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Processing/activation of at least four interleukin-1β converting enzyme-like proteases occurs during the execution phase of apoptosis in human monocytic tumor cells

机译:在人单核细胞肿瘤细胞凋亡的执行阶段,发生至少四种白介素-1β转化酶样蛋白酶的加工/激活

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摘要

Identification of the processing/activation of multiple interleukin-1β converting enzyme (ICE)–like proteases and their target substrates in the intact cell is critical to our understanding of the apoptotic process. In this study we demonstrate processing/activation of at least four ICE-like proteases during the execution phase of apoptosis in human monocytic tumor THP.1 cells. Apoptosis was accompanied by processing of Ich-1, CPP32, and Mch3α to their catalytically active subunits, and lysates from these cells displayed a proteolytic activity with kinetics, characteristic of CPP32/Mch3α but not of ICE. Fluorescence-activated cell sorting was used to obtain pure populations of normal and apoptotic cells. In apoptotic cells, extensive cleavage of Ich-1, CPP32, and Mch3α was observed together with proteolysis of the ICE-like protease substrates, poly (ADP-ribose) polymerase (PARP), the 70-kD protein component of U1 small nuclear ribonucleoprotein (U170K), and lamins A/B. In contrast, no cleavage of CPP32, Mch3α or the substrates was observed in normal cells. In cells exposed to an apoptotic stimulus, some processing of Ich-1 was detected in morphologically normal cells, suggesting that cleavage of Ich-1 may occur early in the apoptotic process. The ICE-like protease inhibitor, benzyloxycarbonyl-Val-Ala-Asp (OMe) fluoromethyl ketone (Z-VAD.FMK), inhibited apoptosis and cleavage of Ich-1, CPP32, Mch3α, Mch2α, PARP, U1-70K, and lamins. These results suggest that Z-VAD.FMK inhibits apoptosis by inhibiting a key effector protease upstream of Ich-1, CPP32, Mch3α, and Mch2α. Together these observations demonstrate that processing/activation of Ich-1, CPP32, Mch3α, and Mch2α accompanies the execution phase of apoptosis in THP.1 cells. This is the first demonstration of the activation of at least four ICE-like proteases in apoptotic cells, providing further evidence for a requirement for the activation of multiple ICE-like proteases during apoptosis.
机译:完整细胞中多种白介素-1β转换酶(ICE)样蛋白酶及其靶底物的加工/激活的鉴定对于我们了解凋亡过程至关重要。在这项研究中,我们证明了在人类单核细胞THP.1细胞凋亡执行阶段,至少有四种ICE样蛋白酶的加工/激活。凋亡伴随着Ich-1,CPP32和Mch3α加工成它们的催化活性亚基,来自这些细胞的裂解物表现出具有动力学的蛋白水解活性,是CPP32 /Mch3α的特征,而不是ICE。荧光激活细胞分选用于获得正常细胞和凋亡细胞的纯种群。在凋亡细胞中,观察到Ich-1,CPP32和Mch3α的广泛切割,以及ICE样蛋白酶底物,聚(ADP-核糖)聚合酶(PARP)的蛋白水解,U1小核核糖核蛋白的70-kD蛋白成分。 (U170K)和lamins A / B。相反,在正常细胞中未观察到CPP32,Mch3α或底物的裂解。在暴露于凋亡刺激的细胞中,形态学正常的细胞中检测到了Ich-1的某些加工,这表明Ich-1的切割可能发生在凋亡过程的早期。 ICE样蛋白酶抑制剂苄氧基羰基-Val-Ala-Asp(OMe)氟甲基酮(Z-VAD.FMK)抑制Ich-1,CPP32,Mch3α,Mch2α,PARP,U1-70K和Lamins的凋亡和裂解。这些结果表明,Z-VAD.FMK通过抑制Ich-1,CPP32,Mch3α和Mch2α上游的关键效应蛋白酶来抑制细胞凋亡。这些观察结果共同证明,Ich-1,CPP32,Mch3α和Mch2α的加工/激活伴随着THP.1细胞凋亡的执行阶段。这是凋亡细胞中至少四种ICE样蛋白酶活化的首次证明,为凋亡期间需要多种ICE样蛋白酶活化提供了进一步的证据。

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