The biochemical mechanism of caspase-2 activation

被引:0
|
作者
B C Baliga
S H Read
S Kumar
机构
[1] Hanson Institute,Department of Medicine
[2] IMVS,undefined
[3] Adelaide University,undefined
来源
Cell Death & Differentiation | 2004年 / 11卷
关键词
caspase-2; dimerization; activation; proteolytic cleavage; initiator caspase;
D O I
暂无
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学科分类号
摘要
A unified model for initiator caspase activation has previously been proposed based on the biochemical analysis of caspase-8 and -9. Caspase-2 is structurally related to caspase-9, but its mechanism of activation is not known. Using an uncleavable mutant of caspase-2, we show that dimerization (and not processing) is the key event that drives initial procaspase-2 activation. Following dimerization, caspase-2 undergoes autocatalytic cleavage that promotes its stable dimerization and further enhances the catalytic activity of caspase-2. Although the caspase-2 zymogen does not require cleavage for the initial acquisition of activity, intersubunit cleavage is required to generate levels of activity required to induce cell death by overexpression. We also provide evidence that the reported disulfide bond linkage between two caspase-2 monomers is dispensable for caspase-2 dimerization. As caspase-2 does not require cleavage for its initial activation, our findings confirm caspase-2 to be a bona fide initiator caspase.
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页码:1234 / 1241
页数:7
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