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配体诱导的膜IgM与B细胞细胞骨架基质的结合不是通过Igαβ异二聚体介导的。

The ligand-induced membrane IgM association with the cytoskeletal matrix of B cells is not mediated through the Ig alpha beta heterodimer.

作者信息

Hartwig J H, Jugloff L S, De Groot N J, Grupp S A, Jongstra-Bilen J

机构信息

Department of Immunology, University of Toronto, Ontario, Canada.

出版信息

J Immunol. 1995 Oct 15;155(8):3769-79.

PMID:7561081
Abstract

The B cell Ag receptor complex consists of membrane-associated Ig (mIg), Ig alpha, and Ig beta, associated molecules that have been implicated in transducing the activation signal that occurs upon receptor cross-linking. The role of the Ig alpha beta heterodimer in mediating binding to the cytoskeleton is unknown. We studied the ligand-induced association of mIgM with the cytoskeleton following receptor cross-linking in mIgM-expressing B lymphoma lines by biochemical assays, FACS analysis, and electron microscopy. Cytoskeletal association is not detected in unstimulated cells, but occurs rapidly upon anti-IgM-mediated cross-linking. Ig alpha is absent from the cytoskeleton-mIgM complex. To further analyze the possible role of Ig alpha beta in cytoskeletal binding, a surface Ig alpha beta-negative plasmacytoma line was transfected with a mutant form of mIgM (IgM-MutA). IgM-MutA is expressed on the surface despite the lack of Ig alpha beta, and the cytoskeletal binding occurred to a similar extent as in Ig-alpha-positive cell lines. In another transfectant expressing a mutated form of human mIgM (YS:VV), which does not have the capacity to bind to Ig alpha beta, the association of the receptor with the cytoskeleton appeared to be more extensive (100%) and faster than with mouse mIgM. These data indicate that Ig-associated Ig alpha beta proteins are not required for mIgM association with the cytoskeleton.

摘要

B细胞抗原受体复合物由膜相关免疫球蛋白(mIg)、免疫球蛋白α(Igα)和免疫球蛋白β(Igβ)组成,这些相关分子参与转导受体交联时发生的激活信号。Igαβ异二聚体在介导与细胞骨架结合中的作用尚不清楚。我们通过生化分析、荧光激活细胞分选(FACS)分析和电子显微镜,研究了在表达mIgM的B淋巴瘤细胞系中受体交联后,配体诱导的mIgM与细胞骨架的结合。在未刺激的细胞中未检测到细胞骨架结合,但在抗IgM介导的交联后迅速发生。细胞骨架-mIgM复合物中不存在Igα。为了进一步分析Igαβ在细胞骨架结合中的可能作用,用mIgM的突变形式(IgM-MutA)转染了一种表面Igαβ阴性的浆细胞瘤细胞系。尽管缺乏Igαβ,IgM-MutA仍在表面表达,并且细胞骨架结合的程度与Igα阳性细胞系相似。在另一种表达人mIgM突变形式(YS:VV)的转染细胞中,该突变形式不具备与Igαβ结合的能力,受体与细胞骨架的结合似乎更广泛(100%)且比与小鼠mIgM的结合更快。这些数据表明,mIgM与细胞骨架的结合不需要Ig相关的Igαβ蛋白。

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