首页> 外文期刊>Molecular and Cellular Endocrinology >Ca2+-PKC-caspase 3-like protease pathway mediates DNA and nuclear fragmentation in ecdysteroid-induced programmed cell death.
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Ca2+-PKC-caspase 3-like protease pathway mediates DNA and nuclear fragmentation in ecdysteroid-induced programmed cell death.

机译:Ca2 + -PKC-胱天蛋白酶3样蛋白酶途径介导蜕皮激素诱导的程序性细胞死亡中的DNA和核片段化。

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摘要

20-Hydroxyecdysone (20E) induces programmed cell death in the anterior silk gland of the silkworm. Here, we report the direct interaction between Ca(2+) and protein kinase C (PKC)-caspase 3-like protease pathway in the 20E-induced cell death. The calcium ionophore can mimic 20E effects in inducing DNA and nuclear fragmentation, but such mimicry is only possible in the glands precultured for 18 h with 20E. The simultaneous presence of translation inhibitor with 20E in the preculture showed that de novo protein synthesis was needed to mimic 20E effects by the calcium ionophore. Both a PKC inhibitor and a caspase 3 inhibitor inhibited the mimicking effects. After substitution of the calcium ionophore for 20E, caspase 3-like protease was fully activated 12h later, and DNA and nuclear fragmentation occurred faster than continuous 20E stimuli. The results show the presence of a Ca(2+)-PKC-caspase 3-like protease pathway in 20E signaling, and possible involvement of the pathway up to the mobilization of Ca(2+) in regulating the timing of cell death in vivo.
机译:20-羟基蜕皮激素(20E)诱导家蚕前丝腺中程序性细胞死亡。在这里,我们报告在20E诱导的细胞死亡中Ca(2+)和蛋白激酶C(PKC)-caspase 3-like蛋白酶途径之间的直接相互作用。钙离子载体可以模拟20E在诱导DNA和核片段化中的作用,但是这种模仿仅在用20E预培养18小时的腺体中才有可能。预培养物中同时存在翻译抑制剂和20E,这表明需要从头合成蛋白质来模拟钙离子载体对20E的作用。 PKC抑制剂和caspase 3抑制剂均抑制了模仿效果。用钙离子载体取代20E后,半胱天冬酶3样蛋白酶在12h后被完全激活,DNA和核片段的发生比连续20E刺激快。结果表明,在20E信号中存在Ca(2 +)-PKC-胱天蛋白酶3样蛋白酶途径,并可能参与该途径直至动员Ca(2+)来调节体内细胞死亡的时间。

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