| Literature DB >> 32413285 |
Edward P Harvey1, Zachary J Hauseman1, Daniel T Cohen1, T Justin Rettenmaier2, Susan Lee1, Annissa J Huhn1, Thomas E Wales3, Hyuk-Soo Seo4, James Luccarelli1, Catherine E Newman1, Rachel M Guerra1, Gregory H Bird1, Sirano Dhe-Paganon4, John R Engen3, James A Wells2, Loren D Walensky5.
Abstract
The BCL-2 family is composed of anti- and pro-apoptotic members that respectively protect or disrupt mitochondrial integrity. Anti-apoptotic overexpression can promote oncogenesis by trapping the BCL-2 homology 3 (BH3) "killer domains" of pro-apoptotic proteins in a surface groove, blocking apoptosis. Groove inhibitors, such as the relatively large BCL-2 drug venetoclax (868 Da), have emerged as cancer therapies. BFL-1 remains an undrugged oncogenic protein and can cause venetoclax resistance. Having identified a unique C55 residue in the BFL-1 groove, we performed a disulfide tethering screen to determine if C55 reactivity could enable smaller molecules to block BFL-1's BH3-binding functionality. We found that a disulfide-bearing N-acetyltryptophan analog (304 Da adduct) effectively targeted BFL-1 C55 and reversed BFL-1-mediated suppression of mitochondrial apoptosis. Structural analyses implicated the conserved leucine-binding pocket of BFL-1 as the interaction site, resulting in conformational remodeling. Thus, therapeutic targeting of BFL-1 may be achievable through the design of small, cysteine-reactive drugs.Entities:
Keywords: BCL-2 family; BFL-1/A1; BH3; anti-apoptotic; apoptosis; cancer; covalent inhibitor; disulfide tethering; mitochondria; small molecule
Mesh:
Substances:
Year: 2020 PMID: 32413285 PMCID: PMC7405809 DOI: 10.1016/j.chembiol.2020.04.004
Source DB: PubMed Journal: Cell Chem Biol ISSN: 2451-9448 Impact factor: 8.116