自动处理的胱天蛋白酶在焦磷酸中靶向GSDMD的结构机制。,Cell

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自动处理的胱天蛋白酶在焦磷酸中靶向GSDMD的结构机制。
Cell ( IF 45.5 ) Pub Date : 2020-02-17 , DOI: 10.1016/j.cell.2020.02.002
Kun Wang ₁ , Qi Sun ₂ , Xiu Zhong ₁ , Mengxue Zeng ₃ , Huan Zeng ₄ , Xuyan Shi ₃ , Zilin Li ₂ , Yupeng Wang ₂ , Qiang Zhao ₅ , Feng Shao ₆ , Jingjin Ding ₄

Affiliation

Peking University-Tsinghua University-National Institute of Biological Sciences Joint Graduate Program, National Institute of Biological Sciences, 102206 Beijing, China; National Institute of Biological Sciences, Beijing, 102206 Beijing, China.
Research Unit of Pyroptosis and Immunity, Chinese Academy of Medical Sciences 2019RU076, 102206 Beijing, China; National Institute of Biological Sciences, Beijing, 102206 Beijing, China.
National Institute of Biological Sciences, Beijing, 102206 Beijing, China.
National Laboratory of Biomacromolecules, CAS Center for Excellence in Biomacromolecules, Institute of Biophysics, Chinese Academy of Sciences, 100101 Beijing, China; National Institute of Biological Sciences, Beijing, 102206 Beijing, China.
Organ Transplant Center, The First Affiliated Hospital, Sun Yat-sen University, 510080 Guangzhou, China.
Peking University-Tsinghua University-National Institute of Biological Sciences Joint Graduate Program, National Institute of Biological Sciences, 102206 Beijing, China; Research Unit of Pyroptosis and Immunity, Chinese Academy of Medical Sciences 2019RU076, 102206 Beijing, China; National Institute of Biological Sciences, Beijing, 102206 Beijing, China; Tsinghua Institute of Multidisciplinary Biomedical Research, Tsinghua University, 102206 Beijing, China.

炎性体激活的caspase-1和LPS激活的caspase-11 / 4/5裂解了热解执行蛋白GSDMD。切割从GSMDD-C-末端结构域解开孔形成结构域。caspase如何识别GSDMD及其与caspase激活的联系尚不清楚。在这里，我们显示了产生p10产物的特定于位点的caspase-4 / 11自动加工，对于裂解GSDMD和诱导发烧是必需的和足够的。p10形式的自动加工的caspase-4 / 11以高亲和力结合GSDMD-C结构域。自动处理和未处理的capase-11的结构比较可确定自动处理诱导的β折叠。在caspase-4 / 11-GSDMD-C复合晶体结构中，β片组织了疏水性GSDMD结合界面，只有p10形式的caspase-4 / 11才可能。结合促进二聚化介导的半胱天冬酶激活，使得切割独立于切割位点四肽序列。caspase-1-GSDMD-C复合物的晶体结构显示出相似的GSDMD识别模式。我们的研究揭示了针对胱天蛋白酶的前所未有的底物靶向机制。疏水性界面为开发特异于光解胱天蛋白酶的抑制剂提供了额外的空间。

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更新日期：2020-02-28

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