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用于治疗动物利什曼原虫病的核苷类似物。

Nucleoside analogues for the treatment of animal trypanosomiasis.

机构信息

Laboratory of Microbiology, Parasitology and Hygiene (LMPH), Infla-Med Centre of Excellence, University of Antwerp, Wilrijk, Belgium.

Institute of Infection, Immunity and Inflammation, College of Medical, Veterinary and Life Sciences, University of Glasgow, United Kingdom.

出版信息

Int J Parasitol Drugs Drug Resist. 2022 Aug;19:21-30. doi: 10.1016/j.ijpddr.2022.05.001. Epub 2022 May 6.

Abstract

Animal trypanosomiasis (AT) is a parasitic disease with high socio-economic impact. Given the limited therapeutic options and problems of toxicity and drug resistance, this study assessed redirecting our previously identified antitrypanosomal nucleosides for the treatment of AT. Promising hits were identified with excellent in vitro activity across all important animal trypanosome species. Compound 7, an inosine analogue, and our previously described lead compound, 3'-deoxytubercidin (8), showed broad spectrum anti-AT activity, metabolic stability in the target host species and absence of toxicity, but with variable efficacy ranging from limited activity to full cure in mouse models of Trypanosoma congolense and T. vivax infection. Several compounds show promise against T. evansi (surra) and T. equiperdum (dourine). Given the preferred target product profile for a broad-spectrum compound against AT, this study emphasizes the need to include T. vivax in the screening cascade given its divergent susceptibility profile and provides a basis for lead optimization towards such broad spectrum anti-AT compound.

摘要

动物锥虫病(AT)是一种具有高度社会经济影响的寄生虫病。鉴于治疗选择有限,以及毒性和耐药性问题,本研究评估了重新定位我们之前发现的抗锥虫核苷,用于治疗 AT。在所有重要的动物锥虫物种中,都发现了具有优异体外活性的有前途的化合物。肌苷类似物化合物 7 和我们之前描述的先导化合物 3'-去氧胸苷(8)表现出广谱抗 AT 活性、在目标宿主物种中的代谢稳定性和无毒性,但在感染刚果锥虫和 T. vivax 的小鼠模型中疗效各不相同,从有限的活性到完全治愈不等。几种化合物对 T. evansi(苏拉)和 T. equiperdum(杜林病)有一定疗效。鉴于广谱化合物针对 AT 的首选目标产品特征,本研究强调需要将 T. vivax 纳入筛选级联,因为其具有不同的敏感性特征,并为针对这种广谱抗 AT 化合物的先导化合物优化提供了基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3106/9111543/621ad4b86ff6/ga1.jpg

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