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Ordering of caspases in cells undergoing apoptosis by the intrinsic pathway.

机译:半胱天冬酶在通过内在途径经历凋亡的细胞中的顺序。

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Caspases are a family of aspartate-specific cysteine proteases responsible for the biochemical and morphological changes that occur during the execution phase of apoptosis. The hierarchical ordering of caspases has been clearly established using dATP-activated cell lysates to model the intrinsic pathway induced by initial mitochondrial perturbation. In this model, caspase-9, the apical caspase, directly processes and activates the effector caspases, caspase-3 and -7, and then active caspase-3 but not caspase-7, processes caspase-2 and -6, and subsequently the activated caspase-6 processes caspase-8 and -10. To address the possibility that this model in vitro system might not reflect the precise ordering of caspases in intact cells, we have examined this possibility in cells induced to undergo apoptosis by activation of the intrinsic pathway. We have used caspase deficient cells, small interference RNA for caspase-6 and -7, and a specific caspase-3 inhibitor. In contrast to the earlier in vitro studies, we now show that in intact cells caspase-7 can also directly process and activate caspase-2 and -6. The processing of caspase-2 and -6 occurs within the cytoplasm and active caspase-6 is then responsible for both the processing of caspase-8 and the cleavage of caspase-6 substrates, including lamin A/C.
机译:胱天蛋白酶是天冬氨酸特异性半胱氨酸蛋白酶的家族,其负责在凋亡执行阶段发生的生化和形态变化。已使用dATP激活的细胞裂解物对由最初的线粒体扰动诱导的内在途径进行建模,明确建立了半胱天冬酶的分层顺序。在此模型中,顶端的半胱天冬酶caspase-9直接处理并激活效应半胱天冬酶caspase-3和-7,然后激活caspase-3,但不激活caspase-3,先处理caspase-2和-6,然后再处理激活的caspase-6处理caspase-8和-10。为了解决这种模型体外系统可能无法反映完整细胞中半胱氨酸蛋白酶的精确顺序的可能性,我们已经研究了通过内在途径激活而诱导发生凋亡的细胞中的这种可能性。我们已经使用了caspase缺陷细胞,用于caspase-6和-7的小干扰RNA以及特定的caspase-3抑制剂。与早期的体外研究相反,我们现在显示在完整细胞中caspase-7也可以直接加工并激活caspase-2和-6。 caspase-2和-6的加工在细胞质内发生,然后活性caspase-6负责caspase-8的加工和caspase-6底物(包括层粘蛋白A / C)的切割。

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