| Literature DB >> 28723548 |
Hong-Sheng Dai1, Nathaniel Griffin2, Chelsea Bolyard3, Hsiaoyin Charlene Mao2, Jianying Zhang4, Timothy P Cripe5, Tadahiro Suenaga6, Hisashi Arase6, Ichiro Nakano7, E A Chiocca8, Balveen Kaur3, Jianhua Yu2, Michael A Caligiuri9.
Abstract
Clearance of pathogens or tumor cells by antibodies traditionally requires both Fab and Fc domains of IgG. Here, we show the Fc domain of IgG alone mediates recognition and clearance of herpes simplex virus (HSV1)-infected cells. The human natural killer (NK) cell surface is naturally coated with IgG bound by its Fc domain to the Fcγ receptor CD16a. NK cells utilize the Fc domain of bound IgG to recognize gE, an HSV1-encoded glycoprotein that also binds the Fc domain of IgG but at a site distinct from CD16a. The bridge formed by the Fc domain between the HSV1-infected cell and the NK cell results in NK cell activation and lysis of the HSV1-infected cell in the absence of HSV1-specific antibody in vitro and prevents fatal HSV1 infection in vivo. This mechanism also explains how bacterial IgG-binding proteins regulate NK cell function and may be broadly applicable to Fcγ-receptor-bearing cells.Entities:
Keywords: ADCC; CD16a; DC-MEGE; FcBCC; HSV1; NK cells; gE; herpes virus; protein A; protein G
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Year: 2017 PMID: 28723548 PMCID: PMC5568648 DOI: 10.1016/j.immuni.2017.06.019
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745