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在促凋亡应激过程中,通过高尔基解体和半胱天冬酶切割使神经酰胺转移蛋白失活。

Inactivation of ceramide transfer protein during pro-apoptotic stress by Golgi disassembly and caspase cleavage.

机构信息

Department of Cell Biology, Johns Hopkins University School of Medicine, 725 N. Wolfe Street, Baltimore, MD 21205, U.S.A.

出版信息

Biochem J. 2012 Mar 1;442(2):391-401. doi: 10.1042/BJ20111461.

Abstract

The mammalian Golgi apparatus is composed of multiple stacks of cisternal membranes organized laterally into a polarized ribbon. Furthermore, trans-Golgi membranes come in close apposition with ER (endoplasmic reticulum) membranes to form ER-trans-Golgi contact sites, which may facilitate transfer of newly synthesized ceramide from the ER to SM (sphingomyelin) synthase at the trans-Golgi via CERT (ceramide transfer protein). CERT interacts with both ER and Golgi membranes, and together with Golgi morphology contributes to efficient SM synthesis. In the present study, we show that Golgi disassembly during pro-apoptotic stress induced by TNFα (tumour necrosis factor α) and anisomycin results in decreased levels of CERT at the Golgi region. This is accompanied by a caspase-dependent loss of full-length CERT and reduction in de novo SM synthesis. In vitro, CERT is cleaved by caspases 2, 3 and 9. Truncated versions of CERT corresponding to fragments generated by caspase 2 cleavage at Asp213 were mislocalized and did not promote efficient de novo SM synthesis. Thus it is likely that during cellular stress, disassembly of Golgi structure together with inactivation of CERT by caspases causes a reduction in ceramide trafficking and SM synthesis, and could contribute to the cellular response to pro-apoptotic stress.

摘要

哺乳动物的高尔基体由多个 cisternal 膜堆叠组成,这些膜横向排列成一个极化的带状结构。此外,trans-Golgi 膜与 ER(内质网)膜紧密相邻,形成 ER-trans-Golgi 接触位点,这可能有助于通过 CERT(ceramide transfer protein)将新合成的 ceramide 从 ER 转移到 trans-Golgi 中的 SM(sphingomyelin)合成酶。CERT 与 ER 和高尔基体膜相互作用,与高尔基体形态一起有助于有效的 SM 合成。在本研究中,我们表明,TNFα(肿瘤坏死因子 α)和 anisomycin 诱导的促凋亡应激期间高尔基体的解体导致高尔基体区域 CERT 水平降低。这伴随着 caspase 依赖性全长 CERT 的丧失和新的 SM 合成减少。在体外,CERT 被 caspase 2、3 和 9 切割。与 caspase 2 在 Asp213 处切割产生的片段相对应的 CERT 截断形式被错误定位,并且不能促进有效的新的 SM 合成。因此,在细胞应激期间,高尔基体结构的解体以及 caspase 对 CERT 的失活可能导致 ceramide 转运和 SM 合成减少,并可能有助于细胞对促凋亡应激的反应。

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