A Gated Hydrophobic Funnel Within BAX Binds Long-chain Alkenals to Potentiate Pro-apoptotic Function

Overview

Journal bioRxiv

Date 2025 Jan 7

PMID 39763924

Authors

Jesse D Gelles

Yiyang Chen

Mark P A Luna-Vargas

Ariele Viacava Follis

Stella G Bayiokos

Jarvier N Mohammed

Tara M Sebastian

M Abdullah Al Noman

Ngoc Dung Pham

Yi Shi

Richard W Kriwacki

Jerry E Chipuk

Affiliations

Soon will be listed here.

Abstract

Mitochondria maintain a biochemical environment that cooperates with BH3-only proteins (e.g., BIM) to potentiate BAX activation, the key event to initiate physiological and pharmacological forms of apoptosis. The sphingosine-1-phosphate metabolite 2-trans-hexadecenal (2t-hexadecenal) is one such component described to support BAX activation, but molecular mechanisms remain largely unknown. Here, we utilize complementary biochemical and biophysical techniques to reveal that 2t-hexadecenal non-covalently interacts with BAX, and cooperates with BIM to stimulate early-activation steps of monomeric BAX. Integrated structural and computational approaches reveal 2t-hexadecenal binds an undefined region - a hydrophobic cavity formed by core-facing residues of α5, α6, and gated by α8 - we now term the "BAX actuating funnel" (BAF). We define alkenal length and α8 mobility as critical determinants for 2t-hexadecenal synergy with BIM and BAX, and demonstrate that proline 168 allosterically regulates BAF function. Collectively, this work imparts detailed molecular insights advancing our fundamental knowledge of BAX regulation and identifies a regulatory region with implications for biological and therapeutic opportunities.

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