Caspase-8 Blocks Receptor-Interacting Protein Kinase-1 Kinase-Independent Necroptosis during Embryogenesis.

Haiwei Zhang, Xiaoxia Wu, Ming Li, Xiaoming Li, Lingxia Wang, Jianling Liu, Yangjing Ou, Xuanhui Wu, Mingyan Xing, Fang Li, Xiaoming Zhao, Han Liu, Connor Jones, Jiangshan Deng, Qun Xie, Yue Zhang, Yan Luo, Yuwu Zhao, Haibing Zhang
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Abstract

Caspase-8 (Casp8) suppresses receptor-interacting protein kinase-3 (RIPK3)/mixed lineage kinase domain-like protein (MLKL)-dependent necroptosis, demonstrated by the genetic evidence that deletion of Ripk3 or Mlkl prevented embryonic lethality of Casp8-deficient mice. However, the detailed mechanisms by which Casp8 deficiency triggers necroptosis during embryonic development remain unclear. In this article, we show that Casp8 deletion caused formation of the RIPK1-RIPK3 necrosome in the yolk sac, leading to vascularization defects, prevented by MLKL and RIPK3 deficiency, or RIPK3 RHIM mutant (RIPK3 V448P), but not by the RIPK1 kinase-dead mutant (RIPK1 K45A). In addition, Ripk1K45A/K45ACasp8 -/- mice died on embryonic day 14.5, which was delayed to embryonic day 17.5 by ablation of one allele in Ripk1 and was completely rescued by ablation of Mlkl Our results revealed an in vivo role of RIPK3 RHIM and RIPK1K45A scaffold-mediated necroptosis in Casp8 deficiency embryonic development and suggested that the Casp8-deficient yolk sac might be implicated in identifying novel regulators as an in vivo necroptotic model.

胚胎发生过程中Caspase-8阻断受体相互作用蛋白激酶-1激酶不依赖的坏死性上睑下垂。
Casp8 (Casp8)抑制受体相互作用蛋白激酶-3 (RIPK3)/混合谱系激酶结构域样蛋白(MLKL)依赖的necroptosis,遗传学证据表明,RIPK3或MLKL的缺失可防止Casp8缺陷小鼠的胚胎致死。然而,Casp8缺乏在胚胎发育过程中引发坏死性死亡的详细机制尚不清楚。在这篇文章中,我们发现Casp8缺失导致卵黄囊中RIPK1-RIPK3坏死体的形成,导致血管化缺陷,这被MLKL和RIPK3缺陷或RIPK3 RHIM突变体(RIPK3 V448P)阻止,而不是被RIPK1激酶死亡突变体(RIPK1 K45A)阻止。此外,Ripk1K45A/K45ACasp8 -/-小鼠在胚胎第14.5天死亡,通过消融Ripk1的一个等位基因延迟到胚胎第17.5天,并通过消融mlk1完全恢复。我们的研究结果揭示了RIPK3 RHIM和Ripk1K45A支架介导的坏死坏死在Casp8缺乏症胚胎发育中的体内作用,并提示Casp8缺乏症卵黄囊可能与鉴定新的调节因子作为体内坏死坏死模型有关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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