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Discovery and hit-to-lead evaluation of piperazine amides as selective state-dependent NaV1.7 inhibitors

机译：哌嗪酰胺作为选择性依赖状态的NaV1.7抑制剂的发现和领先优势评估

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NaV1.7 is a particularly compelling target for the treatment of pain. Herein, we report the discovery and evaluation of a series of piperazine amides that exhibit state-dependent inhibition of NaV1.7. After demonstrating significant pharmacodynamic activity with early lead compound >14 in a NaV1.7-dependent behavioural mouse model, we systematically established SAR trends throughout each sector of the scaffold. The information gleaned from this modular analysis was then applied additively to quickly access analogues that encompass an optimal balance of properties, including NaV1.7 potency, selectivity over NaV1.5, aqueous solubility, and microsomal stability.

机译：NaV1.7是治疗疼痛特别引人注目的靶标。在这里，我们报告发现和评估一系列显示NaV1.7的状态依赖性抑制的哌嗪酰胺。在依赖NaV1.7的行为小鼠模型中证明了早期铅化合物> 14 具有显着的药代动力学活性后，我们系统地建立了支架各个部分的SAR趋势。然后将从该模块化分析中收集的信息相加，以快速访问类似物，这些类似物具有最佳的性能平衡，包括NaV1.7效能，对NaV1.5的选择性，水溶性和微粒体稳定性。

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期刊名称 MedChemComm
作者
Brian A. Sparling; S. Yi; J. Able; H. Bregman; Erin F. DiMauro; R. S. Foti; H. Gao; A. Guzman-Perez; H. Huang; M. Jarosh; T. Kornecook; J. Ligutti; B. C. Milgram; B. D. Moyer; B. Youngblood; V. L. Yu; M. M. Weiss;
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年(卷),期 2017(8),4
年度 2017
页码 744–754
总页数 11
原文格式 PDF
正文语种
中图分类分子生物学;药物化学;
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专利

1. Discovery and hit-to-lead evaluation of piperazine amides as selective, state-dependent Na_V1.7 inhibitors [J] . Brian A. Sparling, S. Yi, J. Able, MedChemComm . 2017,第4期

机译：对哌嗪酰胺作为选择性，状态依赖性NA_V1.7抑制剂的发现和击中铅评估
2. Synthesis and Evaluation of (4-Chlorobenzhydryl) Piperazine Amides as Sodium Channel Nav1.7 Inhibitors [J] . Back Seung Keun, Kam Yoo Lim, Oh Jung Ae, Bulletin of the Korean Chemical Society . 2015,第9期

机译：钠通道Nav1.7抑制剂（4-氯联苯甲基）哌嗪酰胺的合成与评价
3. The discovery of azetidine-piperazine di -amides as potent, selective and reversible monoacylglycerol lipase (MAGL) inhibitors [J] . Zhu Bin, Connolly Peter J., Zhang Yue-Mei, Bioorganic and Medicinal Chemistry Letters . 2020,第14期

机译：将氮丁胺 - 哌嗪二 - 酰胺的发现为有效，选择性和可逆的单酰基甘油脂肪酶（Mag1）抑制剂
4. Fabrication of a poly(piperazine-amide)/polysulfone hollow fiber membrane for effective removal of heavy metals in industrial wastewater [C] . Kexiang Zhao International Conference on BioMedical Engineering and Informatics . 2014

机译：聚（哌嗪酰胺）/聚砜中空纤维膜的制备，可有效去除工业废水中的重金属
5. Application of organocatalysis to the synthesis of chiral morpholines, piperazines, aziridines, azetidines, beta-fluoroamines, and gamma-fluoroamines; discovery of selective phospholipase D inhibitors with optimized in vivo properties. [D] . O'Reilly, Matthew C. 2014

机译：有机催化在合成手性吗啉，哌嗪，氮丙啶，氮杂环丁烷，β-氟胺和γ-氟胺中的应用；发现具有优化体内特性的选择性磷脂酶D抑制剂。
6. Pharmacological characterization of a novel potent selective and orally active fatty acid amide hydrolase inhibitor PKM‐833 (R)‐N‐(pyridazin‐3‐yl)‐4‐(7‐(trifluoromethyl)chroman‐4‐yl)piperazine‐1‐carboxamide in rats: Potential for the treatment of inflammatory pain [O] . Toshiya Endo, Takashi Takeuchi, Shunsuke Maehara 2020

机译：一种新型有效选择性和口服活性的脂肪酸酰胺水解酶抑制剂PKM-833 （R）-N-（哒嗪-3-基）-4-（7-（三氟甲基）苯并吡喃-4-基的药理特性）大鼠中的哌嗪-1羧酰胺：治疗炎性疼痛的潜力
7. Discovery of a Selective, State-Independent Inhibitor of NaV1.7 by Modification of Guanidinium Toxins [O] . H Pajouhesh, JT Beckley, A Delwig, 2019

机译：通过修饰胍毒素的改性，发现选择性状态无关抑制剂NAV1.7

Discovery and hit-to-lead evaluation of piperazine amides as selective state-dependent NaV1.7 inhibitors

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