Author:
Peart Akindele Nadine A.,Katamoni Laharika Dasharath,Brockhurst Jacqueline,Ghimire Shristi,Suwanmanee San,Pieterse Lisa,Metcalf Pate Kelly A.,Bunyan Elaine,Bannister Roy,Cihlar Tomas,Porter Danielle P.,Griffin Diane E.
Abstract
AbstractMeasles is a systemic disease initiated in the respiratory tract with widespread measles virus (MeV) infection of lymphoid tissue. Mortality can be substantial, but no licensed antiviral therapy is available. We evaluated both post-exposure prophylaxis and treatment with remdesivir, a broad-spectrum antiviral, using a well-characterized rhesus macaque model of measles. Animals were treated with intravenous remdesivir for 12 days beginning either 3 days after intratracheal infection (post-exposure prophylaxis, PEP) or 11 days after infection at the onset of disease (late treatment, LT). As PEP, remdesivir lowered levels of viral RNA in peripheral blood mononuclear cells, but RNA rebounded at the end of the treatment period and infectious virus was continuously recoverable. MeV RNA was cleared more rapidly from lymphoid tissue, was variably detected in the respiratory tract, and not detected in urine. PEP did not improve clinical disease nor lymphopenia and reduced the antibody response to infection. In contrast, LT had little effect on levels of viral RNA or the antibody response but also did not decrease clinical disease. Therefore, remdesivir transiently suppressed expression of viral RNA and limited dissemination when provided as PEP, but virus was not cleared and resumed replication without improvement in the clinical disease parameters evaluated.
Funder
National Institutes of Health
Bauernschmidt Committee of Johns Hopkins School of Medicine
Chulabhorn Royal Academy
Gilead Sciences
Publisher
Springer Science and Business Media LLC
Cited by
3 articles.
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