| Literature DB >> 33563755 |
Kathrin Kläsener1,2,3, Julia Jellusova1,2,3,4, Geoffroy Andrieux5,6, Ulrich Salzer7, Chiara Böhler1,2,3, Sebastian N Steiner8,9, Jonas B Albinus8,9, Marco Cavallari1,2,3, Beatrix Süß10, Reinhard E Voll7, Melanie Boerries5,6,11, Bernd Wollscheid8,9, Michael Reth12,2,3.
Abstract
CD20 is a B cell-specific membrane protein and represents an attractive target for therapeutic antibodies. Despite widespread usage of anti-CD20 antibodies for B cell depletion therapies, the biological function of their target remains unclear. Here, we demonstrate that CD20 controls the nanoscale organization of receptors on the surface of resting B lymphocytes. CRISPR/Cas9-mediated ablation of CD20 in resting B cells resulted in relocalization and interaction of the IgM-class B cell antigen receptor with the coreceptor CD19. This receptor rearrangement led to a transient activation of B cells, accompanied by the internalization of many B cell surface marker proteins. Reexpression of CD20 restored the expression of the B cell surface proteins and the resting state of Ramos B cells. Similarly, treatment of Ramos or naive human B cells with the anti-CD20 antibody rituximab induced nanoscale receptor rearrangements and transient B cell activation in vitro and in vivo. A departure from the resting B cell state followed by the loss of B cell identity of CD20-deficient Ramos B cells was accompanied by a PAX5 to BLIMP-1 transcriptional switch, metabolic reprogramming toward oxidative phosphorylation, and a shift toward plasma cell development. Thus, anti-CD20 engagement or the loss of CD20 disrupts membrane organization, profoundly altering the fate of human B cells.Entities:
Keywords: B lymphocyte; CD20; plasma cell; therapeutic antibody
Year: 2021 PMID: 33563755 PMCID: PMC7896350 DOI: 10.1073/pnas.2021342118
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205