Discovery and in Vitro Optimization of 3-Sulfamoylbenzamidesas ROMK Inhibitors

机译：3-氨磺酰基苯甲酰胺的发现和体外优化作为ROMK抑制剂

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摘要

Inhibitors of the renal outer medullary potassium channel (ROMK) show promise as novel mechanism diuretics, with potentially lower risk of diuretic-induced hypokalemia relative to current thiazide and loop diuretics. Here, we report the identification of a novel series of 3-sulfamoylbenzamide ROMK inhibitors. Starting from HTS hit >4, this series was optimized to provide ROMK inhibitors with good in vitro potencies and well-balanced ADME profiles. In contrast to previously reported small-molecule ROMK inhibitors, members of this series were demonstrated to be highly selective for inhibition of human over rat ROMK and to be insensitive to the N171D pore mutation that abolishes inhibitory activity of previously reported ROMK inhibitors.

机译：肾外髓质钾通道（ROMK）抑制剂有望作为新型机制利尿剂，与目前的噻嗪类和loop利尿剂相比，利尿剂引起的低钾血症的风险可能更低。在这里，我们报告鉴定的新型3-氨磺酰基苯甲酰胺ROMK抑制剂系列。从HTS第> 4 开始，对该系列进行了优化，以为ROMK抑制剂提供良好的体外效能和均衡的ADME谱。与先前报道的小分子ROMK抑制剂相反，该系列成员被证明对人类的抑制作用高于大鼠ROMK，并且对消除先前报道的ROMK抑制剂的抑制活性的N171D孔突变不敏感。

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期刊名称 ACS Medicinal Chemistry Letters
作者
Matthew F. Sammons; *; Sujay V. Kharade; *; Kevin J. Filipski; Markus Boehm; Aaron C. Smith; Andre Shavnya; Dilinie P. Fernando; ⊥; Matthew S. Dowling; Philip A. Carpino; Neil A. Castle; #; Shannon G. Zellmer; #; Brett M. Antonio; #; James R. Gosset; Anthony Carlo; Jerod S. Denton;
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年(卷),期 2018(9),2
年度 2018
页码 125–130
总页数 6
原文格式 PDF
正文语种
中图分类药物化学;
关键词
ROMK Kir1.1 potassium channel inhibitors diuretics hypertension;

机译：ROMK;Kir1.1;钾通道抑制剂;利尿剂;高血压;

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专利

1. Discovery and in Vitro Optimization of 3-Sulfamoylbenzamides as ROMK Inhibitors [J] . Sammons Matthew F., Kharade Sujay V., Filipski Kevin J., ACS medicinal chemistry letters . 2018,第2期

机译：3-磺酰苯甲酰苯胺的发现和体外优化作为romk抑制剂
2. In Vitro Pharmacokinetic Optimizations of AM2-S31N Channel Blockers Led to the Discovery of Slow-Binding Inhibitors with Potent Antiviral Activity against Drug-Resistant Influenza A Viruses [J] . Yuanxiang Wang, Yanmei Hu, Shuting Xu, Journal of Medicinal Chemistry . 2018,第3期

机译：体外药代动力学优化AM2-S31N通道阻断器导致对耐药性流感病毒的有效抗病毒活性的缓慢结合抑制剂的发现
3. Discovery of 4?Aryl?N?arylcarbonyl-2-aminothiazoles as Hec1/Nek2 Inhibitors. Part I: Optimization of in Vitro Potencies and Pharmacokinetic Properties [J] . Ying-Shuan E. Lee, Shih-Hsien Chuang, Lynn Y. L. Huang, Journal of Medicinal Chemistry . 2014,第10期

机译：发现作为Hec1 / Nek2抑制剂的4′芳基′N′芳基羰基-2-氨基噻唑。第一部分：体外效能和药代动力学特性的优化
4. Optimization of targeted therapies to inhibit smooth muscle cell invasion in vitro [C] . Kennedy, C.E., Massia, Engineering in Medicine and Biology Society, 2003. Proceedings of the 25th Annual International Conference of the IEEE . 2003

机译：优化靶向疗法以抑制体外平滑肌细胞侵袭
5. Computer-aided discovery of novel natural product inhibitors of receptor tyrosine kinases and their rational semisynthetic optimizations for multiple malignancies control. [D] . Mohyeldin, Mohamed M. 2016

机译：计算机辅助发现的受体酪氨酸激酶的新型天然产物抑制剂及其对多种恶性肿瘤的合理的半合成优化。
6. In Vitro Pharmacokinetic Optimizations of AM2-S31N Channel Blockers Led to the Discovery of Slow-Binding Inhibitors with Potent Antiviral Activity against Drug-Resistant Influenza A Viruses [O] . Yuanxiang Wang, Yanmei Hu, Shuting Xu, -1

机译：AM2-S31N通道阻滞剂的体外药代动力学优化可导致发现具有抗药性甲型流感病毒的强抗病毒活性的慢结合抑制剂
7. Discovery of MK-7145, an Oral Small Molecule ROMK Inhibitor for the Treatment of Hypertension and Heart Failure [O] . Haifeng Tang, Yuping Zhu, Nardos Teumelsan, 2016

机译：发现MK-7145，一种用于治疗高血压和心力衰竭的口服小分子ROMK抑制剂

Discovery and in Vitro Optimization of 3-Sulfamoylbenzamidesas ROMK Inhibitors

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