Discovery of SPH3127: A Novel, Highly Potent, and Orally Active Direct Renin Inhibitor.
Daisuke IijimaHiroshi SugamaYoichi TakahashiMiki HiraiYuko TogashiJianshu XieJingkang ShenYing KeHidenori AkatsukaTakayuki KawaguchiKei TakedomiAkiko KashimaMasashi NishioYosuke InuiHikaru YonedaGuangxin XiaToru IijimaPublished in: Journal of medicinal chemistry (2022)
Renin is the rate-limiting enzyme in the renin-angiotensin-aldosterone system (RAAS) which regulates blood pressure and renal function and hence is an attractive target for the treatment of hypertension and cardiovascular/renal diseases. However, the development of direct renin inhibitors (DRIs) with favorable oral bioavailability has been a longstanding challenge for many years. This problem was thought to be because most of the reported DRIs were peptide-like structures or nonpeptide-like structures with a molecular weight (MW) of > 600. Therefore, we tried to find nonpeptidomimetic DRIs with a MW of < 500 and discovered the promising 2-carbamoyl morpholine derivative 4 . In our efforts to improve the pharmacokinetic profile of 4 without a significant increase in the MW, we discovered compound 18 (SPH3127), which demonstrated higher bioavailability and a more potent antihypertensive effect in preclinical models than aliskiren and has completed a phase II clinical trial for essential hypertension.
Keyphrases
- blood pressure
- phase ii
- angiotensin converting enzyme
- clinical trial
- angiotensin ii
- hypertensive patients
- open label
- heart rate
- high resolution
- small molecule
- double blind
- study protocol
- stem cells
- phase iii
- blood glucose
- type diabetes
- randomized controlled trial
- placebo controlled
- cell therapy
- quality improvement
- high throughput
- single cell
- replacement therapy