BH3 Domains other than Bim and Bid Can Directly Activate Bax/Bak

Blanca Schafer,Jerry E. Chipuk,Tomomi Kuwana,Tudor Moldoveanu,Jacob Wolf,Han Du

doi:10.1074/jbc.m110.167148

Blanca Schafer, Jerry E. Chipuk

Open Access

https://doi.org/10.1074/jbc.m110.167148

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Abstract

Bcl-2 family proteins regulate a critical step in apoptosis referred to as mitochondrial outer membrane permeabilization (MOMP). Members of a subgroup of the Bcl-2 family, known as the BH3-only proteins, activate pro-apoptotic effectors (Bax and Bak) to initiate MOMP. They do so by neutralizing pro-survival Bcl-2 proteins and/or directly activating Bax/Bak. Bim and Bid are reported to be direct activators; however, here we show that BH3 peptides other than Bim and Bid exhibited various degrees of direct activation of the effector Bax or Bak, including Bmf and Noxa BH3s. In the absence of potent direct activators, such as Bim and Bid, we unmasked novel direct activator BH3 ligands capable of inducing effector-mediated cytochrome c release and liposome permeabilization, even when both Bcl-xL- and Mcl-1-type anti-apoptotic proteins were inhibited. The ability of these weaker direct activator BH3 peptides to cause MOMP correlated with that of the corresponding full-length proteins to induce apoptosis in the absence of Bim and Bid. We propose that, in certain contexts, direct activation by BH3-only proteins other than Bim and Bid may significantly contribute to MOMP and apoptosis.

Highlights

We found that Bim and Bid BH3 peptides are the most effective direct activators, promoting Baxmediated membrane permeabilization, and that all BH3 peptides acted as de-repressors, or sensitizers, contributing to mitochondrial outer membrane permeabilization (MOMP) by stably binding to and inhibiting the anti-apoptotic members [22]
We propose that direct activation is not an all-or-none phenomenon, but most BH3-only proteins possess this activity in various degrees
Our analysis suggests a hierarchy of direct activation based on the activities of the BH3 regions in isolation with Bim and Bid, followed by Bmf and Noxa, Puma, Bik, and Hrk, and Bad

Summary

Introduction

It has been shown that certain BH3-only proteins displace activator BH3-only proteins (Bim, cleaved Bid or Puma in some instances) from anti-apoptotic proteins, which will directly activate Bax/Bak. We investigated the membrane permeabilization by Bcl-2 family proteins in a defined liposome system, using BH3 peptides [13, 22]. Immunoblotting for Bcl-2 Family Proteins—MEFs or digitonin-permeabilized cell pellets (25 ␮g protein) were loaded onto 12% SDS-PAGE gels and transferred to nitrocellulose membrane for immunoblotting using antibodies against Bcl-2 family members; anti-Bcl-2 (Santa Cruz Biotechnology, sc23960 and BD, 554087), anti-Bcl-xL (Santa Cruz Biotechnology, sc-8392), anti-Bcl-w (Calbiochem, 197209), anti-Mcl-1 (Rockland, 600-401-394), anti-Bax (Santa Cruz Biotechnology, sc-493), anti-Bak (Upstate, 06 –536), anti-Bid (R & D, AF860), anti-Bmf (Lifespan, LS-C4126), and anti-Bim

Results

Conclusion