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左旋咪唑联合苯并咪唑治疗实验性恰加斯病的影响。

Impact of levamisole in co-administration with benznidazole on experimental Chagas disease.

机构信息

Laboratório de Biologia Celular, Pavilhão Cardoso Fontes,Instituto Oswaldo Cruz (IOC/Fiocruz),Avenida Brasil, 4365, Manguinhos, 21040-900,Rio de Janeiro, RJ,Brazil.

Laboratório de Biologia Molecular e Doenças Endêmicas, Pavilhão Leônidas Deane,Instituto Oswaldo Cruz (IOC/Fiocruz),Avenida Brasil,4365, Manguinhos, 21040-900,Rio de Janeiro, RJ,Brazil.

出版信息

Parasitology. 2019 Jul;146(8):1055-1062. doi: 10.1017/S0031182019000374. Epub 2019 May 3.

Abstract

Levamisole (Lms) is an anthelminthic drug with immunomodulatory activity. Chagas disease (CD) is caused by Trypanosoma cruzi and there is very low access to the drugs available, benznidazole (Bz) and nifurtimox, both far from ideal. In a drug-repurposing strategy to test potential activity as antiparasitic and immunomodulatory agent for CD, Lms was assayed on acute T. cruzi murine infection, alone and in co-administration with Bz. During protocol standardization, 100 and 10 mpk of Bz given for five consecutive days resulted in parasitaemia suppression and 100% animal survival only with the highest dose. Flow cytometry showed that both optimal (100 mpk) and suboptimal (10 mpk) doses of Bz equally decreased the plasma levels of cytokines commonly elevated in this acute infection model. Lms alone (10-0.5 mpk) did not decrease parasitaemia nor mortality rates. Co-administration was investigated using the suboptimal dose of Bz and different doses of Lms. While Bz 10 mpk did not alter parasitaemia, the combo partially reduced it but only slightly promoted animal survival. This effect could be related to Th1-response modulation since interleukin-6 and interferon-γ were higher after treatment with the combo.

摘要

左旋咪唑(Lms)是一种具有免疫调节活性的抗蠕虫药物。恰加斯病(CD)由克氏锥虫引起,可用药物(苯并咪唑(Bz)和硝呋替莫)非常有限,而且都不理想。在一项药物再利用策略中,为了测试左旋咪唑作为 CD 抗寄生虫和免疫调节剂的潜在活性,在急性 T. cruzi 感染的小鼠模型中单独和与 Bz 联合使用了 Lms。在方案标准化过程中,连续 5 天给予 100 和 10 mpk 的 Bz 可抑制寄生虫血症并使 100%的动物存活,只有最高剂量才有此效果。流式细胞术显示,两种剂量(100 mpk 和 10 mpk)的 Bz 均同等降低了该急性感染模型中常见升高的细胞因子的血浆水平。单独使用 Lms(10-0.5 mpk)既不能降低寄生虫血症,也不能降低死亡率。使用亚最佳剂量的 Bz 和不同剂量的 Lms 进行了联合用药研究。虽然 Bz 10 mpk 并未改变寄生虫血症,但联合用药部分降低了寄生虫血症,但仅略有提高动物存活率。这种效果可能与 Th1 反应的调节有关,因为在联合用药后白细胞介素-6 和干扰素-γ水平更高。

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