Bcl-2通过其BH4结构域阻断由线粒体Ras介导的凋亡信号传导。

Bcl-2, via its BH4 domain, blocks apoptotic signaling mediated by mitochondrial Ras.

作者信息

Denis Gerald V, Yu Qiang, Ma Peihong, Deeds Linda, Faller Douglas V, Chen Chang-Yan

机构信息

Cancer Research Center and Department of Medicine, Boston University School of Medicine, Boston, Massachusetts 02118, USA.

出版信息

J Biol Chem. 2003 Feb 21;278(8):5775-85. doi: 10.1074/jbc.M210202200. Epub 2002 Dec 10.

DOI:10.1074/jbc.M210202200

PMID:12477721

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11093621/

Abstract

Bcl-2 protects cells against Ras-mediated apoptosis; this protection coincides with its binding to Ras. However, the protection mechanism has remained enigmatic. Here, we demonstrate that, upon apoptotic stimulation, newly synthesized Bcl-2 redistributes to mitochondria, interacts there with activated Ras, and blocks Ras-mediated apoptotic signaling. We also show, by employing bcl-2 mutants, that the BH4 domain of Bcl-2 binds to Ras and regulates its anti-apoptotic activity. Experiments with a C-terminal-truncated Ras or a farnesyltransferase inhibitor demonstrate that the CAAX motif of Ras is essential for apoptotic signaling and Bcl-2 association. The results indicate a potential mechanism by which Bcl-2 protects cells against Ras-mediated apoptotic signaling.

摘要

Bcl-2保护细胞免受Ras介导的凋亡；这种保护作用与其与Ras的结合同时发生。然而，保护机制一直不明。在此，我们证明，在凋亡刺激下，新合成的Bcl-2重新分布到线粒体，在那里与活化的Ras相互作用，并阻断Ras介导的凋亡信号传导。我们还通过使用bcl-2突变体表明，Bcl-2的BH4结构域与Ras结合并调节其抗凋亡活性。用C末端截短的Ras或法尼基转移酶抑制剂进行的实验表明，Ras的CAAX基序对于凋亡信号传导和Bcl-2缔合至关重要。这些结果表明了Bcl-2保护细胞免受Ras介导的凋亡信号传导的潜在机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ae8c/11093621/d58ce8525e4c/nihms-1992072-f0001.jpg

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Bcl-2通过其BH4结构域阻断由线粒体Ras介导的凋亡信号传导。

Bcl-2, via its BH4 domain, blocks apoptotic signaling mediated by mitochondrial Ras.

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