RIKEN Systems and Structural Biology Center, 1-7-22 Suehiro-cho, Tsurumi, Yokohama 230-0045, Japan.
Expert Opin Drug Discov. 2012 Dec;7(12):1177-92. doi: 10.1517/17460441.2012.727394. Epub 2012 Sep 25.
Pim1 is a unique, constitutively active serine/threonine kinase, and is a potent oncogene overexpressed in a range of hematologic malignancies and solid cancers. It functions as a signaling regulator in cell proliferation and survival pathways through substrate phosphorylation. More than 400 small molecular Pim1 inhibitors with IC(50)/Ki < 10 μM have been registered in the ChEMBL. However, no drug targeting Pim1 has been launched at this present time.
The authors provide a review of Pim1 inhibitors from the viewpoint of the structural analysis of the Pim1-inhibitor complexes. PDB data and PubMed literature searches were performed. The inhibitors have been classified and summarized by their interactions with Pim1 residues, to facilitate desirable inhibitor design.
To obtain a potent and selective Pim1 inhibitor as a lead compound, the authors propose the development of compounds which simultaneously interact with both the ATP binding site (Lys67, Glu121 and Phe49) and substrate binding residues (Asp128, Asp131 and Glu171). The development of Pim1 inhibitors could lead to new therapeutic options for a number of hematological malignancies and prostate cancer in the future.
Pim1 是一种独特的、组成性激活的丝氨酸/苏氨酸激酶,在多种血液恶性肿瘤和实体瘤中过表达,是一种有效的癌基因。它通过底物磷酸化在细胞增殖和存活途径中作为信号调节剂发挥作用。在 ChEMBL 中已有超过 400 种小分子 Pim1 抑制剂的 IC(50)/Ki<10μM。然而,目前尚无针对 Pim1 的药物上市。
作者从 Pim1-抑制剂复合物的结构分析角度综述了 Pim1 抑制剂。进行了 PDB 数据和 PubMed 文献检索。根据抑制剂与 Pim1 残基的相互作用对抑制剂进行分类和总结,以促进理想的抑制剂设计。
为了获得作为先导化合物的有效且选择性的 Pim1 抑制剂,作者提出开发同时与 ATP 结合位点(Lys67、Glu121 和 Phe49)和底物结合残基(Asp128、Asp131 和 Glu171)相互作用的化合物。开发 Pim1 抑制剂可能会为未来的许多血液恶性肿瘤和前列腺癌提供新的治疗选择。
