Direct Infection of B Cells by Dengue Virus Modulates B Cell Responses in a Cambodian Pediatric Cohort

Dengue is an acute viral disease caused by dengue virus (DENV), which is transmitted by mosquitoes. Symptoms of DENV infection range from inapparent to severe and can be life-threatening. DENV replicates in primary immune cells such as dendritic cells and macrophages, which contribute to the dissemi...

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Veröffentlicht in:Frontiers in immunology 2021-02, Vol.11, p.594813-594813
Hauptverfasser: Upasani, Vinit, Vo, Hoa Thi My, Auerswald, Heidi, Laurent, Denis, Heng, Sothy, Duong, Veasna, Rodenhuis-Zybert, Izabela A, Dussart, Philippe, Cantaert, Tineke
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Sprache:eng
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Zusammenfassung:Dengue is an acute viral disease caused by dengue virus (DENV), which is transmitted by mosquitoes. Symptoms of DENV infection range from inapparent to severe and can be life-threatening. DENV replicates in primary immune cells such as dendritic cells and macrophages, which contribute to the dissemination of the virus. Susceptibility of other immune cells such as B cells to direct infection by DENV and their subsequent response to infection is not well defined. In a cohort of 60 Cambodian children, we showed that B cells are susceptible to DENV infection. Moreover, we show that B cells can support viral replication of laboratory adapted and patient-derived DENV strains. B cells were permissive to DENV infection albeit low titers of infectious virions were released in cell supernatants CD300a, a phosphatidylserine receptor, was identified as a potential attachment factor or receptor for entry of DENV into B cells. In spite of expressing Fc -receptors, antibody-mediated enhancement of DENV infection was not observed in B cells in an model. Direct infection by DENV induced proliferation of B cells in dengue patients and plasmablast/plasma cell formation . To summarize, our results show that B cells are susceptible to direct infection by DENV CD300a and the subsequent B cell responses could contribute to dengue pathogenesis.
ISSN:1664-3224
1664-3224
DOI:10.3389/fimmu.2020.594813