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双噻唑鎓盐的前药是口服有效的抗疟药。

Prodrugs of bisthiazolium salts are orally potent antimalarials.

作者信息

Vial Henri J, Wein Sharon, Farenc Christine, Kocken Clemens, Nicolas Olivier, Ancelin Marie Laure, Bressolle Francoise, Thomas Alan, Calas Michèle

机构信息

Unité Mixte de Recherche 5539, Centre National de la Recherche Scientifique/Université Montpellier II, Case 107, Place Eugène Bataillon, 34095 Montpellier Cedex 5, France.

出版信息

Proc Natl Acad Sci U S A. 2004 Oct 26;101(43):15458-63. doi: 10.1073/pnas.0404037101. Epub 2004 Oct 18.

DOI:10.1073/pnas.0404037101
PMID:15492221
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC523447/
Abstract

We created neutral antimalarial prodrugs that deliver bisthiazolium compounds with antimalarial activity in the nanomolar range. These drugs primarily affect early intraerythrocytic stages through rapid, nonreversible cytotoxicity. The compounds are suitable for both parenteral and oral use and plasma promotes rapid conversion of the prodrug into the drug. We demonstrate that very low doses offer protection in a murine model of malaria. The drugs show great potential for curing high parasitemia with short-course treatments. Oral administration of the TE3 prodrug completely cures Plasmodium cynomolgi infection in rhesus monkeys. The drugs specifically accumulate inside infected erythrocytes, block phosphatidylcholine biosynthesis, and interact with hemozoin. To our knowledge, this class of compounds represents one of the most potent antimalarials tested to date. These unique properties signal a promising future for this class of antimalarial.

摘要

我们合成了具有抗疟疾活性的中性抗疟前药,这些前药能够释放双噻唑鎓化合物,其抗疟活性在纳摩尔范围内。这些药物主要通过快速、不可逆的细胞毒性作用于红细胞内早期阶段。这些化合物适用于肠胃外和口服给药,血浆可促进前药快速转化为药物。我们证明,极低剂量的药物在疟疾小鼠模型中具有保护作用。这些药物在短疗程治疗高寄生虫血症方面显示出巨大潜力。口服TE3前药可完全治愈恒河猴体内的食蟹猴疟原虫感染。这些药物特异性地积聚在受感染的红细胞内,阻断磷脂酰胆碱的生物合成,并与疟原虫色素相互作用。据我们所知,这类化合物是迄今为止测试过的最有效的抗疟药物之一。这些独特的特性预示着这类抗疟药物有着光明的前景。

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