Departments of †Discovery Chemistry, ‡Neurosciences, §Biochemical and Cellular Pharmacology, ∥Drug Metabolism and Pharmacokinetics, ⊥Safety Assessment, and #Structural Biology, Genentech, Inc. , 1 DNA Way, South San Francisco, California 94080, United States.
J Med Chem. 2014 Feb 13;57(3):921-36. doi: 10.1021/jm401654j. Epub 2014 Jan 15.
Leucine-rich repeat kinase 2 (LRRK2) has drawn significant interest in the neuroscience research community because it is one of the most compelling targets for a potential disease-modifying Parkinson's disease therapy. Herein, we disclose structurally diverse small molecule inhibitors suitable for assessing the implications of sustained in vivo LRRK2 inhibition. Using previously reported aminopyrazole 2 as a lead molecule, we were able to engineer structural modifications in the solvent-exposed region of the ATP-binding site that significantly improve human hepatocyte stability, rat free brain exposure, and CYP inhibition and induction liabilities. Disciplined application of established optimal CNS design parameters culminated in the rapid identification of GNE-0877 (11) and GNE-9605 (20) as highly potent and selective LRRK2 inhibitors. The demonstrated metabolic stability, brain penetration across multiple species, and selectivity of these inhibitors support their use in preclinical efficacy and safety studies.
富含亮氨酸重复激酶 2(LRRK2)在神经科学研究领域引起了极大的关注,因为它是最有前途的潜在帕金森病治疗靶点之一。在此,我们披露了结构多样的小分子抑制剂,这些抑制剂适合评估持续体内 LRRK2 抑制的影响。我们使用先前报道的氨基吡唑 2 作为先导分子,能够对 ATP 结合位点的溶剂暴露区域进行结构修饰,这显著提高了人肝细胞稳定性、大鼠游离脑暴露以及 CYP 抑制和诱导的风险。严格应用既定的最佳中枢神经系统设计参数,最终快速鉴定出 GNE-0877(11)和 GNE-9605(20)作为高效且选择性的 LRRK2 抑制剂。这些抑制剂的代谢稳定性、在多种物种中的脑穿透性和选择性表明它们可用于临床前疗效和安全性研究。
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