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将金诺芬重新用于治疗实验性脑弓形体病。

Repurposing auranofin for treatment of Experimental Cerebral Toxoplasmosis.

机构信息

Professor of Parasitology, Faculty of Medicine, Alexandria University, Alexandria, Egypt.

Lecturer of Parasitology, Faculty of Medicine, Alexandria University, Alexandria, Egypt.

出版信息

Acta Parasitol. 2021 Sep;66(3):827-836. doi: 10.1007/s11686-021-00337-z. Epub 2021 Feb 8.

Abstract

PURPOSES

Evaluate the effect of auranofin on the early and late stages of chronic infection with Toxoplasma gondii avirulent ME49 strain.

METHODS

Swiss albino mice were orally inoculated with 10 cysts of Toxoplasma gondii, and orally treated with auranofin or septazole in daily doses of 20 mg/kg or 100 mg /kg, respectively, for 30 days. Treatment began either on the same day of infection and mice were sacrificed at the 60th day postinfection or the treatment started after 60 days of infection and mice were sacrificed at the 90th day postinfection.

RESULTS

Auranofin significantly reduced the brain cyst burden and inflammatory reaction at both stages of infection compared to the infected non-treated control. More remarkably, auranofin significant reduced the brain cyst burden in the late stage, while septazole failed. Hydrogen peroxide level was significantly increased in the brain homogenate of mice treated with auranofin only at the early stage of infection. Ultrastructral studies revealed that the anti-Toxoplasma effect of auranofin is achieved by changing the membrane permeability and inducing apoptosis.

CONCLUSIONS

Thus, auranofin could be an alternative for the standard treatment regimen of toxoplasmosis and these results are considered another achievement for the drug against parasitic infection. Being a FDA-approved drug, it can be rapidly evaluated in clinical trials.

摘要

目的

评估金诺芬对弓形虫弱毒株慢性感染早期和晚期的影响。

方法

瑞士白化病小鼠经口感染 10 个弓形虫包囊,分别以 20mg/kg 或 100mg/kg 的日剂量口服金诺芬或塞曲唑治疗 30 天。治疗开始于感染当天或感染后 60 天开始,感染后 90 天处死小鼠。

结果

与未感染未经治疗的对照组相比,金诺芬在感染的两个阶段均显著降低了脑囊虫负荷和炎症反应。更值得注意的是,金诺芬在晚期显著降低了脑囊虫负荷,而塞曲唑则没有。仅在感染早期,用金诺芬处理的小鼠脑匀浆中过氧化氢水平显著升高。超微结构研究表明,金诺芬的抗弓形虫作用是通过改变膜通透性和诱导细胞凋亡来实现的。

结论

因此,金诺芬可能是弓形虫病标准治疗方案的替代药物,这些结果被认为是该药物抗寄生虫感染的又一成就。作为一种 FDA 批准的药物,它可以在临床试验中快速评估。

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