| RIP1 autophosphorylation is promoted by mitochondrial ROS and is essential for RIP3 recruitment into necrosome | |
| Yingying Zhang ; Zhang YY(张荧荧) ; Sheng Sean Su ; Su S(苏晟) ; Shubo Zhao ; Zhentao Yang ; Chuan-Qi Zhong ; Xin Chen ; Qixu Cai ; Zhang-Hua Yang ; Deli Huang ; Rui Wu ; Jiahuai Han ; Han JH(韩家淮) | |
| 2017-02-08 | |
| 英文摘要 | 韩家淮教授课题组的这项研究揭示了活性氧簇(ROS)通过直接特异地氧化受体相互作用丝氨酸/苏氨酸激酶1(RIP1)上的三个关键的半胱氨酸,进而特异地增强RIP1在S161上的自磷酸化,从而促进坏死小体的形成和程序性细胞坏死的发生。证实了RIP1的激酶活性在程序性细胞坏死中的主要功能是自磷酸化S161,且S161就是人们长期寻找的RIP1上与坏死相关的功能性磷酸化位点。坏死小体的形成是程序性细胞坏死发生的必要复合物,而S161的磷酸化是RIP1有效募集RIP3形成有功能的坏死小体所必需的。由于ROS的产生依赖于坏死小体里的RIP3的功能,因此ROS介导了程序性坏死通路里的正反馈调控。研究阐明了ROS促进程序性细胞坏死的分子机制,回答了领域内长期存在的两个科学问题,对全面解析程序性坏死机制并协助疾病治疗具有重要意义。 张荧荧和苏晟为该论文的共同第一作者。该项研究得到了973计划和国家自然科学基金委员会重点和重大研究计划项目的经费支持。; 【Abstract】Necroptosis is a type of programmed cell death with great significance in many pathological processes. Tumour necrosis factor-a(TNF), a proinflammatory cytokine, is a prototypic trigger of necroptosis. It is known that mitochondrial reactive oxygen species (ROS) promote necroptosis, and that kinase activity of receptor interacting protein 1 (RIP1) is required for TNF-induced necroptosis. However, how ROS function and what RIP1 phosphorylates to promote necroptosis are largely unknown. Here we show that three crucial cysteines in RIP1 are required for sensing ROS, and ROS subsequently activates RIP1 autophosphorylation on serine residue 161 (S161). The major function of RIP1 kinase activity in TNF-induced necroptosis is to autophosphorylate S161. This specific phosphorylation then enables RIP1 to recruit RIP3 and form a functional necrosome, a central controller of necroptosis. Since ROS induction is known to require necrosomal RIP3, ROS therefore function in a positive feedback circuit that ensures effective induction of necroptosis.; This work was supported by the National Natural Science Foundation of China (91029304, 31420103910, 31330047 and 81630042), the National Basic Research Program of China (973 Program; 2015CB553800, 2013CB944903, 2014CB541804), the 111 Project (B12001), the National Science Foundation of China for Fostering Talents in Basic Research (J1310027). |
| 语种 | 中文 |
| 出版者 | Macmillan Publishers Limited |
| 内容类型 | 其他 |
| 源URL | [http://dspace.xmu.edu.cn/handle/2288/127531]  |
| 专题 | 生命科学-已发表论文 |
| 推荐引用方式 GB/T 7714 | Yingying Zhang,Zhang YY,Sheng Sean Su,et al. RIP1 autophosphorylation is promoted by mitochondrial ROS and is essential for RIP3 recruitment into necrosome. 2017-02-08. |
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