Identification of a potent, state-dependent inhibitor of Nav1.7 with oral efficacy in the formalin model of persistent pain

Bregman H.; Berry L.; Buchanan J.L.; Chen A.; Du B.; Feric E.; Hierl M.; Huang L.; Immke D.; Janosky B.; Johnson D.; Li X.; Ligutti J.; Liu D.; Malmberg A.; Matson D.; McDermott J.; Miu P.; Nguyen H.N.; Patel V.F.; Waldon D.; Wilenkin B.; Zheng X.M.; Zou A.; McDonough S.I.; Dimauro E.F.

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Identification of a potent, state-dependent inhibitor of Nav1.7 with oral efficacy in the formalin model of persistent pain

机译：在持续性疼痛的福尔马林模型中鉴定出具有口服药效的有效，状态依赖的Nav1.7抑制剂

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Clinical human genetic studies have recently identified the tetrodotoxin (TTX) sensitive neuronal voltage gated sodium channel Nav1.7 (SCN9A) as a critical mediator of pain sensitization. Herein, we report structure-activity relationships for a novel series of 2,4-diaminotriazines that inhibit hNav1.7. Optimization efforts culminated in compound 52, which demonstrated pharmacokinetic properties appropriate for in vivo testing in rats. The binding site of compound 52 on Nav1.7 was determined to be distinct from that of local anesthetics. Compound 52 inhibited tetrodotoxin-sensitive sodium channels recorded from rat sensory neurons and exhibited modest selectivity against the hERG potassium channel and against cloned and native tetrodotoxin-resistant sodium channels. Upon oral administration to rats, compound 52 produced dose- and exposure-dependent efficacy in the formalin model of pain.

机译：临床人类遗传学研究最近确定了河豚毒素（TTX）敏感的神经元电压门控钠通道Nav1.7（SCN9A）是疼痛敏化的关键介质。在这里，我们报告抑制hNav1.7的2,4-二氨基三嗪系列的新型结构-活性关系。优化工作达到了化合物52的最高水平，化合物52具有适合大鼠体内测试的药代动力学特性。确定了Nav1.7上化合物52的结合位点与局麻药不同。化合物52抑制了从大鼠感觉神经元记录的河豚毒素敏感性钠通道，并且对hERG钾通道以及对克隆的和天然的河豚毒素抗性钠通道表现出适度的选择性。口服给予大鼠后，化合物52在福尔马林疼痛模型中产生剂量依赖性和暴露依赖性的功效。

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《Journal of Medicinal Chemistry 》 |2011年第13期| 共19页
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Bregman H.; Berry L.; Buchanan J.L.; Chen A.; Du B.; Feric E.; Hierl M.; Huang L.; Immke D.; Janosky B.; Johnson D.; Li X.; Ligutti J.; Liu D.; Malmberg A.; Matson D.; McDermott J.; Miu P.; Nguyen H.N.; Patel V.F.; Waldon D.; Wilenkin B.; Zheng X.M.; Zou A.; McDonough S.I.; Dimauro E.F.;
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1. Identification of a potent, state-dependent inhibitor of Nav1.7 with oral efficacy in the formalin model of persistent pain [J] . Bregman H., Berry L., Buchanan J.L., Journal of Medicinal Chemistry . 2011 ,第13期

机译：在持续性疼痛的福尔马林模型中鉴定出具有口服药效的有效，状态依赖的Nav1.7抑制剂
2. Discovery of dual inducibleeuronal nitric oxide synthase (iNOSNOS) inhibitor development candidate 4-((2-cyclobutyl-1 H-imidazo[4,5- b ]pyrazin-1-yl)methyl)-7,8-difluoroquinolin-2(1 H)-one (KD7332) Part 2: Identification of a novel, potent, and selective series of benzimidazole- quinolinone iNOSNOS dimerization inhibitors that are orally active in pain models [J] . Payne J.E., Bonnefous C., Symons K.T., Journal of Medicinal Chemistry . 2010 ,第21期

机译：发现双诱导/神经型一氧化氮合酶（iNOS / nNOS）抑制剂开发候选4-（（2-环丁基-1 H-咪唑并[4,5-b]吡嗪-1-基）甲基）-7,8-二氟喹啉-2（1 H）-one（KD7332）第2部分：鉴定在疼痛模型中具有口服活性的新型，有效和选择性系列的苯并咪唑-喹啉酮iNOS / nNOS二聚抑制剂
3. Discovery of Inducible Nitric Oxide Synthase (iNOS) Inhibitor Development Candidate KD7332, Part 1: Identification of a Novel, Potent, and Selective Series of Quinolinone iNOS Dimerization Inhibitors that are Orally Active in Rodent Pain Models [J] . Bonnefous C, Payne JE, Roppe J, Journal of Medicinal Chemistry . 2009 ,第9期

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Identification of a potent, state-dependent inhibitor of Nav1.7 with oral efficacy in the formalin model of persistent pain

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