Maibaum Jürgen, Stutz Stefan, Göschke Richard, Rigollier Pascal, Yamaguchi Yasuchika, Cumin Frédéric, Rahuel Joseph, Baum Hans-Peter, Cohen Nissim-Claude, Schnell Christian R, Fuhrer Walter, Gruetter Markus G, Schilling Walter, Wood Jeanette M
Novartis Institutes for BioMedical Research, NOVARTIS Pharma AG, WKL-136.683, CH-4002 Basel, Switzerland.
J Med Chem. 2007 Oct 4;50(20):4832-44. doi: 10.1021/jm070316i. Epub 2007 Sep 8.
Due to its function in the rate limiting initial step of the renin-angiotensin system, renin is a particularly promising target for drugs designed to control hypertension, a growing risk to health worldwide. Despite vast efforts over more than two decades, no orally efficacious renin inhibitor had reached the market. As a result of a structure-based topological design approach, we have identified a novel class of small-molecule inhibitors with good oral blood-pressure lowering effects in primates. Further lead optimization aimed for improvement of in vivo potency and duration of action, mainly by P2' modifications at the hydroxyethylene transition-state isostere. These efforts resulted in the discovery of aliskiren (46, CGP060536B, SPP100), a highly potent, selective inhibitor of renin, demonstrating excellent efficacy in sodium-depleted marmosets after oral administration, with sustained duration of action in reducing dose-dependently mean arterial blood pressure. Aliskiren has recently received regulatory approval by the U.S. Food and Drug Administration for the treatment of hypertension.
由于肾素在肾素 - 血管紧张素系统限速起始步骤中发挥作用,它是设计用于控制高血压药物的一个特别有前景的靶点,而高血压在全球范围内对健康构成的风险日益增加。尽管二十多年来付出了巨大努力,但尚无口服有效的肾素抑制剂上市。通过基于结构的拓扑设计方法,我们已确定了一类新型小分子抑制剂,它们在灵长类动物中具有良好的口服降血压效果。进一步的先导化合物优化旨在提高体内效力和作用持续时间,主要通过对羟乙烯过渡态电子等排体进行P2'修饰。这些努力促成了阿利吉仑(46,CGP060536B,SPP100)的发现,它是一种高效、选择性的肾素抑制剂,口服给药后在钠缺乏的狨猴中显示出优异疗效,在剂量依赖性降低平均动脉血压方面具有持续的作用时间。阿利吉仑最近已获得美国食品药品监督管理局的监管批准,用于治疗高血压。
