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Suppression of Fc-gamma-Receptor-Mediated Antibody Effector Function during Persistent Viral Infection

Posted on:2016-05-12Degree:Ph.DType:Dissertation
University:University of California, Los AngelesCandidate:Yamada, DouglasFull Text:PDF
GTID:1474390017983974Subject:Immunology
Abstract/Summary:
Understanding how viruses subvert host immunity and persist is essential for developing strategies to eliminate infection. T cell exhaustion during chronic viral infection is well described, but effects on antibody-mediated effector activity are unclear. Herein, we show that increased amounts of immune complexes generated in mice persistently infected with lymphocytic choriomeningitis virus (LCMV) suppressed multiple Fcgamma-Receptor (FcgammaR) functions. The high amounts of immune complexes suppressed antibody-mediated cell depletion, therapeutic antibody-killing of LCMV infected cells and human CD20-expressing tumors, as well as reduced immune complex-mediated cross-presentation to T cells. Suppression of FcgammaR activity was not due to inhibitory FcgammaRs or high concentrations of free antibody, and proper FcgammaR functions were restored when persistently infected mice specifically lacked immune complexes. Thus, we identify a mechanism of immunosuppression during viral persistence with implications for understanding effective antibody activity aimed at pathogen control.
Keywords/Search Tags:Antibody, Viral
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