Your search keyword '"Gene G. Olinger"' showing total 5 results

1. 3B11-N, a monoclonal antibody against MERS-CoV, reduces lung pathology in rhesus monkeys following intratracheal inoculation of MERS-CoV Jordan-n3/2012

Author

Ognian Bohorov, Lisa E. Hensley, Christopher Bartos, Gene G. Olinger, Michael R. Holbrook, Ralph S. Baric, Jeffrey Solomon, Joshua C. Johnson, Ulas Bagci, Jiusong Sun, Nicholas Oberlander, Daniel J. Mollura, Peter B. Jahrling, Larry Zeitlin, Xianchun Tang, Charles Goodman, Wayne A. Marasco, Louis Huzella, Natasha Bohorova, Kevin J. Whaley, James Pettitt, Reed F. Johnson, Michael H. Paulty, Quan Zhu, Britini L. Ork, Do H. Kim, Jing Qin, Lauren Keith, and Jesus Velasco

Subjects

0301 basic medicine, Male, Middle East respiratory syndrome coronavirus, medicine.drug_class, viruses, Disease, Biology, Lung pathology, medicine.disease_cause, Monoclonal antibody, Antibodies, Viral, Article, 03 medical and health sciences, Virology, Case fatality rate, medicine, Animals, Humans, Lung, Inoculation, Respiratory disease, virus diseases, Antibodies, Monoclonal, medicine.disease, Macaca mulatta, 3. Good health, respiratory tract diseases, Disease Models, Animal, 030104 developmental biology, Immunology, biology.protein, Middle East Respiratory Syndrome Coronavirus, Antibody, Coronavirus Infections

Abstract

Middle East Respiratory Syndrome Coronavirus (MERS-CoV) was identified in 2012 as the causative agent of a severe, lethal respiratory disease occurring across several countries in the Middle East. To date there have been over 1600 laboratory confirmed cases of MERS-CoV in 26 countries with a case fatality rate of 36%. Given the endemic region, it is possible that MERS-CoV could spread during the annual Hajj pilgrimage, necessitating countermeasure development. In this report, we describe the clinical and radiographic changes of rhesus monkeys following infection with 5×10(6) PFU MERS-CoV Jordan-n3/2012. Two groups of NHPs were treated with either a human anti-MERS monoclonal antibody 3B11-N or E410-N, an anti-HIV antibody. MERS-CoV Jordan-n3/2012 infection resulted in quantifiable changes by computed tomography, but limited other clinical signs of disease. 3B11-N treated subjects developed significantly reduced lung pathology when compared to infected, untreated subjects, indicating that this antibody may be a suitable MERS-CoV treatment.

Published

2016

2. Long-term sequelae after Ebola virus disease in Bundibugyo, Uganda: a retrospective cohort study

Author

Alison Taylor, Gene G. Olinger, Hannah Kibuuka, Michael A. Eller, Anna N. Honko, Salim Wakabi, Danielle V Clark, Merlin L. Robb, Lisa E. Hensley, Leigh Anne Eller, Luswa Lukwago, Matthew J. Hepburn, Nelson L. Michael, Monica Millard, and Randal J. Schoepp

Subjects

Adult, Male, Pediatrics, medicine.medical_specialty, viruses, Disease, medicine.disease_cause, Health outcomes, Disease Outbreaks, West africa, Cohort Studies, Young Adult, Humans, Medicine, Uganda, Survivors, Retrospective Studies, Ebola virus, business.industry, Outbreak, Retrospective cohort study, Hemorrhagic Fever, Ebola, Middle Aged, Ebolavirus, Infectious Diseases, Increased risk, Immunology, Female, Observational study, business

Abstract

The limited data available for long-term Ebola virus disease health outcomes suggest that sequelae persist for longer than 1 year after infection. The magnitude of the present outbreak in west Africa necessitates a more complete understanding of the health effects and future medical needs of these patients.We invited adult survivors of the 2007 Bundibugyo Ebola virus outbreak in Uganda and their contacts to take part in an observational study roughly 29 months after the outbreak. We collected information about health status, functional limitations, and demographics. We collected blood samples for clinical chemistry, haematology, and filovirus antibodies using ELISA. Analyses were restricted to probable and confirmed survivors and their seronegative contacts.We recruited 70 survivors of the 2007 Bundibugyo Ebola virus and 223 contacts. We did analyses for 49 probable and confirmed survivors and 157 seronegative contacts. Survivors of the Bundibugyo Ebola virus were at significantly increased risk of ocular deficits (retro-orbital pain [RR 4·3, 95% CI 1·9-9·6; p0·0001], blurred vision [1·9, 1·1-3·2; p=0·018]), hearing loss (2·3, 1·2-4·5; p=0·010), difficulty swallowing (2·1, 1·1-3·9; p=0·017), difficulty sleeping (1·9, 1·3-2·8; p=0·001), arthralgias (2·0, 1·1-3·6; p=0·020), and various constitutional symptoms controlling for age and sex. Chronic health problems (prevalence ratio [PR] 2·1, 95% CI 1·2-3·6; p=0·008) and limitations due to memory loss or confusion (PR 5·8, 1·5-22·4; p=0·010) were also reported more frequently by survivors of Bundibugyo Ebola virus.Long-term sequelae persist for more than 2 years after Ebola virus disease. Definition of health consequences related to Ebola virus disease could improve patient care for survivors and contribute to understanding of disease pathogenesis.Chemical Biological Technologies Directorate, Defense Threat Reduction Agency.

Published

2015

3. Post-exposure therapy of filovirus infections

Author

Gary P. Kobinger, Xiangguo Qiu, Gary Wong, and Gene G. Olinger

Subjects

Primates, Microbiology (medical), Time Factors, Post exposure, medicine.medical_treatment, Virulence, Severe disease, BCX4430, Disease, Biology, Antibodies, Viral, Antiviral Agents, Microbiology, Virology, Filoviridae Infections, medicine, Animals, Biological Products, Nucleoside analogue, General symptoms, Antibodies, Monoclonal, Immunotherapy, Disease Models, Animal, Treatment Outcome, Infectious Diseases, Immunology, Post-Exposure Prophylaxis, medicine.drug

Abstract

Filovirus infections cause fatal hemorrhagic fever characterized by the initial onset of general symptoms before rapid progression to severe disease; the most virulent species can cause death to susceptible hosts within 10 days after the appearance of symptoms. Before the advent of monoclonal antibody (mAb) therapy, infection of nonhuman primates (NHPs) with the most virulent filovirus species was fatal if interventions were not administered within minutes. A novel nucleoside analogue, BCX4430, has since been shown to also demonstrate protective efficacy with a delayed treatment start. This review summarizes and evaluates the potential of current experimental candidates for treating filovirus disease with regard to their feasibility and use in the clinic, and assesses the most promising strategies towards the future development of a pan-filovirus medical countermeasure.

Published

2014

4. Pyridinyl imidazole inhibitors of p38 MAP kinase impair viral entry and reduce cytokine induction by Zaire ebolavirus in human dendritic cells

Author

Joshua C. Johnson, Lisa E. Hensley, Osvaldo Martinez, Gene G. Olinger, Anna N. Honko, and Christopher F. Basler

Subjects

MAPK/ERK pathway, medicine.medical_treatment, Biology, medicine.disease_cause, p38 Mitogen-Activated Protein Kinases, Article, Inhibitory Concentration 50, Viral entry, Virology, medicine, Humans, Enzyme Inhibitors, Antigen-presenting cell, Cells, Cultured, Pharmacology, Ebolavirus, Ebola virus, Imidazoles, Dendritic Cells, Dendritic cell, Virus Internalization, Cell biology, Cytokine, Viral replication, Cytokines

Abstract

Antigen presenting cells (APCs), including macrophages and dendritic cells, are early and sustained targets of Ebola virus (EBOV) infection in vivo. Because EBOV activates mitogen-activated protein kinase (MAPK) signaling upon infection of APCs, we evaluated the effect of pyridinyl imidazole inhibitors of p38 MAPK on EBOV infection of human APCs and EBOV mediated cytokine production from human DCs. The p38 MAPK inhibitors reduced viral replication in PMA-differentiated macrophage-like human THP-1 cells with an IC50 of 4.73 μM (SB202190), 8.26 μM (p38kinhIII) and 8.21 μM (SB203580) and primary human monocyte-derived dendritic cells (MDDCs) with an IC50 of 2.67 μM (SB202190). Furthermore, cytokine production from EBOV-treated MDDCs was inhibited in a dose-dependent manner. A control pyridinyl imidazole compound failed to inhibit either EBOV infection or cytokine induction. Using an established EBOV virus-like particle (VLP) entry assay, we demonstrate that inhibitor pretreatment blocked VLP entry suggesting that the inhibitors blocked infection and replication at least in part by blocking EBOV entry. Taken together, our results indicate that pyridinyl imidazole p38 MAPK inhibitors may serve as leads for the development of therapeutics to treat EBOV infection.

Published

2014

5. Control of Ebola virus infection in mice with recombinant human mannose-binding lectin: Requirement for C3

Author

Gregory T. Spear, Ian C. Michelow, Emmett V. Schmidt, Kazue Takahashi, Gene G. Olinger, Xin Ji, and Louis M. Yantosca

Subjects

Recombinant human mannose-binding lectin, Immunology, Biology, Molecular Biology, Ebola virus infection, Virology

Published

2008