变构调节
化学
对接(动物)
变构酶
小分子
虚拟筛选
激酶
结合位点
药物发现
计算生物学
生物化学
酶
生物
医学
护理部
作者
T.J. Rettenmaier,Hao Fan,Joel Karpiak,Allison K. Doak,Andrej Šali,Brian K. Shoichet,James A. Wells
标识
DOI:10.1021/acs.jmedchem.5b01216
摘要
Finding small molecules that target allosteric sites remains a grand challenge for ligand discovery. In the protein kinase field, only a handful of highly selective allosteric modulators have been found. Thus, more general methods are needed to discover allosteric modulators for additional kinases. Here, we use virtual screening against an ensemble of both crystal structures and comparative models to identify ligands for an allosteric peptide-binding site on the protein kinase PDK1 (the PIF pocket). We optimized these ligands through an analog-by-catalog search that yielded compound 4, which binds to PDK1 with 8 μM affinity. We confirmed the docking poses by determining a crystal structure of PDK1 in complex with 4. Because the PIF pocket appears to be a recurring structural feature of the kinase fold, known generally as the helix αC patch, this approach may enable the discovery of allosteric modulators for other kinases.
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