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Crystal structure of human cyclin-dependent kinase-2 complex with MK2 inhibitor TEI-I01800: insight into the selectivity

机译:具有MK2抑制剂TEI-I01800的人细胞周期蛋白依赖性激酶2复合物的晶体结构:洞察选择性

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摘要

Mitogen-activated protein kinase-activated protein kinase 2 (MK2 or MAPKAP-K2) is a Ser/Thr kinase from the p38 mitogen-activated protein kinase signalling pathway and plays an important role in inflammatory diseases. The crystal structure of the MK2–TEI- complex has been reported; its Gly-rich loop was found to form an α-helix, not a β-sheet as has been observed for other Ser/Thr kinases. TEI- is 177-fold selective against MK2 compared with CDK2; in order to understand the inhibitory mechanism of TEI-, the cyclin-dependent kinase 2 (CDK2) complex structure with TEI- was determined at 2.0 Å resolution. Interestingly, the Gly-rich loop of CDK2 formed a β-sheet that was different from that of MK2. In MK2, TEI- changed the secondary structure of the Gly-rich loop from a β-sheet to an α-helix by collision between Leu70 and a p-ethoxyphenyl group at the 7-position and bound to MK2. However, for CDK2, TEI- bound to CDK2 without this structural change and lost the interaction with the substituent at the 7-position. In summary, the results of this study suggest that the reason for the selectivity of TEI- is the favourable conformation of TEI- itself, making it suitable for binding to the α-form MK2.
机译:丝裂原激活的蛋白激酶激活的蛋白激酶2(MK2或MAPKAP-K2)是来自p38丝裂原激活的蛋白激酶信号传导途径的Ser / Thr激酶,在炎性疾病中起重要作用。已经报道了MK2-TEI-复合物的晶体结构。发现其富含Gly的环形成α-螺旋,而不是其他Ser / Thr激酶所观察到的β-折叠。与CDK2相比,TEI-对MK2的选择性高177倍;为了了解TEI-的抑制机理,确定了TEI-的细胞周期蛋白依赖性激酶2(CDK2)复杂结构的分辨率为2.0Å。有趣的是,CDK2的富含Gly的环形成了一个不同于MK2的β-折叠。在MK2中,TEI-通过Leu70与7位对乙氧基苯基之间的碰撞将富Gly环的二级结构从β-折叠变为α-螺旋,并与MK2结合。然而,对于CDK2,TEI-结合CDK2而没有这种结构变化并且失去了与7位取代基的相互作用。总之,这项研究的结果表明,TEI-选择性的原因是TEI-本身具有良好的构象,使其适合于与α型MK2结合。

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