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Structural basis of IAP recognition by Smac/DIABLO

Author

Listed:
  • Geng Wu

    (Lewis Thomas Laboratory)

  • Jijie Chai

    (Lewis Thomas Laboratory)

  • Tomeka L. Suber

    (310 Aycock Dorm, University of North Carolina at Chapel Hill)

  • Jia-Wei Wu

    (Lewis Thomas Laboratory)

  • Chunying Du

    (University of Texas Southwestern Medical Center)

  • Xiaodong Wang

    (University of Texas Southwestern Medical Center)

  • Yigong Shi

    (Lewis Thomas Laboratory)

Abstract

Apoptosis is an essential process in the development and homeostasis of all metazoans1,2,3,4. The inhibitor-of-apoptosis (IAP) proteins suppress cell death by inhibiting the activity of caspases; this inhibition is performed by the zinc-binding BIR domains5,6 of the IAP proteins. The mitochondrial protein Smac/DIABLO promotes apoptosis by eliminating the inhibitory effect of IAPs through physical interactions7,8,9. Amino-terminal sequences in Smac/DIABLO are required for this function, as mutation of the very first amino acid leads to loss of interaction with IAPs and concomitant loss of Smac/DIABLO function9. Here we report the high-resolution crystal structure of Smac/DIABLO complexed with the third BIR domain (BIR3) of XIAP. Our results show that the N-terminal four residues (Ala-Val-Pro-Ile) in Smac/DIABLO recognize a surface groove on BIR3, with the first residue Ala binding a hydrophobic pocket and making five hydrogen bonds to neighbouring residues on BIR3. These observations provide a structural explanation for the roles of the Smac N terminus as well as the conserved N-terminal sequences in the Drosophila proteins Hid/Grim/Reaper. In conjunction with other observations, our results reveal how Smac may relieve IAP inhibition of caspase-9 activity. In addition to explaining a number of biological observations, our structural analysis identifies potential targets for drug screening.

Suggested Citation

  • Geng Wu & Jijie Chai & Tomeka L. Suber & Jia-Wei Wu & Chunying Du & Xiaodong Wang & Yigong Shi, 2000. "Structural basis of IAP recognition by Smac/DIABLO," Nature, Nature, vol. 408(6815), pages 1008-1012, December.
  • Handle: RePEc:nat:nature:v:408:y:2000:i:6815:d:10.1038_35050012
    DOI: 10.1038/35050012
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    Cited by:

    1. Shuo-Shuo Liu & Tian-Xia Jiang & Fan Bu & Ji-Lan Zhao & Guang-Fei Wang & Guo-Heng Yang & Jie-Yan Kong & Yun-Fan Qie & Pei Wen & Li-Bin Fan & Ning-Ning Li & Ning Gao & Xiao-Bo Qiu, 2024. "Molecular mechanisms underlying the BIRC6-mediated regulation of apoptosis and autophagy," Nature Communications, Nature, vol. 15(1), pages 1-16, December.

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