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Published November 2003 | public
Journal Article Metadata-only

Molecular mechanism of Reaper-Grim-Hid-mediated suppression of DIAP1-dependent Dronc ubiquitination

Chai, Jijie
Yan, Nieng
Huh, Jun R.
Wu, Jia-Wei
Li, Wenyu
Hay, Bruce A.
Shi, Yigong

Abstract

The inhibitor of apoptosis protein DIAP1 inhibits Dronc-dependent cell death by ubiquitinating Dronc. The pro-death proteins Reaper, Hid and Grim (RHG) promote apoptosis by antagonizing DIAP1 function. Here we report the structural basis of Dronc recognition by DIAP1 as well as a novel mechanism by which the RHG proteins remove DIAP1-mediated downregulation of Dronc. Biochemical and structural analyses revealed that the second BIR (BIR2) domain of DIAP1 recognizes a 12-residue sequence in Dronc. This recognition is essential for DIAP1 binding to Dronc, and for targeting Dronc for ubiquitination. Notably, the Dronc-binding surface on BIR2 coincides with that required for binding to the N termini of the RHG proteins, which competitively eliminate DIAP1-mediated ubiquitination of Dronc. These observations reveal the molecular mechanisms of how DIAP1 recognizes Dronc, and more importantly, how the RHG proteins remove DIAP1-mediated ubiquitination of Dronc.

Additional Information

© 2003 Nature Publishing Group. Received 26 June 2003; Accepted 13 August 2003; Published online: 28 September 2003. We thank L. Walsh and others at CHESS for help with beam time and data collection. This research was supported by US National Institutes of Health grants.

Additional details

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Created:
August 19, 2023
Modified:
October 23, 2023