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钙蛋白酶系统作为应激/损伤反应的调节因子。

The calpain system as a modulator of stress/damage response.

作者信息

Demarchi Francesca, Schneider Claudio

机构信息

Laboratorio Nazionale Consorzio Interuniversitario Biotecnologie, AREA Science Park, Trieste, Italy.

出版信息

Cell Cycle. 2007 Jan 15;6(2):136-8. doi: 10.4161/cc.6.2.3759. Epub 2007 Jan 27.

DOI:10.4161/cc.6.2.3759
PMID:17264674
Abstract

Ubiquitously expressed mu- and m-calpain proteases consist of 80-kDa catalytic subunits encoded by the Capn1 and Capn2 genes, respectively, and a common 28-kDa regulatory subunit encoded by the calpain small 1 (Capns1) gene. The mu- and m-calpain proteases have been implicated in both pro-or anti-apoptotic functions. We have found that Capns1 depletion is coupled to increased sensitivity to increased sensitivity to apoptosis triggered by a number of autophagy-inducing stimuli in mammalian cells. Therefore we investigated the involvement of calpains in autophagy using MEFs derived from Capns1 knockout mice and Capns1 depleted human cells as model systems. We found that autophagy is impaired in Capns1 deficient cells by immunostaining of the endogenous autophagosome marker LC3 and electron microscopy experiments. Accordingly, the enhancement of lysosomal activity and long-lived proteins degradation, normally occurring upon starvation, are also reduced. In Capns1 depleted cells ectopic LC3 accumulates in early endosome-like vesicles that might represent a salvage pathway for protein degradation when autophagy is defective. Calpain represents a promising target for cancer therapy since its activity is tightly linked to tumor progression. Indeed it is elevated during transformation, it is required for autophagy and survival of cancer cells and plays a key role in metastatic cell migration and angiogenesis.

摘要

普遍表达的μ-钙蛋白酶和m-钙蛋白酶分别由Capn1和Capn2基因编码的80 kDa催化亚基以及由钙蛋白酶小亚基1(Capns1)基因编码的共同28 kDa调节亚基组成。μ-钙蛋白酶和m-钙蛋白酶已被证明具有促凋亡或抗凋亡功能。我们发现,在哺乳动物细胞中,Capns1的缺失与对多种自噬诱导刺激引发的凋亡敏感性增加有关。因此,我们使用源自Capns1基因敲除小鼠的成纤维细胞(MEFs)和Capns1缺失的人类细胞作为模型系统,研究了钙蛋白酶在自噬中的作用。通过对内源性自噬体标记物LC3进行免疫染色和电子显微镜实验,我们发现Capns1缺陷细胞中的自噬受损。相应地,通常在饥饿时发生的溶酶体活性增强和长寿蛋白降解也减少。在Capns1缺失的细胞中,异位的LC3积聚在早期内体样小泡中,当自噬有缺陷时,这些小泡可能代表蛋白质降解的一种挽救途径。钙蛋白酶是癌症治疗的一个有前景的靶点,因为其活性与肿瘤进展密切相关。事实上,它在细胞转化过程中升高,是癌细胞自噬和存活所必需的,并且在转移性细胞迁移和血管生成中起关键作用。

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