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B淋巴细胞抗原受体的信号缺陷型突变体无法与Ig-α和Ig-β/γ结合。

Signaling-defective mutants of the B lymphocyte antigen receptor fail to associate with Ig-alpha and Ig-beta/gamma.

作者信息

Grupp S A, Campbell K, Mitchell R N, Cambier J C, Abbas A K

机构信息

Department of Pathology, Brigham and Women's Hospital, Boston, Massachusetts 02115.

出版信息

J Biol Chem. 1993 Dec 5;268(34):25776-9.

PMID:8245014
Abstract

The B cell receptor for antigen, the membrane immunoglobulin (mIg) molecule, is normally expressed in association with at least two other proteins, mb-1 (Ig-alpha) and B29 (Ig-beta/gamma). We have previously described a set of murine B cell clones transfected with wild-type and mutated forms of membrane-bound IgM (mIgM) that vary in their ability to transduce signals to the cell interior. Analysis of the B cell receptor complex in signaling and nonsignaling mutants of mIgM reveals complete concordance between intact signaling ability and ability of the mIgM to associate with Ig-alpha and Ig-beta/gamma. These results point to the importance of the mIgM transmembrane region in mediating binding to accessory molecules, and provide support for a role of Ig-alpha and Ig-beta/gamma that extends beyond surface expression to signal transduction in B lymphocytes.

摘要

抗原的B细胞受体,即膜免疫球蛋白(mIg)分子,通常与至少另外两种蛋白质,即mb-1(Ig-α)和B29(Ig-β/γ)一起表达。我们之前描述了一组转染了野生型和突变型膜结合IgM(mIgM)的鼠B细胞克隆,它们将信号转导至细胞内部的能力各不相同。对mIgM的信号转导和非信号转导突变体中的B细胞受体复合物进行分析发现,完整的信号转导能力与mIgM与Ig-α和Ig-β/γ结合的能力之间完全一致。这些结果表明mIgM跨膜区域在介导与辅助分子结合中的重要性,并为Ig-α和Ig-β/γ的作用提供了支持,其作用不仅限于表面表达,还延伸至B淋巴细胞中的信号转导。

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