Vollum Institute, Oregon Health and Science University, 3181 SW Sam Jackson Park Road, Portland, OR, 97239, USA.
Medicinal Chemistry Core, Oregon Health and Science University, 3181 SW Sam Jackson Park Road, Portland, OR, 97239, USA.
ChemMedChem. 2019 Oct 17;14(20):1771-1782. doi: 10.1002/cmdc.201900376. Epub 2019 Sep 25.
Excessive mitochondrial matrix Ca and oxidative stress leads to the opening of a high-conductance channel of the inner mitochondrial membrane referred to as the mitochondrial permeability transition pore (mtPTP). Because mtPTP opening can lead to cell death under diverse pathophysiological conditions, inhibitors of mtPTP are potential therapeutics for various human diseases. High throughput screening efforts led to the identification of a 3-carboxamide-5-phenol-isoxazole compounds as mtPTP inhibitors. While they showed nanomolar potency against mtPTP, they exhibited poor plasma stability, precluding their use in in vivo studies. Herein, we describe a series of structurally related analogues in which the core isoxazole was replaced with a triazole, which resulted in an improvement in plasma stability. These analogues were readily generated using the copper-catalyzed "click chemistry". One analogue, N-(5-chloro-2-methylphenyl)-1-(4-fluoro-3-hydroxyphenyl)-1H-1,2,3-triazole-4-carboxamide (TR001), was efficacious in a zebrafish model of muscular dystrophy that results from mtPTP dysfunction whereas the isoxazole isostere had minimal effect.
过量的线粒体基质 Ca 和氧化应激导致线粒体内膜的高电导通道(线粒体通透性转换孔,mtPTP)打开。由于 mtPTP 的开放会导致多种病理生理条件下的细胞死亡,因此 mtPTP 抑制剂是治疗各种人类疾病的潜在疗法。高通量筛选工作导致了 3-羧酰胺-5-酚-异恶唑化合物被鉴定为 mtPTP 抑制剂。虽然它们对 mtPTP 的抑制作用具有纳摩尔效力,但它们的血浆稳定性较差,排除了它们在体内研究中的应用。在此,我们描述了一系列结构相关的类似物,其中核心异恶唑被三唑取代,从而提高了血浆稳定性。这些类似物可以使用铜催化的“点击化学”轻松生成。一种类似物,N-(5-氯-2-甲基苯基)-1-(4-氟-3-羟基苯基)-1H-1,2,3-三唑-4-甲酰胺(TR001),在由 mtPTP 功能障碍引起的肌肉萎缩症的斑马鱼模型中是有效的,而异恶唑等排物则效果甚微。
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