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天然沙利度胺产物:强效 20S 蛋白酶体抑制剂,有望成为癌症化疗药物。

Salinosporamide natural products: Potent 20 S proteasome inhibitors as promising cancer chemotherapeutics.

机构信息

Kekulé-Institut für Organische Chemie und Biochemie, Rheinische Friedrich-Wilhelms-Universität Bonn, Gerhard-Domagk Strasse 1, 53121 Bonn, Deutschland.

出版信息

Angew Chem Int Ed Engl. 2010 Dec 3;49(49):9346-67. doi: 10.1002/anie.201000728.

Abstract

Proteasome inhibitors are rapidly evolving as potent treatment options in cancer therapy. One of the most promising drug candidates of this type is salinosporamide A from the bacterium Salinispora tropica. This marine natural product possesses a complex, densely functionalized γ-lactam-β-lactone pharmacophore, which is responsible for its irreversible binding to its target, the β subunit of the 20S proteasome. Salinosporamide A entered phase I clinical trials for the treatment of multiple myeloma only three years after its discovery. The strong biological activity and the challenging structure of this compound have fueled intense academic and industrial research in recent years, which has led to the development of more than ten syntheses, the elucidation of its biosynthetic pathway, and the generation of promising structure-activity relationships and oncological data. Salinosporamide A thus serves as an intriguing example of the successful interplay of modern drug discovery and biomedical research, medicinal chemistry and pharmacology, natural product synthesis and analysis, as well as biosynthesis and bioengineering.

摘要

蛋白酶体抑制剂在癌症治疗中迅速成为有效的治疗选择。这种类型最有前途的候选药物之一是来自海洋细菌盐单胞菌的盐诺司帕米 A。这种海洋天然产物具有复杂的、高度官能化的γ-内酰胺-β-内酰胺药效团,这使其能够不可逆地与靶标 20S 蛋白酶体的β亚基结合。盐诺司帕米 A 在发现后的三年内就进入了多发性骨髓瘤的 I 期临床试验。该化合物具有很强的生物活性和挑战性的结构,这激发了近年来学术界和工业界的大量研究,这些研究导致了十多种合成方法的发展、其生物合成途径的阐明,以及有前途的结构-活性关系和肿瘤学数据的产生。盐诺司帕米 A 因此成为现代药物发现和生物医学研究、药物化学和药理学、天然产物合成和分析以及生物合成和生物工程成功互动的一个有趣例子。

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