The DIAP1 RING finger mediates ubiquitination of Dronc and is indispensable for regulating apoptosis

Author:  ["Rebecca Wilson","Lakshmi Goyal","Mark Ditzel","Anna Zachariou","David A. Baker","Julie Agapite","Hermann Steller","Pascal Meier"]

Publication:  Nature Cell Biology

CITE.CC academic search helps you expand the influence of your papers.
Tags:  general   CellBiology   CancerResearch   DevelopmentalBiology   StemCells   Biological

Abstract

Members of the Inhibitor of Apoptosis Protein (IAP) family block activation of the intrinsic cell death machinery by binding to and neutralizing the activity of pro-apoptotic caspases. In Drosophila melanogaster, the pro-apoptotic proteins Reaper (Rpr), Grim and Hid (head involution defective) all induce cell death by antagonizing the anti-apoptotic activity of Drosophila IAP1 (DIAP1), thereby liberating caspases. Here, we show that in vivo, the RING finger of DIAP1 is essential for the regulation of apoptosis induced by Rpr, Hid and Dronc. Furthermore, we show that the RING finger of DIAP1 promotes the ubiquitination of both itself and of Dronc. Disruption of the DIAP1 RING finger does not inhibit its binding to Rpr, Hid or Dronc, but completely abrogates ubiquitination of Dronc. Our data suggest that IAPs suppress apoptosis by binding to and targeting caspases for ubiquitination.

Cite this article

Wilson, R., Goyal, L., Ditzel, M. et al. The DIAP1 RING finger mediates ubiquitination of Dronc and is indispensable for regulating apoptosis. Nat Cell Biol 4, 445–450 (2002). https://doi.org/10.1038/ncb799

View full text

>> Full Text:   The DIAP1 RING finger mediates ubiquitination of Dronc and is indispensable for regulating apoptosis

Reaper eliminates IAP proteins through stimulated IAP degradation and generalized translational inhi

Morgue mediates apoptosis in the Drosophila melanogaster retina by promoting degradation of DIAP1