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The contribution of apoptosis-inducing factor, caspase-activated DNase, and inhibitor of caspase-activated DNase to the nuclear phenotype and DNA degradation during apoptosis.

机译:凋亡诱导因子,caspase激活的DNase和caspase激活的DNase抑制剂对细胞凋亡过程中的核表型和DNA降解的贡献。

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摘要

We have assessed the contribution of apoptosis-inducing factor (AIF) and inhibitor of caspase-activated DNase (ICAD) to the nuclear morphology and DNA degradation pattern in staurosporine-induced apoptosis. Expression of D117E ICAD, a mutant that is resistant to caspase cleavage at residue 117, prevented low molecular weight (LMW) DNA fragmentation, stage II nuclear morphology, and detection of terminal deoxynucleotidyl transferase staining. However, high molecular weight (HMW) DNA fragmentation and stage I nuclear morphology remained unaffected. On the other hand, expression of either D224E or wild type ICAD had no effect on DNA fragmentation or nuclear morphology. In addition, both HMW and LMW DNA degradation required functional executor caspases. Interestingly, silencing of endogenous AIF abolished type I nuclear morphology without any effect on HMW or LMW DNA fragmentation. Together, these results demonstrate that AIF is responsible for stage I nuclear morphology and suggest that HMW DNA degradation is a caspase-activated DNase and AIF-independent process.
机译:我们已经评估了凋亡诱导因子(AIF)和胱天蛋白酶激活的脱氧核糖核酸酶(ICAD)抑制剂对星形孢菌素诱导的细胞凋亡的核形态和DNA降解模式的贡献。 D117E ICAD的表达是一种突变体,对残基117处的半胱天冬酶裂解有抵抗力,可防止低分子量(LMW)DNA片段化,II期核形态和末端脱氧核苷酸转移酶染色的检测。但是,高分子量(HMW)DNA片段化和I期核形态仍不受影响。另一方面,D224E或野生型ICAD的表达对DNA片段化或核形态没有影响。此外,HMW和LMW DNA降解都需要功能执行子胱天蛋白酶。有趣的是,内源性AIF沉默消除了I型核形态,而对HMW或LMW DNA片段没有任何影响。总之,这些结果表明AIF负责I期核形态,并表明HMW DNA降解是caspase激活的DNase和AIF独立的过程。

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