关键词: B cell development B cell response B cell signaling antigen internalization antigen presentation cytoskeleton non-muscle myosin

Mesh : Animals Antibody Formation / immunology Antigens / metabolism B-Lymphocytes / cytology immunology Biomarkers / metabolism Bone Marrow Cells / cytology Cell Membrane / metabolism Cell Movement Cell Proliferation Cytokinesis Endocytosis Lymphocyte Activation / immunology Mice, Inbred C57BL Nonmuscle Myosin Type IIA / metabolism Peritoneum / cytology Receptors, Antigen, B-Cell / metabolism Solubility Spleen / cytology

来  源:   DOI:10.1016/j.celrep.2018.04.087   PDF(Pubmed)

Abstract:
B cell responses are regulated by antigen acquisition, processing, and presentation to helper T cells. These functions are thought to depend on contractile activity of non-muscle myosin IIa. Here, we show that B cell-specific deletion of the myosin IIa heavy chain reduced the numbers of bone marrow B cell precursors and splenic marginal zone, peritoneal B1b, and germinal center B cells. In addition, myosin IIa-deficient follicular B cells acquired an activated phenotype and were less efficient in chemokinesis and extraction of membrane-presented antigens. Moreover, myosin IIa was indispensable for cytokinesis. Consequently, mice with myosin IIa-deficient B cells harbored reduced serum immunoglobulin levels and did not mount robust antibody responses when immunized. Altogether, these data indicate that myosin IIa is a negative regulator of B cell activation but a positive regulator of antigen acquisition from antigen-presenting cells and that myosin IIa is essential for B cell development, proliferation, and antibody responses.
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