukocyte profiles were indicative of an acute inflammatory response. Increased liver enzymes were observed shortly after exposure. Taken together, these factors suggest that the cynomolgus monkey is a reliable animal model for human disease.

Published

2021

26. Immunogenicity and Efficacy of a Measles Virus-Vectored Chikungunya Vaccine in Nonhuman Primates

Author

Shannan L. Rossi, William S Lawrence, Sabrina Schrauf, Jessica A. Plante, Eryu Wang, Jason E. Comer, Scott C. Weaver, Katrin Ramsauer, and Sasha R. Azar

Subjects

Male, 0301 basic medicine, Antibodies, Viral, medicine.disease_cause, Body Temperature, Immunogenicity, Vaccine, vaccine, Immunology and Allergy, Medicine, Chikungunya, Neutralizing antibody, Vaccines, biology, Immunogenicity, Vaccination, virus diseases, 3. Good health, Infectious Diseases, Cytokines, Female, Genetic Vectors, Measles Vaccine, 030106 microbiology, Immunization, Secondary, nonhuman primate, Viremia, Measles, Virus, Measles virus, Major Articles and Brief Reports, 03 medical and health sciences, Animals, Humans, chikungunya virus, business.industry, Viral Vaccines, biology.organism_classification, medicine.disease, Antibodies, Neutralizing, Virology, Disease Models, Animal, Macaca fascicularis, 030104 developmental biology, 13. Climate action, biology.protein, Chikungunya Fever, business

Abstract

Background Chikungunya virus (CHIKV) infection can result in chikungunya fever (CHIKF), a self-limited acute febrile illness that can progress to chronic arthralgic sequelae in a large percentage of patients. A new measles virus-vectored vaccine was developed to prevent CHIKF, and we tested it for immunogenicity and efficacy in a nonhuman primate model. Methods Nine cynomolgus macaques were immunized and boosted with the measles virus-vectored chikungunya vaccine or sham-vaccinated. Sera were taken at multiple times during the vaccination phase to assess antibody responses against CHIKV. Macaques were challenged with a dose of CHIKV previously shown to cause fever and viremia, and core body temperature, viremia, and blood cell and chemistry panels were monitored. Results The vaccine was well tolerated in all macaques, and all seroconverted (high neutralizing antibody [PRNT80 titers, 40–640] and enzyme-linked immunosorbent assay titers) after the boost. Furthermore, the vaccinated primates were protected against viremia, fever, elevated white blood cell counts, and CHIKF-associated cytokine changes after challenge with the virulent La Reunión CHIKV strain. Conclusions These results further document the immunogenicity and efficacy of a measles-vectored chikungunya vaccine that shows promise in Phase I–II clinical trials. These findings are critical to human health because no vaccine to combat CHIKF is yet licensed., Chikungunya fever is a debilitating human disease. A measles-based vaccine expressing chikungunya proteins can protect nonhuman primates from disease, including fever, white blood cell count reduction, viremia, and proinflammatory cytokine levels. Lineage cross-reactive antibodies are also produced.

Published

2019

27. Mucosal Challenge Ferret Models of Ebola Virus Disease

Author

Cheryl A. Triplett, Jason E. Comer, Jeanon N. Smith, Trevor Brasel, Melicia Gainey, Nancy A. Niemuth, Shane Massey, Jennifer K. Smith, Andrew Kocsis, Thomas L. Rudge, and Matthew Hyde

Subjects

0301 basic medicine, Microbiology (medical), medicine.medical_specialty, mucosal challenge, 030106 microbiology, lcsh:Medicine, Mucous membrane of nose, Disease, medicine.disease_cause, Virus, Article, 03 medical and health sciences, Ebola virus, medicine, Immunology and Allergy, Molecular Biology, ferret, General Immunology and Microbiology, Clinical pathology, business.industry, lcsh:R, 030104 developmental biology, Infectious Diseases, Immunology, Histopathology, Nasal administration, business, Viral load

Abstract

Recent studies have shown the domestic ferret (Mustela putorius furo) to be a promising small animal model for the study of Ebola virus (EBOV) disease and medical countermeasure evaluation. To date, most studies have focused on traditional challenge routes, predominantly intramuscular and intranasal administration. Here, we present results from a non-clinical pathogenicity study examining oronasal, oral, and ocular mucosal challenge routes in ferrets. Animals were challenged with 1, 10, or 100 plaque forming units EBOV followed by monitoring of disease progression and biosampling. Ferrets administered virus via oronasal and oral routes met euthanasia criteria due to advanced disease 5–10 days post-challenge. Conversely, all ferrets dosed via the ocular route survived until the scheduled study termination 28-day post-challenge. In animals that succumbed to disease, a dose/route response was not observed, increases in disease severity, febrile responses, serum and tissue viral load, alterations in clinical pathology, and gross/histopathology findings were similar between subjects. Disease progression in ferrets challenged via ocular administration was unremarkable throughout the study period. Results from this study further support the ferret as a model for EBOV disease following oral and nasal mucosa exposure.

Published

2021

28. A synthetic peptide CTL vaccine targeting nucleocapsid confers protection from SARS-CoV-2 challenge in rhesus macaques

Author

Scott Burkholz, Thomas Bey, Reid M. Rubsamen, Paul L. Harris, Christopher Massey, Thomas Hodge, C. V. Herst, Peter M. Lloyd, Richard Carback, Trevor Brasel, Tikoes Blankenberg, Jason E. Comer, Lu Wang, and Serban Ciotlos

Subjects

0301 basic medicine, viruses, Immunology, Macaque, Article, Epitope, 03 medical and health sciences, 0302 clinical medicine, Immune system, COVID-19 (Disease), vaccine, biology.animal, Drug Discovery, MHC class I, Pharmacology (medical), Pharmacology, Vaccines, biology, SARS-CoV-2, animal model, macaque, T cell, Viral proteins, MHC class I peptide, Virology, respiratory tract diseases, Vaccination, CTL, 030104 developmental biology, Infectious Diseases, 030220 oncology & carcinogenesis, Vaccines--Research, biology.protein, Peptide vaccine, Medicine, Viral load

Abstract

BackgroundPersistent transmission of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) has given rise to a COVID-19 pandemic. Several vaccines, evoking protective spike antibody responses, conceived in 2020, are being deployed in mass public health vaccination programs. Recent data suggests, however, that as sequence variation in the spike genome accumulates, some vaccines may lose efficacy.MethodsUsing a macaque model of SARS-CoV-2 infection, we tested the efficacy of a peptide-based vaccine targeting MHC Class I epitopes on the SARS-CoV-2 nucleocapsid protein. We administered biodegradable microspheres with synthetic peptides and adjuvants to rhesus macaques. Unvaccinated control and vaccinated macaques were challenged with 1 x 108 TCID50 units of SARS-CoV-2, followed by assessment of clinical symptoms, viral load, chest radiographs, sampling of peripheral blood and bronchoalveolar lavage (BAL) fluid for downstream analysis.ResultsVaccinated animals were free of pneumonia-like infiltrates characteristic of SARS-CoV-2 infection and presented with lower viral loads relative to controls. Gene expression in cells collected from BAL samples of vaccinated macaques revealed a unique signature associated with enhanced development of adaptive immune responses relative to control macaques.ConclusionsWe demonstrate that a room temperature stable peptide vaccine based on known immunogenic HLA Class I bound CTL epitopes from the nucleocapsid protein can provide protection against SARS-CoV-2 infection in non-human primates.Graphical Abstract

Published

2021

29. The Fc-mediated effector functions of a potent SARS-CoV-2 neutralizing antibody, SC31, isolated from an early convalescent COVID-19 patient, are essential for the optimal therapeutic efficacy of the antibody

Author

Chien-Te K Tseng, Dipti Thakkar, Boyd-Kirkup Jerome Douglas, Trevor Brasel, Paul A. MacAry, Dong Ling Wang, Jason E. Comer, Hannes Hentze, Ingram Piers, Brendon J. Hanson, Angeline P.C. Lim, Guan Siyu, Maricela Torres, Kiren Purushotorman, Damian O’Connell, Jacklyn J.Y. Neo, Guo Hui Teo, Steven K.K. Wong, Conrad E.Z. Chan, Shirley Gek Kheng Seah, Venkateshan S. Prativadibhayankara, Paul Edward Hutchinson, De Hoe Chye, Jenny G. Low, Gary S.L. Loh, Kantharaj Ethirajulu, David C. Lye, Jie Hui Lim, Pui San Wong, Barnaby Edward Young, Alan D.T. Barrett, and Shane Massey

Subjects

Genetically modified mouse, biology, business.industry, Epitope, Immune system, In vivo, Immunology, biology.protein, Medicine, Antibody-dependent enhancement, Antibody, business, Neutralizing antibody, Viral load

Abstract

SARS-CoV-2-neutralizing antibodies are promising therapeutics for COVID-19. However, little is known about the mechanisms of action of these antibodies or their effective dosing windows. We report the discovery and development of SC31, a potent SARS-CoV-2 neutralizing IgG1 antibody, originally isolated from a convalescent patient at day 27 after the onset of symptoms. Neutralization occurs via a binding epitope that maps within the ACE2 interface of the SARS-CoV-2 Spike protein, conserved across all common circulating SARS-CoV-2 mutants. In SARS-CoV-2 infected K18-human ACE2 transgenic mice, SC31 demonstrated potent survival benefit by dramatically reducing viral load concomitant with attenuated pro-inflammatory responses linked to severe systemic disease, such as IL-6. Comparison with a Fc-null LALA variant of SC31 demonstrated that optimal therapeutic efficacy of SC31 requires intact Fc-mediated effector functions that can further induce an IFNγ-driven anti-viral immune response. Dose-dependent efficacy for SC31 was observed down to 5mg/kg when dosed before the activation of lung inflammatory responses. Importantly, despite FcγR binding, no evidence of antibody dependent enhancement was observed with the Fc-competent SC31 even at sub-therapeutic doses. Therapeutic efficacy was confirmed in SARS-CoV-2-infected hamsters, where SC31 again significantly reduced viral load, decreased lung lesions and inhibited progression to severe disease manifestations. This study underlines the potential for significant COVID-19 patient benefit for the SC31 antibody that justifies rapid advancement to the clinic, as well as highlighting the importance of appropriate mechanistic and functional studies during development.One Sentence SummaryAnti-SARS-CoV-2 IgG1 antibody SC31 controls infectionin vivoby blocking SP:ACE2 binding and triggering a Fc-mediated anti-viral response.

Published

2020

30. Physiological Responses to Multiple Low-Doses of Bacillus anthracis Spores in the Rabbit Model of Inhalation Anthrax

Author

Stephanie A. Hines, Tonya L. Nichols, Gregory V. Stark, Sarah C. Taft, Roy E. Barnewall, and Jason E. Comer

Subjects

Microbiology (medical), low-dose, 040301 veterinary sciences, Physiology, lcsh:Medicine, Article, 0403 veterinary science, 03 medical and health sciences, Respiration, medicine, Immunology and Allergy, Molecular Biology, Bacillus anthracis, 030304 developmental biology, Inhalation exposure, Colony-forming unit, dose-response, 0303 health sciences, General Immunology and Microbiology, biology, business.industry, lcsh:R, fungi, anthrax, 04 agricultural and veterinary sciences, biology.organism_classification, medicine.disease, Pathophysiology, Spore, Infectious Diseases, Bacteremia, multiple dose, pathology, physiological response, business, Respiration rate

Abstract

Bacillus anthracis spores that are re-aerosolized from surface deposits after initial contamination present significant health risks for personnel involved in decontamination. To model repeated exposure to low dose B. anthracis spores, three groups of seven rabbits were challenged with multiple low-doses of B. anthracis spores 5 days a week for 3 weeks. Mortality, body temperature, heart and respiration rates, hematology, C-reactive protein, bacteremia, and serum protective antigen were monitored for 21 days post-exposure after the last of multiple doses. All rabbits exposed to a mean daily dose of 2.91 &times, 102 colony forming units (CFU) survived and showed minimal physiological changes attributable to exposure. One of seven rabbits receiving a mean daily dose of 1.22 &times, 103 CFU died and four of seven receiving a mean daily dose of 1.17 &times, 104 CFU died. The LD50 was calculated to be 8.1 &times, 103 CFU of accumulated dose. Rabbits that succumbed to the higher dose exhibited bacteremia and increases above baseline in heart rate, respiration rate, and body temperature. Two rabbits in the mean daily dose group of 1.17 &times, 104 CFU exhibited clinical signs of inhalation anthrax yet survived. This study provides a description of lethality, pathophysiology, and pathology in a controlled multiple low-dose inhalation exposure study of B. anthracis in the rabbit model. The data suggest that the accumulated dose is important in survival outcome and that a subset of rabbits may show clinical signs of disease but fully recover without therapeutic intervention

Published

2020

31. Teixobactin Provides Protection against Inhalation Anthrax in the Rabbit Model

Author

Johnny W. Peterson, Elbert B. Whorton, Jason E. Comer, William S Lawrence, Satheesh K Sivasubramani, Dallas Hughes, Losee L Ling, David W.C. Beasley, Jennifer E. Peel, and Wallace B. Baze

Subjects

0301 basic medicine, Microbiology (medical), medicine.drug_class, 030106 microbiology, Antibiotics, Teixobactin, lcsh:Medicine, Article, Microbiology, rabbit model, 03 medical and health sciences, Levofloxacin, antibiotic, medicine, Immunology and Allergy, protective antigen, Molecular Biology, Bacillus anthracis, inhalation, General Immunology and Microbiology, Inhalation, biology, business.industry, Lethal dose, lcsh:R, anthrax, biology.organism_classification, medicine.disease, infection, 030104 developmental biology, Infectious Diseases, Bacteremia, business, Bacteria, medicine.drug

Abstract

The use of antibiotics is a vital means of treating infections caused by the bacteria Bacillus (B.) anthracis. Importantly, with the potential future use of multidrug-resistant strains of B. anthracis as bioweapons, new antibiotics are needed as alternative therapeutics. In this blinded study, we assessed the protective efficacy of teixobactin, a recently discovered antibiotic, against inhalation anthrax infection in the adult rabbit model. New Zealand White rabbits were infected with a lethal dose of B. anthracis Ames spores via the inhalation route, and blood samples were collected at various times to assess antigenemia, bacteremia, tissue bacterial load, and antibody production. Treatments were administered upon detection of B. anthracis protective antigen in the animals&rsquo, sera. For comparison, a fully protective dose of levofloxacin was used as a positive control. Rabbits treated with teixobactin showed 100% survival following infection, and the bacteremia was completely resolved by 24&ndash, 48 h post-treatment. In addition, the bacterial/spore loads in tissues of the animals treated with teixobactin were either zero or dramatically less relative to that of the negative control animals. Moreover, microscopic evaluation of the tissues revealed decreased pathology following treatment with teixobactin. Overall, these results show that teixobactin was protective against inhalation anthrax infection in the rabbit model, and they indicate the potential of teixobactin as a therapeutic for the disease.

Published

2020

32. Achieving consistent multiple daily low-dose Bacillus anthracis spore inhalation exposures in the rabbit model

Author

Roy E Barnewall, Jason E Comer, Brian eMiller, Bradford W Gutting, Daniel N Wolfe, Alison E Director-Myska, Tonya L Nichols, and Sarah C Taft

Subjects

Anthrax, Bacillus anthracis, Spores, Inhalation exposures, Low-dose, Subchronic exposures, Microbiology, QR1-502

Abstract

Repeated low-level exposures to Bacillus anthracis could occur before or after the remediation of an environmental release. This is especially true for persistent agents such as Bacillus anthracis spores, the causative agent of anthrax. Studies were conducted to examine aerosol methods needed for consistent daily low aerosol concentrations to deliver a low-dose (less than 106 colony forming units (CFU) of B. anthracis spores) and included a pilot feasibility characterization study, acute exposure study, and a multiple fifteen day exposure study. This manuscript focuses on the state-of-the-science aerosol methodologies used to generate and aerosolize consistent daily low aerosol concentrations and resultant low inhalation doses. The pilot feasibility characterization study determined that the aerosol system was consistent and capable of producing very low aerosol concentrations. In the acute, single day exposure experiment, targeted inhaled doses of 1 x 102, 1 x 103, 1 x 104, and 1 x 105 CFU were used. In the multiple daily exposure experiment, rabbits were exposed multiple days to targeted inhaled doses of 1 x 102, 1 x 103, and 1 x 104 CFU. In all studies, targeted inhaled doses remained fairly consistent from rabbit to rabbit and day to day. The aerosol system produced aerosolized spores within the optimal mass median aerodynamic diameter particle size range to reach deep lung alveoli. Consistency of the inhaled dose was aided by monitoring and recording respiratory parameters during the exposure with real-time plethysmography. Overall, the presented results show that the animal aerosol system was stable and highly reproducible between different studies and multiple exposure days.

Published

2012

33. The Fc-mediated effector functions of a potent SARS-CoV-2 neutralizing antibody, SC31, isolated from an early convalescent COVID-19 patient, are essential for the optimal therapeutic efficacy of the antibody

Author

Jie Hui Lim, Pui San Wong, Steven K.K. Wong, Chien Te K. Tseng, Guan Siyu, Paul A. MacAry, Shane Massey, Shirley Gek Kheng Seah, Alan D.T. Barrett, Dipti Thakkar, Jenny G. Low, Guo Hui Teo, Kantharaj Ethirajulu, Jason E. Comer, Brendon J. Hanson, Boyd-Kirkup Jerome Douglas, Ingram Piers, Venkateshan S. Prativadibhayankara, Barnaby Edward Young, Trevor Brasel, Angeline P.C. Lim, Hannes Hentze, Maricela Torres, Dongling Wang, Kiren Purushotorman, Jacklyn J.Y. Neo, Conrad E.Z. Chan, De Hoe Chye, Paul Edward Hutchinson, and Gary S.L. Loh

Subjects

RNA viruses, Male, 0301 basic medicine, Viral Diseases, Chemokine, Physiology, Coronaviruses, Cancer Treatment, Monkeys, Biochemistry, Epitope, Neutralization, Immunoglobulin G, Medical Conditions, 0302 clinical medicine, Immune Physiology, Cricetinae, Chlorocebus aethiops, Medicine and Health Sciences, Medicine, 030212 general & internal medicine, Enzyme-Linked Immunoassays, Neutralizing antibody, Pathology and laboratory medicine, Mammals, Immune System Proteins, Multidisciplinary, biology, Eukaryota, Medical microbiology, Viral Load, Infectious Diseases, Oncology, Viruses, Vertebrates, Spike Glycoprotein, Coronavirus, Hamsters, Cytokines, Female, Angiotensin-Converting Enzyme 2, SARS CoV 2, Pathogens, Chemokines, Antibody, Viral load, Macaque, Research Article, Primates, SARS coronavirus, Science, Immunology, Mice, Transgenic, Research and Analysis Methods, Microbiology, Rodents, Antibodies, 03 medical and health sciences, Immune system, Antibody Therapy, Virology, Old World monkeys, Animals, Humans, Immunoassays, Vero Cells, Dose-Response Relationship, Drug, SARS-CoV-2, business.industry, Organisms, Viral pathogens, Biology and Life Sciences, Proteins, COVID-19, Covid 19, Convalescence, Antibodies, Neutralizing, Macaca mulatta, Microbial pathogens, Immunoglobulin Fc Fragments, Disease Models, Animal, 030104 developmental biology, Amniotes, Immunologic Techniques, biology.protein, Clinical Immunology, Clinical Medicine, business, Zoology, Viral Transmission and Infection

Abstract

Although SARS-CoV-2-neutralizing antibodies are promising therapeutics against COVID-19, little is known about their mechanism(s) of action or effective dosing windows. We report the generation and development of SC31, a potent SARS-CoV-2 neutralizing antibody, isolated from a convalescent patient. Antibody-mediated neutralization occurs via an epitope within the receptor-binding domain of the SARS-CoV-2 Spike protein. SC31 exhibited potent anti-SARS-CoV-2 activities in multiple animal models. In SARS-CoV-2 infected K18-human ACE2 transgenic mice, treatment with SC31 greatly reduced viral loads and attenuated pro-inflammatory responses linked to the severity of COVID-19. Importantly, a comparison of the efficacies of SC31 and its Fc-null LALA variant revealed that the optimal therapeutic efficacy of SC31 requires Fc-mediated effector functions that promote IFNγ-driven anti-viral immune responses, in addition to its neutralization ability. A dose-dependent efficacy of SC31 was observed down to 5mg/kg when administered before viral-induced lung inflammatory responses. In addition, antibody-dependent enhancement was not observed even when infected mice were treated with SC31 at sub-therapeutic doses. In SARS-CoV-2-infected hamsters, SC31 treatment significantly prevented weight loss, reduced viral loads, and attenuated the histopathology of the lungs. In rhesus macaques, the therapeutic potential of SC31 was evidenced through the reduction of viral loads in both upper and lower respiratory tracts to undetectable levels. Together, the results of our preclinical studies demonstrated the therapeutic efficacy of SC31 in three different models and its potential as a COVID-19 therapeutic candidate.

Published

2021

34. Modeling Rabbit Responses to Single and Multiple Aerosol Exposures ofBacillus anthracisSpores

Author

Margaret E. Coleman, Darrell W. Donahue, Harry M. Marks, Jason E. Comer, Sarah C. Taft, Stephanie A. Hines, and Timothy A. Bartrand

Subjects

0301 basic medicine, Empirical data, 030106 microbiology, Baseline model, Biology, biology.organism_classification, Aerosol, Bacillus anthracis, Data set, 03 medical and health sciences, 030104 developmental biology, Dosing schedules, Physiology (medical), Statistics, Safety, Risk, Reliability and Quality, Survival analysis, Weibull distribution

Abstract

Survival models are developed to predict response and time-to-response for mortality in rabbits following exposures to single or multiple aerosol doses of Bacillus anthracis spores. Hazard function models were developed for a multiple-dose data set to predict the probability of death through specifying functions of dose response and the time between exposure and the time-to-death (TTD). Among the models developed, the best-fitting survival model (baseline model) is an exponential dose-response model with a Weibull TTD distribution. Alternative models assessed use different underlying dose-response functions and use the assumption that, in a multiple-dose scenario, earlier doses affect the hazard functions of each subsequent dose. In addition, published mechanistic models are analyzed and compared with models developed in this article. None of the alternative models that were assessed provided a statistically significant improvement in fit over the baseline model. The general approach utilizes simple empirical data analysis to develop parsimonious models with limited reliance on mechanistic assumptions. The baseline model predicts TTDs consistent with reported results from three independent high-dose rabbit data sets. More accurate survival models depend upon future development of dose-response data sets specifically designed to assess potential multiple-dose effects on response and time-to-response. The process used in this article to develop the best-fitting survival model for exposure of rabbits to multiple aerosol doses of B. anthracis spores should have broad applicability to other host-pathogen systems and dosing schedules because the empirical modeling approach is based upon pathogen-specific empirically-derived parameters.

Published

2017

35. Repurposing the antimalarial pyronaridine tetraphosphate to protect against Ebola virus infection

Author

Joel S. Freundlich, Peter B. Madrid, Manu Anantpadma, Sean Ekins, Robert A. Davey, Jason E. Comer, Thomas J. Lane, and Christopher Massey

Subjects

Male, RNA viruses, 0301 basic medicine, Physiology, RC955-962, Cultured tumor cells, Pathology and Laboratory Medicine, medicine.disease_cause, Mice, chemistry.chemical_compound, 0302 clinical medicine, Immune Physiology, Arctic medicine. Tropical medicine, Medicine and Health Sciences, Medicine, media_common, Mice, Inbred BALB C, Innate Immune System, Chemotaxis, Animal Models, Ebolavirus, Body Fluids, 3. Good health, Cell Motility, Drug repositioning, Blood, Infectious Diseases, Experimental Organism Systems, Medical Microbiology, Filoviruses, Viral Pathogens, Viruses, Cytokines, Cell lines, Female, Anatomy, Pathogens, Chemokines, Public aspects of medicine, RA1-1270, Biological cultures, Ebola Virus, Research Article, Immunology, 030231 tropical medicine, Mouse Models, Viremia, Antiviral Agents, Microbiology, Blood Plasma, Antimalarials, 03 medical and health sciences, Model Organisms, Pharmacokinetics, Animals, Humans, media_common.cataloged_instance, HeLa cells, Naphthyridines, European union, Microbial Pathogens, Pharmacology, Pyronaridine, Ebola virus, Hemorrhagic Fever Viruses, Euthanasia, business.industry, Drug Repositioning, Organisms, Public Health, Environmental and Occupational Health, Biology and Life Sciences, Cell Biology, Hemorrhagic Fever, Ebola, Molecular Development, Cell cultures, medicine.disease, Virology, Research and analysis methods, 030104 developmental biology, chemistry, Artesunate, Immune System, Animal Studies, business, Malaria, Developmental Biology

Abstract

Recent outbreaks of the Ebola virus (EBOV) have focused attention on the dire need for antivirals to treat these patients. We identified pyronaridine tetraphosphate as a potential candidate as it is an approved drug in the European Union which is currently used in combination with artesunate as a treatment for malaria (EC50 between 420 nM—1.14 μM against EBOV in HeLa cells). Range-finding studies in mice directed us to a single 75 mg/kg i.p. dose 1 hr after infection which resulted in 100% survival and statistically significantly reduced viremia at study day 3 from a lethal challenge with mouse-adapted EBOV (maEBOV). Further, an EBOV window study suggested we could dose pyronaridine 2 or 24 hrs post-exposure to result in similar efficacy. Analysis of cytokine and chemokine panels suggests that pyronaridine may act as an immunomodulator during an EBOV infection. Our studies with pyronaridine clearly demonstrate potential utility for its repurposing as an antiviral against EBOV and merits further study in larger animal models with the added benefit of already being used as a treatment against malaria., Author summary To date there is no approved drug for Ebola Virus infection. Our approach has been to assess drugs that are already approved for other uses in various countries. Using computational models, we have previously identified three such drugs and demonstrated their activity against the Ebola virus in vitro. We now report on the in vitro absorption, metabolism, distribution, excretion and pharmacokinetic properties of one of these molecules, namely the antimalarial pyronaridine. We justify efficacy testing in the mouse model of ebola infection. We also demonstrate that a single dose of this drug is 100% effective against the virus. This study provides important preclinical evaluation of this already approved drug and justifies its selection for larger animal efficacy studies.

Published

2019

36. Repurposing Quinacrine against Ebola Virus Infection

Author

Thomas R, Lane, Jason E, Comer, Alexander N, Freiberg, Peter B, Madrid, and Sean, Ekins

Subjects

Mice, Inbred BALB C, Drug Repositioning, Microbial Sensitivity Tests, Tilorone, Hemorrhagic Fever, Ebola, Viral Load, Ebolavirus, Antiviral Agents, Survival Analysis, Antimalarials, Disease Models, Animal, Mice, Quinacrine, Chlorocebus aethiops, Animals, Humans, Caco-2 Cells, Vero Cells, HeLa Cells

Abstract

Quinacrine hydrochloride is a small-molecule, orally bioavailable drug that has been used clinically as an antimalarial and for many other applications. A machine learning model trained on Ebola virus (EBOV) screening data identified quinacrine as a potent (nanomolar) in vitro inhibitor. In the current study, quinacrine 25 mg/kg was shown to protect 70% of mice (statistically significant) from a lethal challenge with mouse-adapted EBOV with once-daily intraperitoneal dosing for 8 days.

Published

2019

37. Filovirus Virulence in Interferon α/β and γ Double Knockout Mice, and Treatment with Favipiravir

Author

Birte Kalveram, Terry L. Juelich, Olivier Escaffre, Alexander N. Freiberg, David Perez, Natasha Neef, Jason E. Comer, Trevor Brasel, Jennifer K. Smith, Jeanon N. Smith, Lihong Zhang, and Shane Massey

Subjects

0301 basic medicine, Male, filovirus, interferon receptor knockout, 030106 microbiology, lcsh:QR1-502, Spleen, Favipiravir, medicine.disease_cause, Antiviral Agents, Proof of Concept Study, lcsh:Microbiology, Article, 03 medical and health sciences, Gene Knockout Techniques, Mice, Ebola virus, Virology, medicine, Filoviridae Infections, Animals, Marburg Virus Disease, mouse, Receptors, Interferon, Ebolavirus, Mice, Knockout, biology, Virulence, Hemorrhagic Fever, Ebola, Marburgvirus, biology.organism_classification, Filoviridae, Amides, Bundibugyo ebolavirus, Disease Models, Animal, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, Liver, Pyrazines, Knockout mouse, RNA, Viral, Female, Taï Forest ebolavirus

Abstract

The 2014 Ebolavirus outbreak in West Africa highlighted the need for vaccines and therapeutics to prevent and treat filovirus infections. A well-characterized small animal model that is susceptible to wild-type filoviruses would facilitate the screening of anti-filovirus agents. To that end, we characterized knockout mice lacking &alpha, /&beta, and &gamma, interferon receptors (IFNAGR KO) as a model for wild-type filovirus infection. Intraperitoneal challenge of IFNAGR KO mice with several known human pathogenic species from the genus Ebolavirus and Marburgvirus, except Bundibugyo ebolavirus and Ta&iuml, Forest ebolavirus, caused variable mortality rate. Further characterization of the prototype Ebola virus Kikwit isolate infection in this KO mouse model showed 100% lethality down to a dilution equivalent to 1.0 &times, 10&minus, 1 pfu with all deaths occurring between 7 and 9 days post-challenge. Viral RNA was detectable in serum after challenge with 1.0 &times, 102 pfu as early as one day after infection. Changes in hematology and serum chemistry became pronounced as the disease progressed and mirrored the histological changes in the spleen and liver that were also consistent with those described for patients with Ebola virus disease. In a proof-of-principle study, treatment of Ebola virus infected IFNAGR KO mice with favipiravir resulted in 83% protection. Taken together, the data suggest that IFNAGR KO mice may be a useful model for early screening of anti-filovirus medical countermeasures.

Published

2019

38. Cell-Type Apoptosis in Lung during SARS-CoV-2 Infection

Author

Tania Garron, Bin Gong, Yuan Qiu, Eric C Gong, Thomas G. Ksiazek, Yakun Liu, Jason E. Comer, Changcheng Zhou, Junying Zheng, Zhengchen Su, Paul J. Boor, Trevor Brasel, Yang Jin, Y Whitney Yin, and Qing Chang

Subjects

Microbiology (medical), ARDS, Cell type, viruses, non-human primate, Lung injury, Article, Umbilical vein, lung, Alveolar cells, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, Immunology and Allergy, Medicine, human, Diffuse alveolar damage, Molecular Biology, 030304 developmental biology, 0303 health sciences, Lung, General Immunology and Microbiology, SARS-CoV-2, business.industry, epithelial cell, apoptosis, TUNEL assay, respiratory system, medicine.disease, co-culture, respiratory tract diseases, Endothelial stem cell, Infectious Diseases, medicine.anatomical_structure, Apoptosis, 030220 oncology & carcinogenesis, endothelial cell, Cancer research, Vero cell, business

Abstract

The SARS-CoV-2 pandemic has inspired renewed interest in understanding the fundamental pathology of acute respiratory distress syndrome (ARDS) following infection because fatal COVID-19 cases are commonly linked to respiratory failure due to ARDS. The pathologic alteration known as diffuse alveolar damage in endothelial and epithelial cells is a critical feature of acute lung injury in ARDS. However, the pathogenesis of ARDS following SRAS-CoV-2 infection remains largely unknown.In the present study, we examined apoptosis in post-mortem lung sections from COVID-19 patients and lung tissues from a non-human primate model of SARS-CoV-2 infection, in a cell-type manner, including type 1 and 2 alveolar cells and vascular endothelial cells (ECs), macrophages, and T cells. Multiple-target immunofluorescence (IF) assays and western blotting suggest both intrinsic and extrinsic apoptotic pathways are activated during SARS-CoV-2 infection. Furthermore, we observed that SARS-CoV-2 fails to induce apoptosis in human bronchial epithelial cells (i.e., BEAS2B cells) and primary human umbilical vein endothelial cells (HUVECs), which are refractory to SARS-CoV-2 infection. However, infection of co-cultured Vero cells and HUVECs or Vero cells and BEAS2B cells with SARS-CoV-2 induced apoptosis in both Vero cells and HUVECs/BEAS2B cells, but did not alter the permissiveness of HUVECs or BEAS2B cells to the virus. Post-exposure treatment of the co-culture of Vero cells and HUVECs with an EPAC1-specific activator ameliorated apoptosis in HUVECs. These findings may help to delineate a novel insight into the pathogenesis of ARDS following SARS-CoV-2 infection.

Published

2021

39. Efficacy of Tilorone Dihydrochloride against Ebola Virus Infection

Author

Claire McFarlane, Jon C. Mirsalis, Sean Ekins, Alexander N. Freiberg, Anush Harutyunyan, Jason E. Comer, Kathleen O’Loughlin, Carol E. Green, Peter B. Madrid, and Mary A. Lingerfelt

Subjects

Male, 0301 basic medicine, Tilorone, Pharmacology, medicine.disease_cause, Antiviral Agents, Excretion, Mice, 03 medical and health sciences, Pharmacokinetics, Cell Line, Tumor, medicine, Animals, Humans, Distribution (pharmacology), Pharmacology (medical), Mice, Inbred BALB C, Interferon inducer, Ebola virus, Chemistry, Hemorrhagic Fever, Ebola, Ebolavirus, Virology, Bioavailability, 030104 developmental biology, Infectious Diseases, Toxicity, Microsomes, Liver, Female, Caco-2 Cells, medicine.drug

Abstract

Tilorone dihydrochloride (tilorone) is a small-molecule, orally bioavailable drug that is used clinically as an antiviral outside the United States. A machine-learning model trained on anti-Ebola virus (EBOV) screening data previously identified tilorone as a potent in vitro EBOV inhibitor, making it a candidate for the treatment of Ebola virus disease (EVD). In the present study, a series of in vitro ADMET (absorption, distribution, metabolism, excretion, toxicity) assays demonstrated the drug has excellent solubility, high Caco-2 permeability, was not a P-glycoprotein substrate, and had no inhibitory activity against five human CYP450 enzymes (3A4, 2D6, 2C19, 2C9, and 1A2). Tilorone was shown to have 52% human plasma protein binding with excellent plasma stability and a mouse liver microsome half-life of 48 min. Dose range-finding studies in mice demonstrated a maximum tolerated single dose of 100 mg/kg of body weight. A pharmacokinetics study in mice at 2- and 10-mg/kg dose levels showed that the drug is rapidly absorbed, has dose-dependent increases in maximum concentration of unbound drug in plasma and areas under the concentration-time curve, and has a half-life of approximately 18 h in both males and females, although the exposure was ∼2.5-fold higher in male mice. Tilorone doses of 25 and 50 mg/kg proved efficacious in protecting 90% of mice from a lethal challenge with mouse-adapted with once-daily intraperitoneal (i.p.) dosing for 8 days. A subsequent study showed that 30 mg/kg/day of tilorone given i.p. starting 2 or 24 h postchallenge and continuing through day 7 postinfection was fully protective, indicating promising activity for the treatment of EVD.

Published

2018

40. First vaccine approval under the FDA Animal Rule

Author

Jason E. Comer, Trevor Brasel, and David W.C. Beasley

Subjects

0301 basic medicine, Pharmacology, Licensure, medicine.medical_specialty, business.industry, 030106 microbiology, Immunology, MEDLINE, 3. Good health, Food and drug administration, 03 medical and health sciences, 030104 developmental biology, Infectious Diseases, Clinical research, Family medicine, Perspective, medicine, Pharmacology (medical), business

Abstract

The US Food and Drug Administration’s Animal Rule was established to facilitate licensure of new products for life-threatening conditions when traditional efficacy trials in humans are unethical or impractical. In November, 2015 BioThrax became the first vaccine to receive approval for a new indication via this pathway. The basis for this approval and use of Animal Rule or other non-traditional approval pathways for licensure of vaccines for serious conditions are discussed.

Published

2016

41. Development of an Inhalational Bacillus anthracis Exposure Therapeutic Model in Cynomolgus Macaques

Author

Lisa N. Henning, Gabriel T. Meister, Bryan D. Ray, Kevin P. Tordoff, Gregory V. Stark, Jason E. Comer, and Katherine A. B. Knostman

Subjects

Male, Microbiology (medical), medicine.medical_specialty, Time Factors, Bacterial Toxins, Clinical Biochemistry, Immunology, Anthrax, Antigen, Animals, Immunology and Allergy, Medicine, Blood culture, Respiratory Tract Infections, Antigens, Bacterial, biology, medicine.diagnostic_test, United States Food and Drug Administration, business.industry, Lethal dose, Primate Diseases, Antibodies, Monoclonal, Brain, biology.organism_classification, medicine.disease, Antibodies, Bacterial, Survival Analysis, United States, Bacillus anthracis, Disease Models, Animal, Macaca fascicularis, Bacteremia, Monoclonal, biology.protein, Clinical Immunology, Female, Histopathology, Guideline Adherence, Antibody, business, Biomarkers

Abstract

Appropriate animal models are required to test medical countermeasures to bioterrorist threats. To that end, we characterized a nonhuman primate (NHP) inhalational anthrax therapeutic model for use in testing anthrax therapeutic medical countermeasures according to the U.S. Food and Drug Administration Animal Rule. A clinical profile was recorded for each NHP exposed to a lethal dose ofBacillus anthracisAmes spores. Specific diagnostic parameters were detected relatively early in disease progression, i.e., by blood culture (∼37 h postchallenge) and the presence of circulating protective antigen (PA) detected by electrochemiluminescence (ECL) ∼38 h postchallenge, whereas nonspecific clinical signs of disease, i.e., changes in body temperature, hematologic parameters (ca. 52 to 66 h), and clinical observations, were delayed. To determine whether the presentation of antigenemia (PA in the blood) was an appropriate trigger for therapeutic intervention, a monoclonal antibody specific for PA was administered to 12 additional animals after the circulating levels of PA were detected by ECL. Seventy-five percent of the monoclonal antibody-treated animals survived compared to 17% of the untreated controls, suggesting that intervention at the onset of antigenemia is an appropriate treatment trigger for this model. Moreover, the onset of antigenemia correlated with bacteremia, and NHPs were treated in a therapeutic manner. Interestingly, brain lesions were observed by histopathology in the treated nonsurviving animals, whereas this observation was absent from 90% of the nonsurviving untreated animals. Our results support the use of the cynomolgus macaque as an appropriate therapeutic animal model for assessing the efficacy of medical countermeasures developed against anthrax when administered after a confirmation of infection.

Published

2012

42. Characterization of a Therapeutic Model of Inhalational Anthrax Using an Increase in Body Temperature in New Zealand White Rabbits as a Trigger for Treatment

Author

Lisa N. Henning, Jason M. Mott, Jason E. Comer, Gabriel T. Meister, Gregory V. Stark, Bryan D. Ray, and Roy E. Barnewall

Subjects

Male, Microbiology (medical), Time Factors, Fever, medicine.medical_treatment, Bacterial Toxins, Clinical Biochemistry, Immunology, Anthrax, medicine, Animals, Immunology and Allergy, New zealand white, Antigens, Bacterial, Blood Cells, biology, C-reactive protein, Antibodies, Monoclonal, Immunotherapy, biology.organism_classification, medicine.disease, Antibodies, Bacterial, Survival Analysis, Bacillus anthracis, Disease Models, Animal, C-Reactive Protein, Protective antigen, Bacteremia, Inhalational anthrax, biology.protein, Clinical Immunology, Female, Rabbits, Antibody, Biomarkers

Abstract

The development of an appropriate animal therapeutic model is essential to assess the potential efficacy of therapeutics for use in the event of a Bacillus anthracis exposure. We conducted a natural history study that showed New Zealand White rabbits exhibited a significant increase in body temperature (SIBT), changes in hematologic parameters, and increases in C-reactive protein and succumbed to disease with an average time to death of approximately 73 h following aerosol challenge with B. anthracis Ames spores. The SIBT was used as a trigger to treat with a fully human monoclonal antibody directed at protective antigen (PA). Ninety percent (9/10) of the treated rabbits survived the lethal inhalational challenge of B. anthracis . Further characterization investigated the protective window of opportunity for anti-PA antibody administration up to 12 h post-onset of SIBT. Eighty-three percent (5/6) of the rabbits treated at SIBT and 100% (6/6) of those treated at 6 h after SIBT survived challenge. Only 67% (4/6) of the rabbits treated at 12 h after SIBT survived. The increase in body temperature corresponded with both bacteremia and antigenemia (PA in the blood), indicating that SIBT is a suitable trigger to initiate treatment in a therapeutic model of inhalational anthrax.

Published

2012

43. Transcriptomic and Innate Immune Responses to Yersinia pestis in the Lymph Node during Bubonic Plague

Author

Dan Long, Rebecca Rosenke, Daniel E. Sturdevant, Jason E. Comer, Kimmo Virtaneva, B. Joseph Hinnebusch, Donald J. Gardner, Stephen F. Porcella, and Aaron B. Carmody

Subjects

Pneumonic plague, Bubo, Chemokine, Yersinia pestis, Immunology, Yersinia, Polymerase Chain Reaction, Microbiology, Bubonic plague, medicine, Animals, Lymph node, Oligonucleotide Array Sequence Analysis, Plague, Host Response and Inflammation, biology, Gene Expression Profiling, Flow Cytometry, medicine.disease, biology.organism_classification, Immunity, Innate, Rats, Infectious Diseases, medicine.anatomical_structure, Septicemic plague, biology.protein, Cytokines, Female, Parasitology, Lymph Nodes, Chemokines, medicine.symptom

Abstract

A delayed inflammatory response is a prominent feature of infection with Yersinia pestis , the agent of bubonic and pneumonic plague. Using a rat model of bubonic plague, we examined lymph node histopathology, transcriptome, and extracellular cytokine levels to broadly characterize the kinetics and extent of the host response to Y. pestis and how it is influenced by the Yersinia virulence plasmid (pYV). Remarkably, dissemination and multiplication of wild-type Y. pestis during the bubonic stage of disease did not induce any detectable gene expression or cytokine response by host lymph node cells in the developing bubo. Only after systemic spread had led to terminal septicemic plague was a transcriptomic response detected, which included upregulation of several cytokine, chemokine, and other immune response genes. Although an initial intracellular phase of Y. pestis infection has been postulated, a Th1-type cytokine response associated with classical activation of macrophages was not observed during the bubonic stage of disease. However, elevated levels of interleukin-17 (IL-17) were present in infected lymph nodes. In the absence of pYV, sustained recruitment to the lymph node of polymorphonuclear leukocytes (PMN, or neutrophils), the major IL-17 effector cells, correlated with clearance of infection. Thus, the ability to counteract a PMN response in the lymph node appears to be a major in vivo function of the Y. pestis virulence plasmid.

Published

2010

44. Human Monoclonal Antibody AVP-21D9 to Protective Antigen Reduces Dissemination of the Bacillus anthracis Ames Strain from the Lungs in a Rabbit Model

Author

Jagadish Sircar, Jennifer Pawlik, Laurie E. Sower, David M. Noffsinger, Lawrence R. Stanberry, Ashok K. Chopra, Bagram M. Chatuev, Scott T. Moen, Ritsuko Sawada, John A. Thomas, Autumn Wenglikowski, Kathryn Bush, Wallace B. Baze, Jason E. Comer, Kristin G. Walberg, Johnny W. Peterson, Wolfgang Scholz, Jason Hardcastle, and Joanna Taormina

Subjects

medicine.medical_specialty, Bacterial Toxins, Immunology, Biology, Microbiology, Anthrax, Ames strain, Antigen, Administration, Inhalation, medicine, Animals, Humans, Lung, Spores, Bacterial, Antigens, Bacterial, Inhalation, Antibodies, Monoclonal, biology.organism_classification, Virology, Bacillus anthracis, Disease Models, Animal, Infectious Diseases, medicine.anatomical_structure, Microbial Immunity and Vaccines, biology.protein, Parasitology, Histopathology, Rabbits, Lymph, Antibody

Abstract

Dutch-belted and New Zealand White rabbits were passively immunized with AVP-21D9, a human monoclonal antibody to protective antigen (PA), at the time of Bacillus anthracis spore challenge using either nasal instillation or aerosol challenge techniques. AVP-21D9 (10 mg/kg) completely protected both rabbit strains against lethal infection with Bacillus anthracis Ames spores, regardless of the inoculation method. Further, all but one of the passively immunized animals (23/24) were completely resistant to rechallenge with spores by either respiratory challenge method at 5 weeks after primary challenge. Analysis of the sera at 5 weeks after primary challenge showed that residual human anti-PA levels decreased by 85 to 95%, but low titers of rabbit-specific anti-PA titers were also measured. Both sources of anti-PA could have contributed to protection from rechallenge. In a subsequent study, bacteriological and histopathology analyses revealed that B. anthracis disseminated to the bloodstream in some naïve animals as early as 24 h postchallenge and increased in frequency with time. AVP-21D9 significantly reduced the dissemination of the bacteria to the bloodstream and to various organs following infection. Examination of tissue sections from infected control animals, stained with hematoxylin-eosin and the Gram stain, showed edema and/or hemorrhage in the lungs and the presence of bacteria in mediastinal lymph nodes, with necrosis and inflammation. Tissue sections from infected rabbits dosed with AVP-21D9 appeared comparable to corresponding tissues from uninfected animals despite lethal challenge with B. anthracis Ames spores. Concomitant treatment with AVP-21D9 at the time of challenge conferred complete protection in the rabbit inhalation anthrax model. Early treatment increased the efficacy progressively and in a dose-dependent manner. Thus, AVP-21D9 could offer an adjunct or alternative clinical treatment regimen against inhalation anthrax.

Published

2007

45. Murine macrophage transcriptional and functional responses to Bacillus anthracis edema toxin

Author

Katie L. Bush, Autumn Wenglikowski, Ashok K. Chopra, Jason E. Comer, Johnny W. Peterson, Cristi L. Galindo, Fan Zhang, and Harold R. Garner

Subjects

Transcription, Genetic, medicine.medical_treatment, Anthrax toxin, Bacterial Toxins, Polymerase Chain Reaction, Microbiology, Adenylyl cyclase, Mice, chemistry.chemical_compound, Cyclic AMP, medicine, Transcriptional regulation, Animals, Transcription factor, Antigens, Bacterial, Phagocytes, biology, Activator (genetics), CCAAT-Enhancer-Binding Protein-beta, Macrophages, Bacterial Infections, Microarray Analysis, biology.organism_classification, Molecular biology, Up-Regulation, Bacillus anthracis, Transcription Factor AP-1, Infectious Diseases, Cytokine, chemistry, Apoptosis, Cytokines, Transcription Factors

Abstract

Edema toxin (EdTx), which is a combination of edema factor and a binding moiety (protective antigen), is produced by Bacillus anthracis, the etiological agent of anthrax. EdTx is an adenylyl cyclase enzyme that converts adenosine triphosphate to adenosine-3′,5′-monophosphate, resulting in interstitial edema seen in anthrax patients. We used GeneChip analysis to examine global transcriptional profiles of EdTx-treated RAW 264.7 murine macrophage-like cells and identified 71 and 259 genes whose expression was significantly altered by the toxin at 3 and 6 h, respectively. Alteration in the expression levels of selected genes was confirmed by real time-reverse transcriptase polymerase chain reaction. The genes with up-regulated expression in macrophages in response to EdTx-treatment were known to be involved in inflammatory responses, regulation of apoptosis, adhesion, immune cell activation, and transcription regulation. Additionally, GeneChip analysis results implied that EdTx-induced activation of activator protein-1 (AP-1) and CAAAT/enhancer-binding protein-beta (C/EBP-β). Gel shift assays were therefore performed, and an increase in the activities of both of these transcription factors was observed within 30 min. EdTx also inhibited tumor necrosis factor alpha production and crippled the phagocytic ability of the macrophages. This is the first report detailing the host cell global transcriptional responses to EdTx.

Published

2006

46. GeneChip Analyses of Global Transcriptional Responses of Murine Macrophages to the Lethal Toxin ofBacillus anthracis

Author

Jason E. Comer, Johnny W. Peterson, Ashok K. Chopra, and Cristi L. Galindo

Subjects

Transcription, Genetic, Anthrax toxin, Bacterial Toxins, Immunology, Mitogen-activated protein kinase kinase, Microbiology, Mice, Gene expression, Animals, Protein kinase A, Gene, Oligonucleotide Array Sequence Analysis, Mitogen-Activated Protein Kinase Kinases, Regulation of gene expression, Antigens, Bacterial, Host Response and Inflammation, biology, Gene Expression Profiling, Macrophages, Proteins, biology.organism_classification, Molecular biology, Bacillus anthracis, Gene expression profiling, Infectious Diseases, Gene Expression Regulation, Parasitology

Abstract

We performed GeneChip analyses on RNA fromBacillus anthracislethal toxin (LeTx)-treated RAW 264.7 murine macrophages to investigate global effects of anthrax toxin on host cell gene expression. Stringent analysis of data revealed that the expression of several mitogen-activated protein kinase kinase-regulatory genes was affected within 1.5 h post-exposure to LeTx. By 3.0 h, the expression of 103 genes was altered, including those involved in intracellular signaling, energy production, and protein metabolism.

Published

2005

47. Identification of the Pseudomonas aeruginosa 1244 Pilin Glycosylation Site

Author

Jason E. Comer, Vincent J. Blanch, Carolyn D. Deal, Mark A. Marshall, and Peter Castric

Subjects

Glycan, Glycosylation, Molecular Sequence Data, Immunology, Biology, Microbiology, Pilus, Epitope, Serine, chemistry.chemical_compound, Humans, Amino Acid Sequence, Protein Precursors, Peptide sequence, Binding Sites, Membrane Proteins, Pili, Sex, biochemical phenomena, metabolism, and nutrition, Molecular Pathogenesis, Infectious Diseases, Epitope mapping, chemistry, Biochemistry, Pilin, Pseudomonas aeruginosa, biology.protein, Epitopes, B-Lymphocyte, bacteria, Parasitology, Fimbriae Proteins, Trisaccharides, Bacterial Outer Membrane Proteins

Abstract

Previous work (P. Castric, F. J. Cassels, and R. W. Carlson, J. Biol. Chem. 276:26479-26485, 2001) has shown the Pseudomonas aeruginosa 1244 pilin glycan to be covalently bound to a serine residue. N-terminal sequencing of pilin fragments produced from endopeptidase treatment and identified by reaction with a glycan-specific monoclonal antibody indicated that the glycan was present between residue 75 and the pilin carboxy terminus. Further sequencing of these peptides revealed that serine residues 75, 81, 84, 105, 106, and 108 were not modified. Conversion of serine 148, but not serine 118, to alanine by site-directed mutagenesis, resulted in loss of the ability to carry out pilin glycosylation when tested in an in vivo system. These results showed the pilin glycan to be attached to residue 148, the carboxy-terminal amino acid. The carboxy-proximal portion of the pilin disulfide loop, which is adjacent to the pilin glycan, was found to be a major linear B-cell epitope, as determined by peptide epitope mapping analysis. Immunization of mice with pure pili produced antibodies that recognized the pilin glycan. These sera also reacted with P. aeruginosa 1244 lipopolysaccharide as measured by Western blotting and enzyme-linked immunosorbent assay.

Published

2002

48. Combination therapy with antibiotics and anthrax immune globulin intravenous (AIGIV) is potentially more effective than antibiotics alone in rabbit model of inhalational anthrax

Author

Srinivas Kammanadiminti, Chris Sinclair, Ravi Kumar Patnaikuni, Gabriel T. Meister, Shantha Kodihalli, and Jason E. Comer

Subjects

Male, Bacterial Diseases, Antibiotics, lcsh:Medicine, Bacteremia, Levofloxacin, Pharmacology, Biochemistry, Zoonoses, Drug Discovery, Medicine and Health Sciences, lcsh:Science, Respiratory Tract Infections, Multidisciplinary, Immune System Proteins, biology, Immunoglobulins, Intravenous, Animal Models, Bacillus anthracis, Anti-Bacterial Agents, Treatment Outcome, Infectious Diseases, Veterinary Diseases, Drug Therapy, Combination, Female, Rabbits, medicine.drug, Research Article, Drug Research and Development, Combination therapy, Infectious Disease Control, medicine.drug_class, Toxemia, Immunology, Placebo, Research and Analysis Methods, Microbiology, Antibodies, Anthrax, Model Organisms, medicine, Animals, Survival rate, Antigens, Bacterial, business.industry, Lethal dose, lcsh:R, Biology and Life Sciences, Proteins, biology.organism_classification, medicine.disease, bacterial infections and mycoses, Disease Models, Animal, lcsh:Q, Clinical Immunology, Veterinary Science, business

Abstract

Background We have evaluated the therapeutic efficacy of AIGIV when given in combination with levofloxacin and the effective window of treatment to assess the added benefit provided by AIGIV over standard antibiotic treatment alone in a New Zealand white rabbit model of inhalational anthrax. Methods Rabbits were exposed to lethal dose of aerosolized spores of Bacillus anthracis (Ames strain) and treated intravenously with either placebo, (normal immune globulin intravenous, IGIV) or 15 U/kg of AIGIV, along with oral levofloxacin treatment at various time points (30–96 hours) after anthrax exposure. Results The majority of treated animals (>88%) survived in both treatment groups when treatment was initiated within 60 hours of post-exposure. However, reduced survival of 55%, 33% and 25% was observed for placebo + levofloxacin group when the treatment was initiated at 72, 84 and 96 hours post-exposure, respectively. Conversely, a survival rate of 65%, 40% and 71% was observed in the AIGIV + levofloxacin treated groups at these time points. Conclusions The combination of AIGIV with antibiotics provided an improvement in survival compared to levofloxacin treatment alone when treatment was delayed up to 96 hours post-anthrax exposure. Additionally, AIGIV treatment when given as an adjunct therapy at any of the time points tested did not interfere with the efficacy of levofloxacin.

Published

2013

49. Evaluation of Intravenous Anthrax Immune Globulin for Treatment of Inhalation Anthrax

Author

Cris Howard, Nancy F. Daczkowski, Gary S. Nabors, William Kramer, Daniel C. Sanford, Jason E. Comer, Nina V. Malkevich, Mohamed Al-Ibrahim, Ajoy C. Chakrabarti, Gabriel T. Meister, Robert J. Hopkins, Mario H. Skiadopoulos, Boris Ionin, Nutan Mytle, Kristopher E. Van Zandt, and Subhendu Basu

Subjects

Male, Time Factors, Bacterial Toxins, Anthrax Vaccines, Clinical Therapeutics, Anthrax, Pharmacokinetics, Double-Blind Method, Animals, Humans, Pharmacology (medical), Infusions, Intravenous, Respiratory Tract Infections, Pharmacology, Spores, Bacterial, Antigens, Bacterial, Anthrax vaccines, Inhalation, biology, Anthrax immune globulin, Vaccination, Anthrax Vaccine Adsorbed, Immunoglobulins, Intravenous, biology.organism_classification, Antibodies, Bacterial, Survival Analysis, Bacillus anthracis, Macaca fascicularis, Infectious Diseases, Tolerability, Immunology, Female, Rabbits, Biomarkers, Half-Life

Abstract

Bacillus anthracis toxins can be neutralized by antibodies against protective antigen (PA), a component of anthrax toxins. Anthrivig (human anthrax immunoglobulin), also known as AIGIV, derived from plasma of humans immunized with BioThrax (anthrax vaccine adsorbed), is under development for the treatment of toxemia following exposure to anthrax spores. The pharmacokinetics (PK) of AIGIV was assessed in naive animals and healthy human volunteers, and the efficacy of AIGIV was assessed in animals exposed via inhalation to aerosolized B. anthracis spores. In the clinical study, safety, tolerability, and PK were evaluated in three dose cohorts (3.5, 7.1, and 14.2 mg/kg of body weight of anti-PA IgG) with 30 volunteers per cohort. The elimination half-life of AIGIV in rabbits, nonhuman primates (NHPs), and humans following intravenous infusion was estimated to be approximately 4, 12, and 24 days, respectively, and dose proportionality was observed. In a time-based treatment study, AIGIV protected 89 to 100% of animals when administered 12 h postexposure; however, a lower survival rate of 39% was observed when animals were treated 24 h postexposure, underscoring the need for early intervention. In a separate set of studies, animals were treated on an individual basis upon detection of a clinical sign or biomarker of disease, namely, a significant increase in body temperature (SIBT) in rabbits and presence of PA in the serum of NHPs. In these trigger-based intervention studies, AIGIV induced up to 75% survival in rabbits depending on the dose and severity of toxemia at the time of treatment. In NHPs, up to 33% survival was observed in AIGIV-treated animals. (The clinical study has been registered at ClinicalTrials.gov under registration no. NCT00845650.)

Published

2013

50. Achieving consistent multiple daily low-dose Bacillus anthracis spore inhalation exposures in the rabbit model

Author

Tonya L. Nichols, Bradford W. Gutting, Sarah C. Taft, Alison E. Director-Myska, Roy E. Barnewall, Brian D. Miller, Jason E. Comer, and Daniel N. Wolfe

Subjects

Multiple exposure, Microbiology (medical), Spores, Aerosolize, Inhalation exposures, Immunology, Low-dose, lcsh:QR1-502, Pharmacology, Microbiology, lcsh:Microbiology, Toxicology, Anthrax, Animals, Subchronic exposures, Respiratory system, Aerosolization, Original Research, Inhalation exposure, Aerosols, Spores, Bacterial, Inhalation Exposure, biology, Inhalation, Chemistry, respiratory system, biology.organism_classification, Bacillus anthracis, Aerosol, Disease Models, Animal, Infectious Diseases, aerosol system, Rabbits

Abstract

Repeated low-level exposures to biological agents could occur before or after the remediation of an environmental release. This is especially true for persistent agents such as B. anthracis spores, the causative agent of anthrax. Studies were conducted to examine aerosol methods needed for consistent daily low aerosol concentrations to deliver a low-dose (less than 10(6) colony forming units (CFU) of B. anthracis spores) and included a pilot feasibility characterization study, acute exposure study, and a multiple 15 day exposure study. This manuscript focuses on the state-of-the-science aerosol methodologies used to generate and aerosolize consistent daily low aerosol concentrations and resultant low inhalation doses to rabbits. The pilot feasibility characterization study determined that the aerosol system was consistent and capable of producing very low aerosol concentrations. In the acute, single day exposure experiment, targeted inhaled doses of 1 × 10(2), 1 × 10(3), 1 × 10(4), and 1 × 10(5) CFU were used. In the multiple daily exposure experiment, rabbits were exposed multiple days to targeted inhaled doses of 1 × 10(2), 1 × 10(3), and 1 × 10(4) CFU. In all studies, targeted inhaled doses remained consistent from rabbit-to-rabbit and day-to-day. The aerosol system produced aerosolized spores within the optimal mass median aerodynamic diameter particle size range to reach deep lung alveoli. Consistency of the inhaled dose was aided by monitoring and recording respiratory parameters during the exposure with real-time plethysmography. Overall, the presented results show that the animal aerosol system was stable and highly reproducible between different studies and over multiple exposure days.

Published

2012