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通过B细胞抗原受体的Ig-α和Ig-β组分的差异信号传导。

Differential signaling through the Ig-alpha and Ig-beta components of the B cell antigen receptor.

作者信息

Kim K M, Alber G, Weiser P, Reth M

机构信息

Max-Planck Institut für Immunbiologie, Freiburg, FRG.

出版信息

Eur J Immunol. 1993 Apr;23(4):911-6. doi: 10.1002/eji.1830230422.

Abstract

The B cell antigen receptor is a complex containing the antigen-binding immunoglobulin molecules and the Ig-alpha/Ig-beta heterodimer which presumably connects the B cell antigen receptor to intracellular signaling components. To analyze the functional properties of the cytoplasmic parts of the B cell antigen receptor, we used the K46 B lymphoma line (IgG2a, kappa) to express chimeric molecules composed of the extracellular and transmembrane part of the CD8 alpha molecule and the cytoplasmic sequence of either the Ig-alpha (CD8 alpha/Ig-alpha), the Ig-beta (CD8 alpha/Ig-beta) protein or the membrane-bound gamma 2a heavy chain (CD8 alpha/gamma 2a). From these three types of chimeric molecules only (CD8 alpha/Ig-alpha and CD8 alpha/Ig-beta, but not CD8 alpha/gamma 2a, could transduce signals, thus providing the first evidence that the cytoplasmic tail of Ig-alpha and Ig-beta have a signaling capacity. After cross-linking with anti-CD8 alpha antibodies, both molecules induced a similar increase in intracellular free calcium ion and in MAP kinase phosphorylation. Protein tyrosine kinases, however, were strongly activated via the CD8 alpha/Ig-alpha and only marginally via the CD8 alpha/Ig-beta molecule. This suggests that the Ig-alpha and Ig-beta proteins have distinct roles during signal transduction through the B cell antigen receptor.

摘要

B细胞抗原受体是一种复合物,包含抗原结合免疫球蛋白分子和Ig-α/Ig-β异二聚体,后者可能将B细胞抗原受体与细胞内信号传导成分相连。为了分析B细胞抗原受体胞质部分的功能特性,我们利用K46 B淋巴瘤细胞系(IgG2a,κ)表达由CD8α分子的胞外和跨膜部分以及Ig-α(CD8α/Ig-α)、Ig-β(CD8α/Ig-β)蛋白或膜结合γ2a重链(CD8α/γ2a)的胞质序列组成的嵌合分子。从这三种类型的嵌合分子中,只有(CD8α/Ig-α和CD8α/Ig-β,而不是CD8α/γ2a)能够转导信号,从而首次证明Ig-α和Ig-β的胞质尾巴具有信号传导能力。用抗CD8α抗体交联后,这两种分子均诱导细胞内游离钙离子和MAP激酶磷酸化出现类似程度的增加。然而,蛋白酪氨酸激酶通过CD8α/Ig-α被强烈激活,而通过CD8α/Ig-β分子仅被微弱激活。这表明Ig-α和Ig-β蛋白在通过B细胞抗原受体的信号转导过程中具有不同的作用。

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