Decoding and unlocking the BCL-2 dependency of cancer cells

被引:0
|
作者
Philippe Juin
Olivier Geneste
Fabien Gautier
Stéphane Depil
Mario Campone
机构
[1] Team 8 “Cell survival and tumor escape in breast cancer”,
[2] UMR 892 INSERM / 6299 CNRS / Université de Nantes,undefined
[3] Institut de Recherche Thérapeutique de l'Université de Nantes,undefined
[4] Institut de Cancérologie de l'Ouest (ICO),undefined
[5] Centre de Lutte contre le Cancer René Gauducheau,undefined
[6] Institut de Recherche Servier,undefined
[7] Cancer Research and Drug Discovery,undefined
来源
Nature Reviews Cancer | 2013年 / 13卷
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摘要
The balance between pro- and anti-apoptotic activities of BCL-2 family members is tipped towards survival in many cancer cells, thus allowing them to survive various stressful environments, tumour stress phenotypes and/or oncogene-induced death signals.As death signals may persist during tumour progression, cancer cells may be addicted to these survival mechanisms and be in a state of dependence on 'BCL-2-like' (BCL-2L) anti-apoptotic proteins.Survival of 'BCL-2L-dependent' cancer cells relies on the maintenance of protein–protein complexes in which the BH3 domain of some pro-apoptotic BCL-2 family members engages a hydrophobic groove at the surface of anti-apoptotic BCL-2L proteins.Structural characterization of the BH3-binding interface of anti-apoptotic BCL-2L proteins has led to the identification of small-molecule BH3 mimetics that disrupt key interactions and promote cancer cell apoptosis by on-target effects.A dual BCL-2 and BCL-XL inhibitor and a specific BCL-2 inhibitor have shown clinical activity in haematological malignancies. The dual inhibitor induces dose-limiting thrombocytopenia owing to BCL-XL inhibition.Finely-tuned inhibition of BCL-XL and of MCL1 in cancer cells by new and selective drugs remains a challenge and a necessity.Understanding the exact effects of inhibitors on endogenous (membrane-localized) complexes, identifying predictive biomarkers for drug efficacy and circumscribing the global biological effects of these compounds is also required.
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页码:455 / 465
页数:10
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