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小鼠bcl-x在B淋巴细胞和T淋巴细胞中的克隆及分子特征分析

Cloning and molecular characterization of mouse bcl-x in B and T lymphocytes.

作者信息

Fang W, Rivard J J, Mueller D L, Behrens T W

机构信息

Department of Medicine/Rheumatology, University of Minnesota, Minneapolis 55455.

出版信息

J Immunol. 1994 Nov 15;153(10):4388-98.

PMID:7963517
Abstract

We report the cloning and initial characterization of the mouse homologues of the bcl-2-related gene, bcl-x. We compare these to the two major isoforms of human bcl-x that were previously identified, bcl-xLong (bcl-xL) which has death repressor activity similar to bcl-2, and bcl-xShort (bcl-xS), an alternative mRNA splice product that deletes a highly conserved domain shared by bcl-2 family members and promotes cell death in transfection studies. In addition to murine (m) bcl-xL and mbcl-xS, we have cloned a novel cDNA isoform that we designate mbcl-x delta TM. This cDNA deletes, by means of alternative splicing, the carboxy terminal transmembrane domain of bcl-x and is predicted to be a soluble, rather than membrane-bound, protein. We found that mbcl-x mRNA is highly inducible in splenocytes stimulated with either anti-CD3 Abs or LPS/dextran sulfate, and that the major species of mbcl-x mRNA in a variety of cell lines and tissues was the xL isoform. Transfection of mbcl-xL or mbcl-xS into Hela cells resulted in targeting primarily to mitochondria, whereas mbcl-x delta TM localized diffusely throughout the cytosol. Overexpression of the novel delta TM isoform in an IL-3-dependent cell line delayed the onset of apoptosis induced by growth factor withdrawal. Thus, a naturally-occurring form of mbcl-x present in lymphocytes that does not localize to the mitochondrial membrane is functional in preventing apoptotic cell death. Moreover, these data suggest that bcl-x provides a life signal in activated lymphocytes.

摘要

我们报告了与bcl-2相关基因bcl-x的小鼠同源物的克隆及初步特性分析。我们将这些与先前鉴定出的人类bcl-x的两种主要异构体进行比较,即具有与bcl-2相似的死亡抑制活性的bcl-x长型(bcl-xL),以及bcl-x短型(bcl-xS),后者是一种选择性mRNA剪接产物,缺失了bcl-2家族成员共有的一个高度保守结构域,并在转染研究中促进细胞死亡。除了小鼠(m)bcl-xL和mbcl-xS外,我们还克隆了一种新的cDNA异构体,命名为mbcl-xδTM。该cDNA通过选择性剪接缺失了bcl-x的羧基末端跨膜结构域,预计是一种可溶性而非膜结合蛋白。我们发现mbcl-x mRNA在用抗CD3抗体或脂多糖/硫酸葡聚糖刺激的脾细胞中高度可诱导,并且在多种细胞系和组织中mbcl-x mRNA的主要类型是xL异构体。将mbcl-xL或mbcl-xS转染到Hela细胞中主要定位于线粒体,而mbcl-xδTM则弥散地分布于整个细胞质中。在依赖白细胞介素-3的细胞系中过表达新的δTM异构体可延迟因生长因子撤除诱导的细胞凋亡的发生。因此,淋巴细胞中存在的一种天然形式的mbcl-x,其不定位于线粒体膜,在预防凋亡性细胞死亡中具有功能。此外,这些数据表明bcl-x在活化的淋巴细胞中提供了一个生存信号。

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