Structure of the CED-4–CED-9 complex provides insights into programmed cell death in Caenorhabditis elegans

被引:0
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作者
Nieng Yan
Jijie Chai
Eui Seung Lee
Lichuan Gu
Qun Liu
Jiaqing He
Jia-Wei Wu
David Kokel
Huilin Li
Quan Hao
Ding Xue
Yigong Shi
机构
[1] Princeton University,Department of Molecular Biology
[2] Lewis Thomas Laboratory,Department of Molecular, Cellular and Developmental Biology
[3] University of Colorado,Department of Life Science
[4] Gwangju Institute of Science and Technology,Molecular Biology and Genetics
[5] Cornell University,Biology Department
[6] Brookhaven National Laboratory,undefined
来源
Nature | 2005年 / 437卷
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摘要
Interplay among four genes—egl-1, ced-9, ced-4 and ced-3—controls the onset of programmed cell death in the nematode Caenorhabditis elegans. Activation of the cell-killing protease CED-3 requires CED-4. However, CED-4 is constitutively inhibited by CED-9 until its release by EGL-1. Here we report the crystal structure of the CED-4–CED-9 complex at 2.6 Å resolution, and a complete reconstitution of the CED-3 activation pathway using homogeneous proteins of CED-4, CED-9 and EGL-1. One molecule of CED-9 binds to an asymmetric dimer of CED-4, but specifically recognizes only one of the two CED-4 molecules. This specific interaction prevents CED-4 from activating CED-3. EGL-1 binding induces pronounced conformational changes in CED-9 that result in the dissociation of the CED-4 dimer from CED-9. The released CED-4 dimer further dimerizes to form a tetramer, which facilitates the autoactivation of CED-3. Together, our studies provide important insights into the regulation of cell death activation in C. elegans.
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页码:831 / 837
页数:6
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