Department of Therapeutic Discovery, Amgen Inc., 1120 Veterans Boulevard, South San Francisco, California 94080, USA.
J Med Chem. 2012 Sep 13;55(17):7667-85. doi: 10.1021/jm300679u. Epub 2012 Aug 29.
Structure-based rational design led to the synthesis of a novel series of potent PI3K inhibitors. The optimized pyrrolopyridine analogue 63 was a potent and selective PI3Kβ/δ dual inhibitor that displayed suitable physicochemical properties and pharmacokinetic profile for animal studies. Analogue 63 was found to be efficacious in animal models of inflammation including a keyhole limpet hemocyanin (KLH) study and a collagen-induced arthritis (CIA) disease model of rheumatoid arthritis. These studies highlight the potential therapeutic value of inhibiting both the PI3Kβ and δ isoforms in the treatment of a number of inflammatory diseases.
基于结构的合理设计导致了一系列新型强效 PI3K 抑制剂的合成。优化的吡咯并吡啶类似物 63 是一种强效且选择性的 PI3Kβ/δ 双重抑制剂,具有适合动物研究的理化性质和药代动力学特征。研究发现类似物 63 在炎症动物模型中有效,包括血蓝蛋白 (KLH) 研究和类风湿关节炎胶原诱导关节炎 (CIA) 疾病模型。这些研究强调了抑制 PI3Kβ 和 δ 同工型在治疗多种炎症性疾病方面的潜在治疗价值。
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