Fc Receptor-Like 6 (FCRL6) Discloses Progenitor B Cell Heterogeneity That Correlates With Pre-BCR Dependent and Independent Pathways of Natural Antibody Selection
Author(s) -
Kazuhito Honjo,
Woong-Jai Won,
R. Glenn King,
Lara Ianov,
David K. Crossman,
Juliet Easlick,
Mikhail A. Shakhmatov,
Mohamed Khass,
André M. Vale,
Robert P. Stephan,
Ran Li,
Randall S. Davis
Publication year - 2020
Publication title -
frontiers in immunology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.646
H-Index - 124
ISSN - 1664-3224
DOI - 10.3389/fimmu.2020.00082
Subject(s) - biology , breakpoint cluster region , b cell receptor , progenitor cell , negative selection , clonal selection , b cell , microbiology and biotechnology , receptor , antibody , immunology , stem cell , genetics , gene , genome
B-1a cells produce “natural” antibodies (Abs) to neutralize pathogens and clear neo self-antigens, but the fundamental selection mechanisms that shape their polyreactive repertoires are poorly understood. Here, we identified a B cell progenitor subset defined by Fc receptor-like 6 (FCRL6) expression, harboring innate-like defense, migration, and differentiation properties conducive for natural Ab generation. Compared to FCRL6 − pro B cells, the repressed mitotic, DNA damage repair, and signaling activity of FCRL6 + progenitors, yielded V H repertoires with biased distal Ighv segment accessibility, constrained diversity, and hydrophobic and charged CDR-H3 sequences. Beyond nascent autoreactivity, V H 11 productivity, which predominates phosphatidylcholine-specific B-1a B cell receptors (BCRs), was higher for FCRL6 + cells as was pre-BCR formation, which was required for Myc induction and V H 11, but not V H 12, B-1a development. Thus, FCRL6 revealed unexpected heterogeneity in the developmental origins, regulation, and selection of natural Abs at the pre-BCR checkpoint with implications for autoimmunity and lymphoproliferative disorders.
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