Chen Lu, Du-Cuny Lei, Moses Sylvestor, Dumas Sabrina, Song Zuohe, Rezaeian Abdol Hossein, Lin Hui-Kuan, Meuillet Emmanuelle J, Zhang Shuxing
Department of Experimental Therapeutics, The University of Texas M. D. Anderson Cancer Center, Houston, Texas, United States of America.
Departments of Nutritional Sciences and Molecular and Cellular Biology, the University of Arizona Cancer Center, Tucson, Arizona, United States of America.
PLoS Comput Biol. 2015 Jan 8;11(1):e1004021. doi: 10.1371/journal.pcbi.1004021. eCollection 2015 Jan.
The Grb2-associated binding protein 1 (GAB1) integrates signals from different signaling pathways and is over-expressed in many cancers, therefore representing a new therapeutic target. In the present study, we aim to target the pleckstrin homology (PH) domain of GAB1 for cancer treatment. Using homology models we derived, high-throughput virtual screening of five million compounds resulted in five hits which exhibited strong binding affinities to GAB1 PH domain. Our prediction of ligand binding affinities is also in agreement with the experimental KD values. Furthermore, molecular dynamics studies showed that GAB1 PH domain underwent large conformational changes upon ligand binding. Moreover, these hits inhibited the phosphorylation of GAB1 and demonstrated potent, tumor-specific cytotoxicity against MDA-MB-231 and T47D breast cancer cell lines. This effort represents the discovery of first-in-class GAB1 PH domain inhibitors with potential for targeted breast cancer therapy and provides novel insights into structure-based approaches to targeting this protein.
Grb2相关结合蛋白1(GAB1)整合来自不同信号通路的信号,并且在许多癌症中过表达,因此代表了一个新的治疗靶点。在本研究中,我们旨在靶向GAB1的普列克底物蛋白同源(PH)结构域用于癌症治疗。利用我们推导的同源模型,对五百万种化合物进行高通量虚拟筛选,得到了五个与GAB1 PH结构域具有强结合亲和力的命中化合物。我们对配体结合亲和力的预测也与实验KD值一致。此外,分子动力学研究表明,GAB1 PH结构域在配体结合后发生了大的构象变化。此外,这些命中化合物抑制了GAB1的磷酸化,并对MDA-MB-231和T47D乳腺癌细胞系表现出强效的、肿瘤特异性的细胞毒性。这项工作代表了首个具有靶向乳腺癌治疗潜力的GAB1 PH结构域抑制剂的发现,并为基于结构的靶向该蛋白的方法提供了新的见解。
