| Literature DB >> 32868930 |
Natalie Burrows1,2, Rachael J M Bashford-Rogers3,4, Vijesh J Bhute5,3, Ana Peñalver5,3, John R Ferdinand6, Benjamin J Stewart6,7, Joscelin E G Smith5,3, Mukta Deobagkar-Lele8, Girolamo Giudice9, Thomas M Connor10, Akimichi Inaba6, Laura Bergamaschi3,11, Sam Smith5,3, Maxine G B Tran12,13, Evangelia Petsalaki9, Paul A Lyons3,11, Marion Espeli14, Brian J P Huntly15, Kenneth G C Smith3,11, Richard J Cornall4,8, Menna R Clatworthy6,7, Patrick H Maxwell5,3.
Abstract
B lymphocyte development and selection are central to adaptive immunity and self-tolerance. These processes require B cell receptor (BCR) signaling and occur in bone marrow, an environment with variable hypoxia, but whether hypoxia-inducible factor (HIF) is involved is unknown. We show that HIF activity is high in human and murine bone marrow pro-B and pre-B cells and decreases at the immature B cell stage. This stage-specific HIF suppression is required for normal B cell development because genetic activation of HIF-1α in murine B cells led to reduced repertoire diversity, decreased BCR editing and developmental arrest of immature B cells, resulting in reduced peripheral B cell numbers. HIF-1α activation lowered surface BCR, CD19 and B cell-activating factor receptor and increased expression of proapoptotic BIM. BIM deletion rescued the developmental block. Administration of a HIF activator in clinical use markedly reduced bone marrow and transitional B cells, which has therapeutic implications. Together, our work demonstrates that dynamic regulation of HIF-1α is essential for normal B cell development.Entities:
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Year: 2020 PMID: 32868930 PMCID: PMC7613233 DOI: 10.1038/s41590-020-0772-8
Source DB: PubMed Journal: Nat Immunol ISSN: 1529-2908 Impact factor: 31.250