Department of Physics, Birzeit University, Birzeit, West Bank, Palestine.
McGovern Medical School, University of Texas Health Science Center at Houston, Department of Integrative Biology & Pharmacology, Houston, TX, United States.
Adv Protein Chem Struct Biol. 2020;122:181-202. doi: 10.1016/bs.apcsb.2020.05.003. Epub 2020 Jun 27.
Significant advances have been made toward discovering allosteric inhibitors for challenging drug targets such as the Ras family of membrane-associated signaling proteins. Malfunction of Ras proteins due to somatic mutations is associated with up to a quarter of all human cancers. Computational techniques have played critical roles in identifying and characterizing allosteric ligand-binding sites on these proteins, and to screen ligand libraries against those sites. These efforts, combined with a wide range of biophysical, structural, biochemical and cell biological experiments, are beginning to yield promising inhibitors to treat malignancies associated with mutated Ras proteins. In this chapter, we discuss some of these developments and how the lessons learned from Ras might be applied to similar other challenging drug targets.
在发现变构抑制剂方面取得了重大进展,这些抑制剂针对的是具有挑战性的药物靶点,如 Ras 家族的膜相关信号蛋白。由于体细胞突变导致 Ras 蛋白功能失调与多达四分之一的人类癌症有关。计算技术在确定和描述这些蛋白质上的变构配体结合位点方面发挥了关键作用,并针对这些位点筛选配体文库。这些努力,结合广泛的生物物理、结构、生化和细胞生物学实验,开始产生有希望的抑制剂来治疗与突变 Ras 蛋白相关的恶性肿瘤。在本章中,我们讨论了其中的一些进展,以及从 Ras 中吸取的经验教训如何应用于类似的其他具有挑战性的药物靶点。
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