| Literature DB >> 32191641 |
Maike Kober-Hasslacher1,2, Hyunju Oh-Strauß1,3, Dilip Kumar2, Valeria Soberon1,3, Carina Diehl1,3, Maciej Lech4, Thomas Engleitner3,5,6, Eslam Katab3,7, Vanesa Fernández-Sáiz3,7, Guido Piontek8, Hongwei Li3,9, Björn Menze3,9, Christoph Ziegenhain10, Wolfgang Enard10, Roland Rad3,5,6, Jan P Böttcher11, Hans-Joachim Anders4, Martina Rudelius8, Marc Schmidt-Supprian1,2,3,5.
Abstract
Single-nucleotide polymorphisms and locus amplification link the NF-κB transcription factor c-Rel to human autoimmune diseases and B cell lymphomas, respectively. However, the functional consequences of enhanced c-Rel levels remain enigmatic. Here, we overexpressed c-Rel specifically in mouse B cells from BAC-transgenic gene loci and demonstrate that c-Rel protein levels linearly dictated expansion of germinal center B (GCB) cells and isotype-switched plasma cells. c-Rel expression in B cells of otherwise c-Rel-deficient mice fully rescued terminal B cell differentiation, underscoring its critical B cell-intrinsic roles. Unexpectedly, in GCB cells transcription-independent regulation produced the highest c-Rel protein levels among B cell subsets. In c-Rel-overexpressing GCB cells this caused enhanced nuclear translocation, a profoundly altered transcriptional program, and increased proliferation. Finally, we provide a link between c-Rel gain and autoimmunity by showing that c-Rel overexpression in B cells caused autoantibody production and renal immune complex deposition.Entities:
Keywords: Autoimmune diseases; Autoimmunity; B cells; Immunology; NF-kappaB
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Year: 2020 PMID: 32191641 PMCID: PMC7260018 DOI: 10.1172/JCI124382
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808