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用小鼠模型对依氟鸟氨酸和苏拉明进行针对伊氏锥虫的体内研究。

In vivo investigations of selected diamidine compounds against Trypanosoma evansi using a mouse model.

机构信息

Parasite Chemotherapy, Department of Medical Parasitology and Infection Biology, Swiss Tropical Institute, Basel, Switzerland.

出版信息

Antimicrob Agents Chemother. 2009 Dec;53(12):5074-9. doi: 10.1128/AAC.00422-09. Epub 2009 Sep 28.

Abstract

Surra is an animal pathogenic protozoan infection, caused by Trypanosoma evansi, that develops into a fatal wasting disease. Control measures rely on diagnosis and treatment. However, with the continuous emergence of drug resistance, this tactic is failing, and the pressing need for new chemotherapeutic agents is becoming critical. With the introduction of novel aromatic diamidines, a new category of antitrypanosomal drugs was discovered. Nevertheless, their efficacy within a T. evansi-infected mouse model was not known. In total, 30 compounds previously selected based on their in vitro activity were tested in a T. evansi mouse model of infection. Six of the compounds were capable of curing T. evansi-infected mice at drug doses as low as 0.5 and 0.25 mg/kg of body weight administered for 4 consecutive days, and they were more effective than the standard drugs suramin, diminazene, and quinapyramine. After all selection criteria were applied, three diamidine compounds (DB 75, DB 867, and DB 1192) qualified as lead compounds and were considered to have the potential to act as preclinical candidates against T. evansi infection.

摘要

苏拉病是一种动物致病性原生动物感染,由伊氏锥虫引起,发展为致命的消瘦病。控制措施依赖于诊断和治疗。然而,随着耐药性的不断出现,这种策略正在失效,迫切需要新的化疗药物。随着新型芳香二脒的引入,发现了一类新的抗锥虫药物。然而,它们在伊氏锥虫感染小鼠模型中的疗效尚不清楚。总共,根据体外活性先前选择的 30 种化合物在伊氏锥虫感染的小鼠模型中进行了测试。有 6 种化合物能够以低至 0.5 和 0.25mg/kg 体重的药物剂量治愈伊氏锥虫感染的小鼠,连续给药 4 天,并且比标准药物苏拉明、苯脒嗪和奎那吡嗪更有效。应用所有选择标准后,三种二脒化合物(DB 75、DB 867 和 DB 1192)符合先导化合物标准,并被认为有可能成为针对伊氏锥虫感染的临床前候选药物。

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