Antibody Prophylaxis and Therapy against West NileVirus Infection in Wild-Type and ImmunodeficientMice

MJ Engle, MS Diamond - Journal of virology, 2003 - Am Soc Microbiol
MJ Engle, MS Diamond
Journal of virology, 2003Am Soc Microbiol
West Nile virus (WNV) is a mosquito-borne Flavivirus that causes encephalitis in a subset of
susceptible humans. Current treatment for WNV infections is supportive, and no specific
therapy or vaccine is available. In this study, we directly tested the prophylactic and
therapeutic efficacy of polyclonal antibodies against WNV. Passive administration of human
gamma globulin or mouse serum prior to WNV infection protected congenic wild-type, B-cell-
deficient (μMT), and T-and B-cell-deficient (RAG1) C57BL/6J mice. Notably, no increased …
Abstract
West Nile virus (WNV) is a mosquito-borne Flavivirus that causes encephalitis in a subset of susceptible humans. Current treatment for WNV infections is supportive, and no specific therapy or vaccine is available. In this study, we directly tested the prophylactic and therapeutic efficacy of polyclonal antibodies against WNV. Passive administration of human gamma globulin or mouse serum prior to WNV infection protected congenic wild-type, B-cell-deficient (μMT), and T- and B-cell-deficient (RAG1) C57BL/6J mice. Notably, no increased mortality due to immune enhancement was observed. Although immune antibody completely prevented morbidity and mortality in wild-type mice, its effect was not durable in immunocompromised mice: many μMT and RAG1 mice eventually succumbed to infection. Thus, antibody by itself did not completely eliminate viral reservoirs in host tissues, consistent with an intact cellular immune response being required for viral clearance. In therapeutic postexposure studies, human gamma globulin partially protected against WNV-induced mortality. In μMT mice, therapy had to be initiated within 2 days of infection to gain a survival benefit, whereas in the wild-type mice, therapy even 5 days after infection reduced mortality. This time point is significant because between days 4 and 5, WNV was detected in the brains of infected mice. Thus, passive transfer of immune antibody improves clinical outcome even after WNV has disseminated into the central nervous system.
American Society for Microbiology