摘要
蛋白激酶是多功能的分子开关,控制信号转导网络中的功能过程,并调节细胞周期和生物体发育的基本生物过程。生物信息的不断增长和对蛋白激酶基因的结构,遗传和药理学研究的显着呼吸已经显着提高了我们对于激酶调节和信号级联中的相互作用的激酶活化,药物结合和变构机制的知识。结构和生物化学蛋白激酶与抑制剂结合的遗传学和分子决定因素的研究一直是临床肿瘤学药物发现努力的基石,导致有效的抗癌疗法的增殖。最近在理解蛋白激酶变构调节方面的进展已经引起了前所未有的努力,旨在发现能够对抗癌症突变体的靶向和变构激酶抑制剂,并且在精确药物肿瘤学倡议的最前沿。尽管激酶功能背后的监管情况多样化,二聚化驱动的激活是许多蛋白激酶家族共同的变构调节的常见机制,最显着的是在生长因子信号传导和人类疾病中发挥核心作用的ErbB和BRAF激酶。在这篇综述中,我们重点关注了ErbB和BRAF激酶的结构,生物化学和计算研究,并讨论了激酶抑制剂的设计和发现如何利用这些激酶基因的结构景观多样性和调控的二聚化依赖机制和激酶活化的变构调节剂。从这个分析的教训可以通知发现特定的靶向疗法和强大的药物组合治疗癌症。
关键词: ErbB激酶,BRAF激酶,二聚化诱导的激酶活化,BRAF自相矛盾激活,变构调节,变构激酶抑制剂,蛋白激酶计算模型,多尺度模拟,激酶残基相互作用网络。
Current Medicinal Chemistry
Title:Leveraging Structural Diversity and Allosteric Regulatory Mechanisms of Protein Kinases in the Discovery of Small Molecule Inhibitors
Volume: 24 Issue: 42
关键词: ErbB激酶,BRAF激酶,二聚化诱导的激酶活化,BRAF自相矛盾激活,变构调节,变构激酶抑制剂,蛋白激酶计算模型,多尺度模拟,激酶残基相互作用网络。
摘要: Protein kinases are versatile molecule switches that govern functional processes in signal transduction networks and regulate fundamental biological processes of cell cycle and organism development. The continuous growth of biological information and a remarkable breath of structural, genetic, and pharmacological studies on protein kinase genes have significantly advanced our knowledge of the kinase activation, drug binding and allosteric mechanisms underlying kinase regulation and interactions in signaling cascades.. Structural and biochemical studies of the genetic and molecular determinants of protein kinases binding with inhibitors have been the cornerstone of drug discovery efforts in clinical oncology leading to proliferation of effective anticancer therapies. Recent advances in understanding allosteric regulation of protein kinases have fueled unprecedented efforts aiming in the discovery of targeted and allosteric kinase inhibitors that can combat cancer mutants and are at the forefront of the precision medicine initiative in oncology. Despite diversity of regulatory scenarios underlying kinase functions, dimerization-driven activation is a common mechanism of allosteric regulation that is shared by many protein kinase families, most notably ErbB and BRAF kinases that play a central role in growth factor signaling and human disease. In this review, we focused on structural, biochemical and computational studies of the ErbB and BRAF kinases and discuss how diversity of the structural landscape for these kinase genes and dimerization- dependent mechanisms of their regulation can be leveraged in the design and discovery of kinase inhibitors and allosteric modulators of kinase activation. The lessons from this analysis could inform discovery of specific targeted therapies and robust drug combinations for cancer treatment.
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Cite this article as:
Leveraging Structural Diversity and Allosteric Regulatory Mechanisms of Protein Kinases in the Discovery of Small Molecule Inhibitors, Current Medicinal Chemistry 2017; 24 (42) . https://dx.doi.org/10.2174/0929867323666161006113418
DOI https://dx.doi.org/10.2174/0929867323666161006113418 |
Print ISSN 0929-8673 |
Publisher Name Bentham Science Publisher |
Online ISSN 1875-533X |
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