吩噻嗪类的抗结核药效动力学。
Antitubercular pharmacodynamics of phenothiazines.
机构信息
Liverpool School of Tropical Medicine, Pembroke Place, Liverpool L3 5QA, UK.
出版信息
J Antimicrob Chemother. 2013 Apr;68(4):869-80. doi: 10.1093/jac/dks483. Epub 2012 Dec 9.
OBJECTIVES
Phenothiazines have been shown to exhibit in vitro and in vivo activity against Mycobacterium tuberculosis (Mtb) and multidrug-resistant Mtb. They are predicted to target the genetically validated respiratory chain component type II NADH:quinone oxidoreductase (Ndh). Using a set of compounds containing the phenothiazine pharmacophore, we have (i) investigated whether chemical validation data support the molecular target and (ii) evaluated pharmacophore tractability for further drug development.
METHODS
Recombinant Mtb Ndh was generated and its functionality confirmed by steady-state kinetics. Pharmacodynamic profiling of the phenothiazines, including antitubercular efficacy in aerobic and O2-limited conditions, time-kill assays and isobole analyses against first-line antituberculars, was performed. Potential mitochondrial toxicity was assessed in a modified HepG2 cell-line assay and against bovine cytochrome bc1.
RESULTS
Steady-state kinetic analyses revealed a substrate preference for coenzyme Q2 and an inability to utilize NADPH. A positive correlation between recombinant Ndh inhibition and kill of aerobically cultured Mtb was observed, whilst enhanced potency was demonstrated in a hypoxic model. Time-kill studies revealed the phenothiazines to be bactericidal whilst isobolograms exposed antagonism with isoniazid, indicative of intracellular NADH/NAD(+) couple perturbation. At therapeutic levels, phenothiazine-mediated toxicity was appreciable; however, specific mitochondrial targeting was excluded.
CONCLUSIONS
Data generated support the hypothesis that Ndh is the molecular target of phenothiazines. The favourable pharmacodynamic properties of the phenothiazines are consistent with a target product profile that includes activity against dormant/persistent bacilli, rapid bactericidal activity and activity against drug-resistant Mtb by a previously unexploited mode of action. These properties warrant further medicinal chemistry to improve potency and safety.
目的
已证实吩噻嗪类药物具有抗结核分枝杆菌(Mtb)和耐多药 Mtb 的体外和体内活性。它们被预测靶向经基因验证的呼吸链成分 II 型 NADH:醌氧化还原酶(Ndh)。使用一组包含吩噻嗪药效团的化合物,我们(i)研究了化学验证数据是否支持分子靶标,以及(ii)评估了药效团的可开发性,以进一步开发药物。
方法
生成重组 Mtb Ndh 并通过稳态动力学确认其功能。对吩噻嗪类药物进行药效学分析,包括在需氧和 O2 受限条件下的抗结核活性、时间杀伤测定和与一线抗结核药物的等摩尔分析,评估其潜在的线粒体毒性在改良的 HepG2 细胞系测定中和牛细胞色素 bc1 中。
结果
稳态动力学分析表明对辅酶 Q2 有底物偏好,并且无法利用 NADPH。观察到重组 Ndh 抑制与需氧培养 Mtb 杀伤之间存在正相关,而在低氧模型中显示出增强的效力。时间杀伤研究表明吩噻嗪类药物具有杀菌作用,而等摩尔图显示与异烟肼的拮抗作用,表明细胞内 NADH/NAD(+) 偶联受到干扰。在治疗水平下,吩噻嗪介导的毒性是明显的;然而,排除了特异性线粒体靶向。
结论
生成的数据支持 Ndh 是吩噻嗪类药物的分子靶标的假说。吩噻嗪类药物的有利药效学特性与目标产品特性一致,包括对休眠/持久杆菌的活性、快速杀菌活性和通过以前未开发的作用模式对耐药 Mtb 的活性。这些特性需要进一步的药物化学研究来提高效力和安全性。
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