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非昔硝唑：一种用于治疗恰加斯病的潜在新药候选物。

Fexinidazole: a potential new drug candidate for Chagas disease.

机构信息

Laboratório de Doença de Chagas, Departamento de Ciências Biológicas & Núcleo de Pesquisas em Ciências Biológicas, Universidade Federal de Ouro Preto, Campus Universitário, Morro do Cruzeiro, Ouro Preto, Brazil.

出版信息

PLoS Negl Trop Dis. 2012;6(11):e1870. doi: 10.1371/journal.pntd.0001870. Epub 2012 Nov 1.

DOI:10.1371/journal.pntd.0001870

PMID:23133682

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3486905/

Abstract

BACKGROUND

New safe and effective treatments for Chagas disease (CD) are urgently needed. Current chemotherapy options for CD have significant limitations, including failure to uniformly achieve parasitological cure or prevent the chronic phase of CD, and safety and tolerability concerns. Fexinidazole, a 2-subsituted 5-nitroimidazole drug candidate rediscovered following extensive compound mining by the Drugs for Neglected Diseases initiative and currently in Phase I clinical study for the treatment of human African trypanosomiasis, was evaluated in experimental models of acute and chronic CD caused by different strains of Trypanosoma cruzi.

METHODS AND FINDINGS

We investigated the in vivo activity of fexinidazole against T. cruzi, using mice as hosts. The T. cruzi strains used in the study were previously characterized in murine models as susceptible (CL strain), partially resistant (Y strain), and resistant (Colombian and VL-10 strains) to the drugs currently in clinical use, benznidazole and nifurtimox. Our results demonstrated that fexinidazole was effective in suppressing parasitemia and preventing death in infected animals for all strains tested. In addition, assessment of definitive parasite clearance (cure) through parasitological, PCR, and serological methods showed cure rates of 80.0% against CL and Y strains, 88.9% against VL-10 strain, and 77.8% against Colombian strain among animals treated during acute phase, and 70% (VL-10 strain) in those treated in chronic phase. Benznidazole had a similar effect against susceptible and partially resistant T. cruzi strains. Fexinidazole treatment was also shown to reduce myocarditis in all animals infected with VL-10 or Colombian resistant T. cruzi strains, although parasite eradication was not achieved in all treated animals at the tested doses.

CONCLUSIONS

Fexinidazole is an effective oral treatment of acute and chronic experimental CD caused by benznidazole-susceptible, partially resistant, and resistant T. cruzi. These findings illustrate the potential of fexinidazole as a drug candidate for the treatment of human CD.

摘要

背景

目前急需寻找安全有效的新型药物来治疗恰加斯病（Chagas disease，CD）。现有的 CD 化学疗法存在诸多局限性，包括不能完全清除寄生虫、无法预防疾病的慢性期、以及安全性和耐受性问题。芬苯达唑是一种经“被忽视疾病药物研发倡议”（Drugs for Neglected Diseases initiative）广泛挖掘化合物后重新发现的 2-取代 5-硝基咪唑类候选药物，目前正处于治疗人类非洲锥虫病的 I 期临床试验阶段。本研究评估了芬苯达唑在不同品系克氏锥虫引起的急性和慢性 CD 实验模型中的体内活性。

方法和发现

本研究使用感染克氏锥虫的小鼠作为宿主，评估了芬苯达唑的体内活性。本研究中使用的克氏锥虫株在先前的小鼠模型中被鉴定为对现有临床用药（苯硝唑和硝呋莫司）敏感（CL 株）、部分耐药（Y 株）和耐药（哥伦比亚株和 VL-10 株）。结果显示，芬苯达唑对所有测试株均具有抗寄生虫血症和降低死亡率的作用。此外，通过寄生虫学、PCR 和血清学方法评估明确的寄生虫清除（治愈）显示，在急性感染期，芬苯达唑对 CL 和 Y 株的治愈率为 80.0%，对 VL-10 株为 88.9%，对哥伦比亚株为 77.8%；在慢性感染期，对 VL-10 株的治愈率为 70%。苯硝唑对敏感和部分耐药的克氏锥虫株也有类似的效果。芬苯达唑治疗还能降低所有感染 VL-10 株或哥伦比亚株耐药克氏锥虫的动物的心肌炎，但在测试剂量下，并非所有治疗动物都能完全清除寄生虫。

结论

芬苯达唑是一种有效治疗苯硝唑敏感、部分耐药和耐药克氏锥虫引起的急性和慢性 CD 的口服药物。这些发现表明芬苯达唑有潜力成为治疗人类 CD 的候选药物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5de1/3486905/536c8949f55a/pntd.0001870.g001.jpg

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非昔硝唑：一种用于治疗恰加斯病的潜在新药候选物。

Fexinidazole: a potential new drug candidate for Chagas disease.

机构信息

出版信息

BACKGROUND

METHODS AND FINDINGS

CONCLUSIONS

背景

方法和发现

结论

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