AI Article Synopsis
- Anti-apoptotic BCL-2 proteins prevent cell death by binding pro-apoptotic proteins, allowing cancer cells to evade treatment by overexpressing these anti-apoptotic proteins.
- Researchers are focusing on drugging the binding pockets of these proteins, with ABT-199 showing success in treating BCL-2-dependent cancers.
- New stapled BH3 peptides that target BFL-1, an anti-apoptotic protein involved in certain cancers, offer a promising therapeutic approach by irreversibly inhibiting it through covalent interactions.
Article Abstract
Anti-apoptotic BCL-2 family proteins block cell death by trapping the critical α-helical BH3 domains of pro-apoptotic members in a surface groove. Cancer cells hijack this survival mechanism by overexpressing a spectrum of anti-apoptotic members, mounting formidable apoptotic blockades that resist chemotherapeutic treatment. Drugging the BH3-binding pockets of anti-apoptotic proteins has become a highest-priority goal, fueled by the clinical success of ABT-199, a selective BCL-2 inhibitor, in reactivating apoptosis in BCL-2-dependent cancers. BFL-1 is a BCL-2 homolog implicated in melanoma, lymphoma, and other cancers, and remains undrugged. A natural juxtaposition of two unique cysteines at the binding interface of the NOXA BH3 helix and BFL-1 pocket informed the development of stapled BH3 peptides bearing acrylamide warheads to irreversibly inhibit BFL-1 by covalent targeting. Given the frequent proximity of native cysteines to regulatory binding surfaces, covalent stapled peptide inhibitors provide a new therapeutic strategy for targeting pathologic protein interactions.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5055752 | PMC |
| http://dx.doi.org/10.1016/j.chembiol.2016.07.022 | DOI Listing |
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