A follicular regulatory Innate Lymphoid Cell population impairs interactions between germinal center Tfh and B cells

滤泡调节性固有淋巴细胞群会损害生发中心 Tfh 细胞和 B 细胞之间的相互作用。

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作者:Margaret H O'Connor ,Roshell Muir ,Marita Chakhtoura ,Michael Fang ,Eirini Moysi ,Susan Moir ,Alison J Carey ,Alyssa Terk ,Carmen N Nichols ,Talibah Metcalf ,Constantinos Petrovas ,Mark J Cameron ,Virginie Tardif ,Elias K Haddad

Abstract

Innate Lymphoid Cells (ILCs) are immune cells typically found on mucosal surfaces and in secondary lymphoid organs where they regulate the immune response to pathogens. Despite their key role in the immune response, there are still fundamental gaps in our understanding of ILCs. Here we report a human ILC population present in the follicles of tonsils and lymph nodes termed follicular regulatory ILCs (ILCFR) that to our knowledge has not been previously identified. ILCFR have a distinct phenotype and transcriptional program when compared to other defined ILCs. Surprisingly, ILCFR inhibit the ability of follicular helper T (Tfh) cells to provide B cell help. The localization of ILCFR to the germinal centers suggests these cells may interfere with germinal center B cell (GC-B) and germinal center Tfh cell (GC-Tfh) interactions through the production of transforming growth factor beta (TGF-β. Intriguingly, under conditions of impaired GC-Tfh-GC-B cell interactions, such as human immunodeficiency virus (HIV) infection, the frequency of these cells is increased. Overall, we predict a role for ILCFR in regulating GC-Tfh-GC-B cell interactions and propose they expand in chronic inflammatory conditions.

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