Human FcγRIIIa activation on splenic macrophages drives the in vivo pathogenesis of dengue disease [article]

Rachel Yamin, Kevin S. Kao, Margaret R. MacDonald, Tineke Cantaert, Charles M. Rice, Jeffrey V. Ravetch, Stylianos Bournazos
2022 bioRxiv   pre-print
AbstractAlthough dengue virus (DENV) infection typically causes asymptomatic disease, DENV-infected patients can experience severe complications. A risk factor for symptomatic disease is pre-existing anti-DENV IgG antibodies. Cellular assays suggested that these antibodies can enhance viral infection of Fcγ receptor (FcγR)-expressing myeloid cells. Recent studies, however, revealed more complex interactions between anti-DENV antibodies and specific FcγRs by demonstrating that modulation of the
more » ... gG Fc glycan correlates with disease severity. To investigate thein vivomechanisms of antibody-mediated dengue pathogenesis, we developed a mouse model for dengue disease that recapitulates the unique complexity of human FcγRs. Our studies reveal that thein vivopathogenic activity of anti-DENV IgG antibodies is exclusively mediated through engagement of FcγRIIIa expressed on splenic macrophages, resulting in inflammatory sequelae and mortality. These findings highlight the importance of IgG-FcγRIIIa interactions in dengue disease, with important implications in the design of safer vaccination approaches and effective therapeutic strategies.
doi:10.1101/2022.11.02.514909 fatcat:cgwy4e7ztzfltfefkcts3n35gu