| Literature DB >> 34762046 |
Michael Jonathan Lehrke1, Michael Jeremy Shapiro1, Matthew J Rajcula1, Madeleine M Kennedy1, Shaylene A McCue1, Kay L Medina1, Virginia Smith Shapiro1.
Abstract
Iron-sulfur (Fe-S) clusters are cofactors essential for the activity of numerous enzymes including DNA polymerases, helicases, and glycosylases. They are synthesized in the mitochondria as Fe-S intermediates and are exported to the cytoplasm for maturation by the mitochondrial transporter ABCB7. Here, we demonstrate that ABCB7 is required for bone marrow B cell development, proliferation, and class switch recombination, but is dispensable for peripheral B cell homeostasis in mice. Conditional deletion of ABCB7 using Mb1-cre resulted in a severe block in bone marrow B cell development at the pro-B cell stage. The loss of ABCB7 did not alter expression of transcription factors required for B cell specification or commitment. While increased intracellular iron was observed in ABCB7-deficient pro-B cells, this did not lead to increased cellular or mitochondrial reactive oxygen species, ferroptosis, or apoptosis. Interestingly, loss of ABCB7 led to replication-induced DNA damage in pro-B cells, independent of VDJ recombination, and these cells had evidence of slowed DNA replication. Stimulated ABCB7-deficient splenic B cells from CD23-cre mice also had a striking loss of proliferation and a defect in class switching. Thus, ABCB7 is essential for early B cell development, proliferation, and class switch recombination.Entities:
Keywords: ABCB7; B cells; immunology; inflammation; iron; mouse
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Year: 2021 PMID: 34762046 PMCID: PMC8585479 DOI: 10.7554/eLife.69621
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140