Your search keyword '"Kern Steven J"' showing total 4 results

1. Characterization and pathogenesis of aerosolized eastern equine encephalitis in the common marmoset (Callithrix jacchus).

Author

Porter AI, Erwin-Cohen RA, Twenhafel N, Chance T, Yee SB, Kern SJ, Norwood D, Hartman LJ, Parker MD, Glass PJ, and DaSilva L

Subjects

Animals, Blood Chemical Analysis, Brain pathology, Brain virology, Encephalomyelitis, Eastern Equine pathology, Encephalomyelitis, Eastern Equine physiopathology, Female, Immunity, Immunohistochemistry, Kidney virology, Lethal Dose 50, Liver virology, Lymph Nodes virology, Male, RNA, Viral analysis, RNA, Viral isolation & purification, Survival Analysis, Viral Load, Viral Plaque Assay, Aerosols, Callithrix virology, Disease Models, Animal, Encephalitis Virus, Eastern Equine pathogenicity, Encephalomyelitis, Eastern Equine veterinary, Encephalomyelitis, Eastern Equine virology

Abstract

Background: Licensed antiviral therapeutics and vaccines to protect against eastern equine encephalitis virus (EEEV) in humans currently do not exist. Animal models that faithfully recapitulate the clinical characteristics of human EEEV encephalitic disease, including fever, drowsiness, anorexia, and neurological signs such as seizures, are needed to satisfy requirements of the Food and Drug Administration (FDA) for clinical product licensing under the Animal Rule., Methods: In an effort to meet this requirement, we estimated the median lethal dose and described the pathogenesis of aerosolized EEEV in the common marmoset (Callithrix jacchus). Five marmosets were exposed to aerosolized EEEV FL93-939 in doses ranging from 2.4 × 10 1 PFU to 7.95 × 10 5 PFU., Results: The median lethal dose was estimated to be 2.05 × 10 2 PFU. Lethality was observed as early as day 4 post-exposure in the highest-dosed marmoset but animals at lower inhaled doses had a protracted disease course where humane study endpoint was not met until as late as day 19 post-exposure. Clinical signs were observed as early as 3 to 4 days post-exposure, including fever, ruffled fur, decreased grooming, and leukocytosis. Clinical signs increased in severity as disease progressed to include decreased body weight, subdued behavior, tremors, and lack of balance. Fever was observed as early as day 2-3 post-exposure in the highest dose groups and hypothermia was observed in several cases as animals became moribund. Infectious virus was found in several key tissues, including brain, liver, kidney, and several lymph nodes. Clinical hematology results included early neutrophilia, lymphopenia, and thrombocytopenia. Key pathological changes included meningoencephalitis and retinitis. Immunohistochemical staining for viral antigen was positive in the brain, retina, and lymph nodes. More intense and widespread IHC labeling occurred with increased aerosol dose., Conclusion: We have estimated the medial lethal dose of aerosolized EEEV and described the pathology of clinical disease in the marmoset model. The results demonstrate that the marmoset is an animal model suitable for emulation of human EEEV disease in the development of medical countermeasures.

Published

2017

2. Erratum to: Characterization and pathogenesis of aerosolized eastern equine encephalitis in the common marmoset (Callithrix jacchus)

Author

Porter, Aimee I., Erwin-Cohen, Rebecca A., Twenhafel, Nancy, Chance, Taylor, Yee, Steven B., Kern, Steven J., Norwood, David, Hartman, Laurie J., Parker, Michael D., Glass, Pamela J., and DaSilva, Luis

Subjects

Aerosols, Male, Immunity, Brain, Callithrix, Viral Plaque Assay, Encephalomyelitis, Eastern Equine, Viral Load, Kidney, Immunohistochemistry, Survival Analysis, Lethal Dose 50, Disease Models, Animal, Infectious Diseases, Liver, Virology, Animals, Encephalitis Virus, Eastern Equine, RNA, Viral, Female, Lymph Nodes, Erratum, Blood Chemical Analysis

Abstract

Licensed antiviral therapeutics and vaccines to protect against eastern equine encephalitis virus (EEEV) in humans currently do not exist. Animal models that faithfully recapitulate the clinical characteristics of human EEEV encephalitic disease, including fever, drowsiness, anorexia, and neurological signs such as seizures, are needed to satisfy requirements of the Food and Drug Administration (FDA) for clinical product licensing under the Animal Rule.In an effort to meet this requirement, we estimated the median lethal dose and described the pathogenesis of aerosolized EEEV in the common marmoset (Callithrix jacchus). Five marmosets were exposed to aerosolized EEEV FL93-939 in doses ranging from 2.4 × 10The median lethal dose was estimated to be 2.05 × 10We have estimated the medial lethal dose of aerosolized EEEV and described the pathology of clinical disease in the marmoset model. The results demonstrate that the marmoset is an animal model suitable for emulation of human EEEV disease in the development of medical countermeasures.

Published

2017

3. Disease progression in mice exposed to low-doses of aerosolized clinical isolates of Burkholderia pseudomallei.

Author

Trevino, Sylvia R., Klimko, Christopher P., Reed, Matthew C., Aponte-Cuadrado, Michael J., Hunter, Melissa, Shoe, Jennifer L., Meyer, Joshua R., Dankmeyer, Jennifer L., Biryukov, Sergei S., Quirk, Avery V., Fritts, Kristen A., Kern, Steven J., Fetterer, David P., Kohler, Lara J., Toothman, Ronald G., Bozue, Joel A., Schellhase, Christopher W., Kreiselmeier, Norman, Daye, Sharon P., and Welkos, Susan L.

Subjects

BURKHOLDERIA pseudomallei, MELIOIDOSIS, IMMUNE response, DISEASE progression, DATA analysis

Abstract

Mouse models have been essential to generate supporting data for the research of infectious diseases. Burkholderia pseudomallei, the etiological agent of melioidosis, has been studied using mouse models to investigate pathogenesis and efficacy of novel medical countermeasures to include both vaccines and therapeutics. Previous characterization of mouse models of melioidosis have demonstrated that BALB/c mice present with an acute infection, whereas C57BL/6 mice have shown a tendency to be more resistant to infection and may model chronic disease. In this study, either BALB/c or C57BL/6 mice were exposed to aerosolized human clinical isolates of B. pseudomallei. The bacterial strains included HBPUB10134a (virulent isolate from Thailand), MSHR5855 (virulent isolate from Australia), and 1106a (relatively attenuated isolate from Thailand). The LD50 values were calculated and serial sample collections were performed in order to examine the bacterial burdens in tissues, histopathological features of disease, and the immune response mounted by the mice after exposure to aerosolized B. pseudomallei. These data will be important when utilizing these models for testing novel medical countermeasures. Additionally, by comparing highly virulent strains with attenuated isolates, we hope to better understand the complex disease pathogenesis associated with this bacterium. [ABSTRACT FROM AUTHOR]

Published

2018

4. Comparison of three non-human primate aerosol models for glanders, caused by Burkholderia mallei.

Author

Waag, David M., Chance, Taylor B., Trevino, Sylvia R., Rossi, Franco D., Fetterer, David P., Amemiya, Kei, Dankmeyer, Jennifer L., Ingavale, Susham S., Tobery, Steven A., Zeng, Xiankun, Kern, Steven J., Worsham, Patricia L., Cote, Christopher K., and Welkos, Susan L.

Subjects

*DONKEYS, *BURKHOLDERIA, *CERCOPITHECUS aethiops, *FOOT & mouth disease, *PRIMATES, *RHESUS monkeys, *HUMORAL immunity, *AEROSOLS

Abstract

Burkholderia mallei is a gram-negative obligate animal pathogen that causes glanders, a highly contagious and potentially fatal disease of solipeds including horses, mules, and donkeys. Humans are also susceptible, and exposure can result in a wide range of clinical forms, i.e., subclinical infection, chronic forms with remission and exacerbation, or acute and potentially lethal septicemia and/or pneumonia. Due to intrinsic antibiotic resistance and the ability of the organisms to survive intracellularly, current treatment regimens are protracted and complicated; and no vaccine is available. As a consequence of these issues, and since B. mallei is infectious by the aerosol route, B. mallei is regarded as a major potential biothreat agent. To develop optimal medical countermeasures and diagnostic tests, well characterized animal models of human glanders are needed. The goal of this study was to perform a head-to-head comparison of models employing three commonly used nonhuman primate (NHP) species, the African green monkey (AGM), Rhesus macaque, and the Cynomolgus macaque. The natural history of infection and in vitro clinical, histopathological, immunochemical, and bacteriological parameters were examined. The AGMs were the most susceptible NHP to B. mallei ; five of six expired within 14 days. Although none of the Rhesus or Cynomolgus macaques succumbed, the Rhesus monkeys exhibited abnormal signs and clinical findings associated with B. mallei infection; and the latter may be useful for modeling chronic B. mallei infection. Based on the disease progression observations, gross and histochemical pathology, and humoral and cellular immune response findings, the AGM appears to be the optimal model of acute, lethal glanders infection. AGM models of infection by B. pseudomallei , the etiologic agent of melioidosis, have been characterized recently. Thus, the selection of the AGM species provides the research community with a single NHP model for investigations on acute, severe, inhalational melioidosis and glanders. • Burkholderia mallei is the bacterial pathogen of glanders, a contagious and potentially fatal disease of solipeds, and a major potential biothreat agent for humans. • To develop optimal medical countermeasures and diagnostic tests for glanders, well characterized animal models are needed. • The goal of this study was to simultaneously compare models employing three commonly used nonhuman primate species, Rhesus and Cynomolgus macaques, and the African Green monkey (AGM). • AGMs provided an optimal model of acute, lethal glanders; and the selection of this NHP affords researchers with a single NHP model for studies on severe inhalational disease by both of the pathogenic Burkholderia species, B. mallei (glanders) and B. pseudomallei (melioidosis). [ABSTRACT FROM AUTHOR]

Published

2021