Survival activity of Bcl-2 homologs Bcl-w and A1 only partially correlates with their ability to bind pro-apoptotic family members

Holmgreen, SP; Huang, DCS; Adams, JM; Cory, S

Author(s): Holmgreen, SP; Huang, DCS; Adams, JM; Cory, S;
Details: Publication Year 1999-06,Volume 6,Issue #6,Page 525-532
Journal Title: CELL DEATH AND DIFFERENTIATION
Publication Type: Journal Article
Abstract: Certain Bcl-2 family members promote cell survival, whereas others promote apoptosis, To explore further how heterodimerization of opposing members affects survival activity, we have compared the abilities of the anti-apoptotic Bcl-w and Al to bind to the pro-apoptotic Bax, Bak, Bad and Bik and to protect cells from their cytotoxic action. Bcl-w co-immunoprecipitated from cell lysates with Bax, Bak, Bad and Bik, but Al bound only Bak and Bik, Mutation of Al at a highly conserved glycine within the BH1 domain prevented binding, but the comparable Bcl-w mutant still bound Bak, Bad and Bik, indicating that the glycine is not essential for all heterodimerization, Bcl-w and Al protected against apoptosis induced by over-expression of Bax or Bad but not that induced by Bak or Bik, With several gene pairs, binding and protection were discordant. The results may reflect critical threshold affinities but also suggest that certain pro-apoptotic proteins may also contribute to apoptosis by a mechanism independent of binding pro-survival proteins.
Publisher: STOCKTON PRESS
Keywords: PROGRAMMED CELL-DEATH; BH3 DOMAIN; CYTOCHROME-C; X-L; SEQUENCE SIMILARITY; PROMOTING PROTEINS; GENE FAMILY; E1B 19K; BCL-X(L); INTERACTS
Publisher's Version: https://doi.org/10.1038/sj.cdd.4400519
Terms of Use/Rights Notice: Refer to copyright notice on published article.

Creation Date: 1999-06-01 12:00:00