Agios Pharmaceuticals, Cambridge, MA 02139-4169, USA.
Science. 2013 May 3;340(6132):622-6. doi: 10.1126/science.1234769. Epub 2013 Apr 4.
A number of human cancers harbor somatic point mutations in the genes encoding isocitrate dehydrogenases 1 and 2 (IDH1 and IDH2). These mutations alter residues in the enzyme active sites and confer a gain-of-function in cancer cells, resulting in the accumulation and secretion of the oncometabolite (R)-2-hydroxyglutarate (2HG). We developed a small molecule, AGI-6780, that potently and selectively inhibits the tumor-associated mutant IDH2/R140Q. A crystal structure of AGI-6780 complexed with IDH2/R140Q revealed that the inhibitor binds in an allosteric manner at the dimer interface. The results of steady-state enzymology analysis were consistent with allostery and slow-tight binding by AGI-6780. Treatment with AGI-6780 induced differentiation of TF-1 erythroleukemia and primary human acute myelogenous leukemia cells in vitro. These data provide proof-of-concept that inhibitors targeting mutant IDH2/R140Q could have potential applications as a differentiation therapy for cancer.
许多人类癌症在编码异柠檬酸脱氢酶 1 和 2(IDH1 和 IDH2)的基因中存在体细胞点突变。这些突变改变了酶活性部位的残基,并赋予癌细胞功能获得,导致致癌代谢物(R)-2-羟基戊二酸(2HG)的积累和分泌。我们开发了一种小分子 AGI-6780,它能够强效且选择性地抑制与肿瘤相关的突变 IDH2/R140Q。AGI-6780 与 IDH2/R140Q 复合物的晶体结构表明,抑制剂以变构方式结合在二聚体界面上。稳态酶学分析的结果与 AGI-6780 的变构和缓慢紧密结合一致。AGI-6780 的治疗诱导了体外 TF-1 红白血病和原发性人急性髓系白血病细胞的分化。这些数据提供了一个概念证明,靶向突变 IDH2/R140Q 的抑制剂可能作为癌症的分化治疗具有潜在的应用。
