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Discovery of MK-7145 an Oral Small Molecule ROMKInhibitor for the Treatment of Hypertension and Heart Failure

机译:发现口服小分子ROMK MK-7145用于治疗高血压和心力衰竭的抑制剂

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摘要

ROMK, the renal outer medullary potassium channel, is involved in potassium recycling at the thick ascending loop of Henle and potassium secretion at the cortical collecting duct in the kidney nephron. Because of this dual site of action, selective inhibitors of ROMK are expected to represent a new class of diureticsatriuretics with superior efficacy and reduced urinary loss of potassium compared to standard-of-care loop and thiazide diuretics. Following our earlier work, this communication will detail subsequent medicinal chemistry endeavors to further improve lead selectivity against the hERG channel and preclinical pharmacokinetic properties. Pharmacological assessment of highlighted inhibitors will be described, including pharmacodynamic studies in both an acute rat diuresisatriuresis model and a subchronic blood pressure model in spontaneous hypertensive rats. These proof-of-biology studies established for the first time that the human and rodent genetics accurately predict the in vivo pharmacology of ROMK inhibitors and supported identification of the first small molecule ROMK inhibitor clinicalcandidate, MK-7145.
机译:ROMK是肾脏的外部髓质钾通道,参与了在Henle的厚上升环处的钾循环以及在肾脏的肾单位皮质收集管中的钾分泌。由于这种双重作用,与护理标准环和噻嗪类利尿剂相比,ROMK的选择性抑制剂有望代表一类新型的利尿剂/利尿剂,具有更高的功效并减少钾的尿流失。在我们的早期工作之后,本交流将详细介绍随后的药物化学工作,以进一步提高针对hERG通道的铅选择性和临床前药代动力学特性。将描述突出显示的抑制剂的药理评估,包括在自发性高血压大鼠的急性大鼠利尿/利尿模型和亚慢性血压模型中的药效学研究。这些生物学证明研究首次确定了人类和啮齿动物的遗传学能够准确预测ROMK抑制剂的体内药理作用,并支持鉴定首个临床上的小分子ROMK抑制剂候选人,MK-7145。

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