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Endophilin A2 regulates B‐cell endocytosis and is required for germinal center and humoral responses
Authors:Dessislava Malinova,Laabiah Wasim,Rebecca Newman,Ana Martí  nez‐  Riañ  o,Niklas Engels,Pavel Tolar
Affiliation:1. Immune Receptor Activation Laboratory, The Francis Crick Institute, London UK ; 2. Wellcome‐Wolfson Institute for Experimental Medicine, Queen''s University Belfast, Belfast UK ; 3. Institute of Cellular & Molecular Immunology, University Medical Center Göttingen, Göttingen Germany ; 4. Institute of Immunity and Transplantation, University College London, London UK
Abstract:Antigen‐specific B‐cell responses require endosomal trafficking to regulate antigen uptake and presentation to helper T cells, and to control expression and signaling of immune receptors. However, the molecular composition of B‐cell endosomal trafficking pathways and their specific roles in B‐cell responses have not been systematically investigated. Here, we report high‐throughput identification of genes regulating B‐cell receptor (BCR)‐mediated antigen internalization using genome‐wide functional screens. We show that antigen internalization depends both on constitutive, clathrin‐mediated endocytosis and on antigen‐induced, clathrin‐independent endocytosis mediated by endophilin A2. Although endophilin A2‐mediated endocytosis is dispensable for antigen presentation, it is selectively required for metabolic support of B‐cell proliferation, in part through regulation of iron uptake. Consequently, endophilin A2‐deficient mice show defects in GC B‐cell responses and production of high‐affinity IgG. The requirement for endophilin A2 highlights a unique importance of clathrin‐independent intracellular trafficking in GC B‐cell clonal expansion and antibody responses.
Keywords:antigen uptake, B‐  cell responses, endocytosis, endophilin A2, germinal center
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