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载阿托伐醌纳米胶囊治疗急性和慢性小鼠弓形虫病的活性评估。

Assessment of the activity of atovaquone-loaded nanocapsules in the treatment of acute and chronic murine toxoplasmosis.

作者信息

Sordet F, Aumjaud Y, Fessi H, Derouin F

机构信息

Laboratoire de Parasitologie-Mycologie, Hôpital Saint-Louis, Paris, France.

出版信息

Parasite. 1998 Sep;5(3):223-9. doi: 10.1051/parasite/1998053223.

Abstract

The aim of this work was to develop a new pharmaceutical form of atovaquone and to study its activity against Toxoplasma gondii in vitro and in vivo. Nanocapsules were chosen as the oral dosage form of administration. An analytical method was developed to determine the drug content in nanocapsules. The stability of these nanocapsules were assessed by following drug content, size, pH and osmolarity for a period of six months. The in vitro activity of atovaquone-loaded nanocapsules against tachyzoites of T. gondii (RH stain) was comparable to its suspension form. In vivo studies were carried out in murine models of acute and chronic toxoplasmosis. Mice acutely infected with the virulent RH strain were orally treated with a dose regimen of 15 mg/kg/day for 10 days, starting from day 1 post-infection. 75% of the mice receiving atovaquone-loaded nanocapsules survived 30 days post-infection, compared to none of untreated controls and none of mice treated with the suspension with the same dose regimen. In mice chronically infected by the COUL or the ME49 strain (Type II strains), then treated for six weeks, treatment with atovaquone (15 mg/kg/d, nanoparticles or suspension) resulted in a decrease of brain parasitic burden, which was significantly more pronounced in ME49-infected mice and in those treated with drug-loaded nanocapsules. These results show that the sensibility of T. gondii to atovaquone is different according to the strains and that the activity of atovaquone in the treatment of toxoplasmosis is enhanced when administered in nanoparticular form.

摘要

这项工作的目的是开发一种新的阿托伐醌药物剂型,并研究其在体外和体内对刚地弓形虫的活性。选择纳米胶囊作为口服给药剂型。开发了一种分析方法来测定纳米胶囊中的药物含量。通过跟踪药物含量、粒径、pH值和渗透压,对这些纳米胶囊进行了为期六个月的稳定性评估。载阿托伐醌纳米胶囊对刚地弓形虫速殖子(RH株)的体外活性与其悬浮液形式相当。在急性和慢性弓形虫病的小鼠模型中进行了体内研究。从感染后第1天开始,对急性感染强毒株RH的小鼠以15mg/kg/天的剂量方案口服给药10天。接受载阿托伐醌纳米胶囊的小鼠中有75%在感染后30天存活,而未治疗的对照组小鼠和接受相同剂量方案悬浮液治疗的小鼠均无存活。在慢性感染COUL或ME49株(II型菌株)的小鼠中,然后治疗六周,用阿托伐醌(15mg/kg/d,纳米颗粒或悬浮液)治疗导致脑内寄生虫负荷降低,这在ME49感染的小鼠和接受载药纳米胶囊治疗的小鼠中更为明显。这些结果表明,刚地弓形虫对阿托伐醌的敏感性因菌株而异,并且阿托伐醌以纳米颗粒形式给药时,其在治疗弓形虫病中的活性增强。

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