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DNA依赖性蛋白激酶是在细胞凋亡早期被特异性切割的自身抗原亚群之一。

DNA-dependent protein kinase is one of a subset of autoantigens specifically cleaved early during apoptosis.

作者信息

Casciola-Rosen L A, Anhalt G J, Rosen A

机构信息

Department of Dermatology, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205, USA.

出版信息

J Exp Med. 1995 Dec 1;182(6):1625-34. doi: 10.1084/jem.182.6.1625.

Abstract

Proteolytic cleavage of key substrates appears to be an important biochemical mechanism underlying the apoptotic process, and the centrality of interleukin 1 beta-converting enzyme (ICE)-like proteases as mediators of apoptosis has been suggested. The identification of the relevant substrates of the ICE protease family during apoptosis therefore constitutes a major challenge. Using human autoantibodies, we demonstrate here that a subset of autoantigens is specifically cleaved early during apoptosis. One of these cleaved molecules is identified as the catalytic subunit of the DNA-dependent protein kinase. The time courses of all proteolytic cleavages are identical and coincide with the onset of morphologic apoptosis. Furthermore, all cleavages share the same inhibition characteristics, which implicate an ICE-like activity(ies). We propose that cleavage of these autoantigens targets these molecules for an autoimmune response by revealing immunocryptic fragments in a proimmune apoptotic setting. Study of the immunogenicity of these fragments may yield insights into the autoimmune targeting of molecules. Moreover, the autoantibodies described will be valuable tools for the elucidation of mechanistically important proteolytic steps along the apoptotic pathway.

摘要

关键底物的蛋白水解切割似乎是凋亡过程背后的一种重要生化机制,并且有人提出白细胞介素1β转换酶(ICE)样蛋白酶作为凋亡介质的核心地位。因此,鉴定凋亡过程中ICE蛋白酶家族的相关底物构成一项重大挑战。利用人类自身抗体,我们在此证明一部分自身抗原在凋亡早期被特异性切割。其中一个被切割的分子被鉴定为DNA依赖性蛋白激酶的催化亚基。所有蛋白水解切割的时间进程相同,且与形态学凋亡的开始一致。此外,所有切割都具有相同的抑制特性,这暗示存在一种ICE样活性。我们提出这些自身抗原的切割通过在促免疫凋亡环境中暴露免疫隐蔽片段,使这些分子成为自身免疫反应的靶标。对这些片段免疫原性的研究可能会深入了解分子的自身免疫靶向作用。此外,所描述的自身抗体将成为阐明凋亡途径中重要机制性蛋白水解步骤的有价值工具。

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