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一种快速、高通量的 Blastocystis spp. 生存力检测方法揭示了甲硝唑耐药性以及药物敏感性的广泛亚型依赖性差异。

A rapid, high-throughput viability assay for Blastocystis spp. reveals metronidazole resistance and extensive subtype-dependent variations in drug susceptibilities.

机构信息

Laboratory of Molecular and Cellular Parasitology, Department of Microbiology, Yong Loo Lin School of Medicine, National University of Singapore, Singapore, Singapore.

出版信息

Antimicrob Agents Chemother. 2011 Feb;55(2):637-48. doi: 10.1128/AAC.00900-10. Epub 2010 Nov 22.

DOI:10.1128/AAC.00900-10
PMID:21098237
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3028762/
Abstract

Blastocystis is an emerging protistan parasite of controversial pathogenesis. Although metronidazole (Mz) is standard therapy for Blastocystis infections, there have been accumulating reports of treatment failure, suggesting the existence of drug-resistant isolates. Furthermore, very little is known about Blastocystis susceptibility to standard antimicrobials. In the present study, we established resazurin and XTT viability microassays for Blastocystis spp. belonging to subtypes 4 and 7, both of which have been suggested to represent pathogenic zoonotic subtypes. The optimized resazurin assay was used to screen a total of 19 compounds against both subtypes. Interestingly, subtype 7 parasites were resistant to Mz, a 1-position-substituted 5-nitroimidazole (5-NI), while subtype 4 parasites were sensitive. Some cross-resistance was observed to tinidazole, another 1-position 5-NI. Conversely, subtype 4 parasites were resistant to emetine, while subtype 7 parasites were sensitive. Position 2 5-NIs were effective against both subtypes, as were ornidazole, nitazoxanide, furazolidone, mefloquine, quinicrine, quinine, cotrimoxazole (trimethoprim-sulfamethoxazole), and iodoacetamide. Both subtypes were resistant to chloroquine, doxycycline, paromomycin, ampicillin, and pyrimethamine. This is the first study to report extensive variations in drug sensitivities among two clinically important subtypes. Our study highlights the need to reevaluate established treatment regimens for Blastocystis infections and offers clear new treatment options for Mz treatment failures.

摘要

芽囊原虫是一种新兴的具有争议性发病机制的原生动物寄生虫。尽管甲硝唑(Mz)是治疗芽囊原虫感染的标准疗法,但越来越多的治疗失败报告表明存在耐药分离株。此外,关于芽囊原虫对标准抗生素的敏感性知之甚少。在本研究中,我们建立了属于亚型 4 和 7 的芽囊原虫属的 Resazurin 和 XTT 生存力微量测定法,这两种亚型都被认为是具有致病性的动物源性亚型。优化的 Resazurin 测定法用于筛选总共 19 种化合物对两种亚型的活性。有趣的是,亚型 7 寄生虫对 Mz 具有抗性,而亚型 4 寄生虫则敏感,这是一种 1 位取代的 5-硝基咪唑(5-NI)。相反,亚型 4 寄生虫对乙胺嘧啶具有抗性,而亚型 7 寄生虫则敏感。另一种 1 位 5-NI 替硝唑也存在交叉耐药性。相反,亚型 4 寄生虫对依米丁具有抗性,而亚型 7 寄生虫则敏感。位置 2 的 5-NIs 对两种亚型均有效,奥硝唑、硝唑尼特、呋喃唑酮、甲氟喹、奎宁、奎宁、复方磺胺甲噁唑(甲氧苄啶-磺胺甲噁唑)和碘乙酰胺也是如此。两种亚型均对氯喹、强力霉素、巴龙霉素、氨苄西林和氨苯砜具有抗性。这是第一项报告两种临床上重要亚型之间药物敏感性广泛变化的研究。我们的研究强调需要重新评估芽囊原虫感染的既定治疗方案,并为 Mz 治疗失败提供明确的新治疗选择。

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