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Lsc regulates marginal-zone B cell migration and adhesion and is required for the IgM T-dependent antibody response.

机译:Lsc调节边缘区B细胞迁移和粘附,是IgM T依赖抗体应答所必需的。

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The humoral immune response to protein antigens is composed of a rapid low-affinity IgM antibody response followed by an IgG response exhibiting higher affinity. Here, we demonstrate that Lsc, a protein that regulates G protein-coupled-receptor signaling and RhoA activation, is required by B lymphocytes for the antigen-specific IgM antibody response to a protein antigen. We further show that in lsc(-/-) mice, MZB cells are selectively affected such that naive and in vivo-activated MZB cells migrate toward sphingosine-1-phosphate at increased proportions but release inefficiently from integrin ligands. Consequently, lsc(-/-) MZB cells do not traffick appropriately in an immune response and do not contribute to the TD antibody response. These data demonstrate that Lsc regulates the migration and adhesion of MZB cells, and this regulation appears to be required for these cells to contribute to the antibody response to TD antigens.
机译:对蛋白质抗原的体液免疫反应由快速的低亲和力IgM抗体反应和随后表现出较高亲和力的IgG反应组成。在这里,我们证明B淋巴细胞需要Lsc(一种调节G蛋白偶联受体信号传导和RhoA激活的蛋白)才能对蛋白质抗原进行抗原特异性IgM抗体反应。我们进一步表明,在lsc(-/-)小鼠中,MZB细胞受到选择性影响,以至于幼稚的和体内激活的MZB细胞朝着鞘氨醇-1-磷酸迁移的比例增加,但从整联蛋白配体中释放效率低下。因此,Isc(-/-)MZB细胞不会在免疫应答中适当运输,并且不会促进TD抗体应答。这些数据表明,Lsc调节MZB细胞的迁移和粘附,并且这些调节似乎是这些细胞促进对TD抗原的抗体反应所必需的。

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