Discovery of a potent and selective ROMK inhibitor with improved pharmacokinetic properties based on an octahydropyrazino[2,1-c][1,4]oxazine scaffold

Yuping Zhu,Reynalda K. de Jesus,Haifeng Tang,Shawn P. Walsh,Jinlong Jiang,Xin Gu,Nardos Teumelsan,Aurash Shahripour,Barbara Pio,Fa-Xiang Ding,Sookhee Ha,Birgit T. Priest,Andrew M. Swensen,Magdalena Alonso-Galicia,John P. Felix,Richard M. Brochu,Timothy Bailey,Brande Thomas-Fowlkes,Xiaoyan Zhou,Lee-Yuh Pai,Caryn Hampton,Melba Hernandez,Karen Owens,Juliann Ehrhart,Sophie Roy,Gregory J. Kaczorowski,Lihu Yang,Emma R. Parmee,Kathleen A. Sullivan,Maria L. Garcia,Alexander Pasternak

Discovery of a potent and selective ROMK inhibitor with improved pharmacokinetic properties based on an octahydropyrazino[2,1-c][1,4]oxazine scaffold

2016

Abstract Following the discovery of small molecule acyl piperazine ROMK inhibitors, the acyl octahydropyrazino[2,1-c][1,4]oxazine series was identified. This series displays improved ROMK/hERG selectivity, and as a consequence, the resulting ROMK inhibitors do not evoke QTc prolongation in an in vivo cardiovascular dog model. Further efforts in this series led to the discovery of analogs with improved pharmacokinetic profiles. This new series also retained comparable ROMK potency compared to earlier leads.

Keywords:

hERG
Small molecule
QTC PROLONGATION
Piperazine
In vivo
ROMK
Pharmacology
Chemistry
Pharmacokinetics
dog model

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