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BH3 mimetics: Status of the field and new developments

机译:BH3模拟物:领域现状和新发展

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Targeting apoptosis is an attractive approach in cancer therapy. The BH3-only proteins of the BCL-2 family (having only the BCL-2 homologydomain BH3) can trigger apoptosis by binding to the prosurvival members of this family and neutralizing their functional activity (sequestration of the proapoptotic Bcl-2 family members). The "BH3 mimetic" concept has prompted the development of small molecules capable of mimicking BH3-only proteins and thus inducing apoptosis. The prototype BH3 mimetic ABT-737 selectively targets the three prosurvival proteins BCL-XL, BCL-2, and BCL-W (but not MCL-1 or A1) and its oral derivative ABT-263 has proved promising in clinical trials. Some putative BH3 mimetics are also tested clinically while others are still being characterized. This article recapitulates the various known BH3 mimetics and presents the recent developments in the field. The latter include (i) the identification of molecular determinants responsible for the specific interactions between BH3 motifs and the binding grooves of prosurvival proteins and (ii) the characterization of new compounds and particularly BH3 mimetics that antagonize either selectively MCL-1 or BCL-2 or a broad range of prosurvival proteins. These data are critical advances toward the discovery of novel anticancer agents.
机译:靶向凋亡是癌症治疗中的一种有吸引力的方法。 BCL-2家族的仅BH3蛋白(仅具有BCL-2同源结构域BH3)可以通过与该家族的生存成员结合并中和其功能活性(螯合促凋亡的Bcl-2家族成员)来触发凋亡。 “ BH3模拟物”的概念促使人们开发出能够模仿仅BH3蛋白的小分子,从而诱导细胞凋亡。原型BH3模拟物ABT-737选择性靶向三种生存蛋白BCL-XL,BCL-2和BCL-W(但不包括MCL-1或A1),并且其口服衍生物ABT-263在临床试验中被证明很有希望。一些推定的BH3模拟物也在临床上进行了测试,而其他一些仍在表征中。本文概述了各种已知的BH3模拟物,并介绍了该领域的最新进展。后者包括(i)鉴定负责BH3基序与存活蛋白结合槽之间特定相互作用的分子决定簇,以及(ii)表征选择性拮抗MCL-1或BCL-2的新化合物,尤其是BH3模拟物或广泛的生存蛋白。这些数据是发现新型抗癌药的关键进展。

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