Bax-derived membrane-active peptides act as potent and direct inducers of apoptosis in cancer cells.

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RESEARCH PRODUCT

Bax-derived membrane-active peptides act as potent and direct inducers of apoptosis in cancer cells.

Germain Gillet Juan G. Valero Yannis Guillemin Jean-luc Coll Julien Prudent Jérôme Kucharczak Jesus Salgado Lucie Sancey Abdel Aouacheria Diana Gimenez

subject

Apoptosis Mitochondrion Mice MESH: Protein Structure Tertiary 0302 clinical medicine Neoplasms genetics MESH: Animals MESH: Neoplasms bcl-2-Associated X Protein 0303 health sciences biology MESH: Peptides Cytochrome c apoptosis Cytochromes c MESH: Cytochromes c proapoptotic Bax Cell biology Mitochondria drug therapy mitochondria 030220 oncology & carcinogenesis Bacterial outer membrane Programmed cell death MESH: Cell Line Tumor MESH: Mitochondria Antineoplastic Agents [SDV.CAN]Life Sciences [q-bio]/Cancer pore-forming peptides chemistry Article 03 medical and health sciences Bcl-2-associated X protein Bcl-2 family Cell Line Tumor Animals Humans MESH: bcl-2-Associated X Protein MESH: Mice 030304 developmental biology MESH: Humans MESH: Apoptosis Bcl-2 family Cell Biology Protein Structure Tertiary anticancer agent antivascular therapy Apoptosis drug effects Cancer cell biology.protein MESH: Antineoplastic Agents pharmacology physiopathology Peptides metabolism

description

SUMMARYAlthough many cancer cells are primed for apoptosis, they usually develop resistance to cell death at multiple levels. Permeabilization of the outer mitochondrial membrane, which is mediated by proapoptotic Bcl-2 family members like Bax, is considered as a point-of-no-return for initiating apoptotic cell death. This crucial role has placed Bcl-2 family proteins as recurrent targets for anticancer drug development. Here, we propose and demonstrate a new concept based on using minimal active version of Bax to induce cell death independently of endogenous Bcl-2 proteins. We show that membrane-active segments of Bax can directly induce the release of mitochondria-residing apoptogenic factors and commit tumor cells promptly and irreversibly to caspase-dependent apoptosis. On this basis, we designed a peptide encompassing part of the Bax pore-forming domain, able to target mitochondria, induce cytochrome c release and trigger caspase-dependent apoptosis. Moreover, this Bax-derived poropeptide produced effective tumor regression after peritumoral injection in a nude mouse xenograft model. Thus, peptides derived from proteins evolutionary functionalized to form pores in the mitochondrial outer membrane represent novel templates for anticancer agents.

year	journal	country	edition	language
2011-02-15

10.1242/jcs.076745 https://www.hal.inserm.fr/inserm-00559538/file/ARTICLE_POROPEPTIDE_word_JCellSci3.pdf