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与临床化合物来司他替尼和托法替布复合的PRK1晶体结构揭示了配体诱导的构象变化。

Crystal structures of PRK1 in complex with the clinical compounds lestaurtinib and tofacitinib reveal ligand induced conformational changes.

作者信息

Chamberlain Philip, Delker Silvia, Pagarigan Barbra, Mahmoudi Afshin, Jackson Pilgrim, Abbasian Mahan, Muir Jeff, Raheja Neil, Cathers Brian

机构信息

Celgene Corporation, San Diego, California, United States of America; Department of Biochemistry and Structural Biology, Celgene Corporation, San Diego, California, United States of America.

Celgene Corporation, San Diego, California, United States of America.

出版信息

PLoS One. 2014 Aug 11;9(8):e103638. doi: 10.1371/journal.pone.0103638. eCollection 2014.

Abstract

Protein kinase C related kinase 1 (PRK1) is a component of Rho-GTPase, androgen receptor, histone demethylase and histone deacetylase signaling pathways implicated in prostate and ovarian cancer. Herein we describe the crystal structure of PRK1 in apo form, and also in complex with a panel of literature inhibitors including the clinical candidates lestaurtinib and tofacitinib, as well as the staurosporine analog Ro-31-8220. PRK1 is a member of the AGC-kinase class, and as such exhibits the characteristic regulatory sequence at the C-terminus of the catalytic domain--the 'C-tail'. The C-tail fully encircles the catalytic domain placing a phenylalanine in the ATP-binding site. Our inhibitor structures include examples of molecules which both interact with, and displace the C-tail from the active site. This information may assist in the design of inhibitors targeting both PRK and other members of the AGC kinase family.

摘要

蛋白激酶C相关激酶1(PRK1)是Rho-GTP酶、雄激素受体、组蛋白去甲基化酶和组蛋白脱乙酰酶信号通路的一个组成部分,这些信号通路与前列腺癌和卵巢癌有关。在此,我们描述了PRK1的无配体形式的晶体结构,以及与一组文献报道的抑制剂(包括临床候选药物来他替尼和托法替布,以及星形孢菌素类似物Ro-31-8220)形成的复合物的晶体结构。PRK1是AGC激酶家族的成员,因此在催化结构域的C末端呈现出特征性的调节序列——“C尾”。C尾完全环绕催化结构域,在ATP结合位点放置了一个苯丙氨酸。我们的抑制剂结构包括既与C尾相互作用又将其从活性位点置换的分子实例。这些信息可能有助于设计针对PRK以及AGC激酶家族其他成员的抑制剂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/afc4/4128815/2c68354324b0/pone.0103638.g001.jpg

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