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Unique and overlapping substrate specificities of caspase-8 and caspase-10

机译:caspase-8和caspase-10独特且重叠的底物特异性

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摘要

Although caspase-8 has an established role as an initiator of death receptor-mediated apoptosis, the function of its closest homolog, caspase-10, is almost completely unknown. To gain a closer insight into the physiological function of caspase-10, we compared the cleavage of known caspase-8 substrates by both initiator caspases. We demonstrate that caspase-10 and -8 have overlapping cleavage preferences for several substrates such as the kinases RIP and PAK2. Interestingly, in other substrates, such as the Bcl-2 protein Bid, we found additional and distinct cleavage sites for both caspases, which might have important consequences for mitochondrial targeting and propagation of the death signal. Caspase-8 and -10 also caused different interchain cleavage patterns of their enzyme precursors. Together, these results suggest that caspase-8 and -10, despite having overlapping functions, also have selective substrate cleavage specificities and might thereby exert nonredundant roles in apoptosis signaling.
机译:尽管caspase-8作为死亡受体介导的细胞凋亡的引发剂已经确立了作用,但其最接近的同系物caspase-10的功能几乎是完全未知的。为了更深入地了解caspase-10的生理功能,我们比较了两种启动子半胱天冬酶对已知caspase-8底物的裂解。我们证明半胱天冬酶10和-8具有重叠的切割偏好的几种底物,如激酶RIP和PAK2。有趣的是,在其他底物(例如Bcl-2蛋白Bid)中,我们发现了两个半胱天冬酶的额外且不同的切割位点,这可能对线粒体靶向和死亡信号的传播产生重要影响。 Caspase-8和-10也引起了其酶前体的不同链间切割模式。总之,这些结果表明,尽管具有重叠的功能,caspase-8和-10也具有选择性的底物切割特异性,因此可能在凋亡信号传导中发挥非冗余作用。

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