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抗抑郁药舍曲林作为药物再利用候选物的杀利什曼原虫活性的分子基础。

Molecular Basis of the Leishmanicidal Activity of the Antidepressant Sertraline as a Drug Repurposing Candidate.

机构信息

Centro de Investigaciones Biológicas (CIB-CSIC), Madrid, Spain.

Centro de Metabolómica y Bioanálisis (CEMBIO), Facultad de Farmacia, Universidad CEU San Pablo, Boadilla del Monte, Madrid, Spain.

出版信息

Antimicrob Agents Chemother. 2018 Nov 26;62(12). doi: 10.1128/AAC.01928-18. Print 2018 Dec.

Abstract

Drug repurposing affords the implementation of new treatments at a moderate cost and under a faster time-scale. Most of the clinical drugs against share this origin. The antidepressant sertraline has been successfully assayed in a murine model of visceral leishmaniasis. Nevertheless, sertraline targets in were poorly defined. In order to get a detailed insight into the leishmanicidal mechanism of sertraline on , unbiased multiplatform metabolomics and transmission electron microscopy were combined with a focused insight into the sertraline effects on the bioenergetics metabolism of the parasite. Sertraline induced respiration uncoupling, a significant decrease of intracellular ATP level, and oxidative stress in promastigotes. Metabolomics evidenced an extended metabolic disarray caused by sertraline. This encompasses a remarkable variation of the levels of thiol-redox and polyamine biosynthetic intermediates, as well as a shortage of intracellular amino acids used as metabolic fuel by Sertraline killed through a multitarget mechanism of action, tackling essential metabolic pathways of the parasite. As such, sertraline is a valuable candidate for visceral leishmaniasis treatment under a drug repurposing strategy.

摘要

药物重利用以适中的成本和更快的时间尺度实现新的治疗方法。大多数针对的临床药物都具有这种起源。抗抑郁药舍曲林已在内脏利什曼病的小鼠模型中成功进行了检测。然而,舍曲林在中的靶点定义不明确。为了更详细地了解舍曲林对的杀利什曼原虫机制,我们结合无偏倚的多平台代谢组学和透射电子显微镜,深入研究了舍曲林对寄生虫生物能量代谢的影响。舍曲林诱导呼吸解偶联、细胞内 ATP 水平显著下降和氧化应激。代谢组学证明了舍曲林引起的代谢紊乱。这包括硫醇氧化还原和多胺生物合成中间产物水平的显著变化,以及作为代谢燃料的细胞内氨基酸的短缺。舍曲林通过针对寄生虫重要代谢途径的多靶点作用机制杀死。因此,舍曲林是一种有价值的候选药物,可用于内脏利什曼病的药物重利用策略治疗。

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