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用阿托伐醌和吡咯烷二硫代氨基甲酸盐处理小鼠体内的刚地弓形虫RH株寄生虫的阶段转化

Stage conversion of Toxoplasma gondii RH parasites in mice by treatment with atovaquone and pyrrolidine dithiocarbamate.

作者信息

Djurković-Djaković Olgica, Nikolić Aleksandra, Bobić Branko, Klun Ivana, Aleksić Anastasija

机构信息

Toxoplasmosis Research Laboratory, Department of Medical Parasitology, Institute for Medical Research, Dr. Subotića 4, P.O. Box 102, 11129 Belgrade, Serbia and Montenegro.

出版信息

Microbes Infect. 2005 Jan;7(1):49-54. doi: 10.1016/j.micinf.2004.09.016. Epub 2004 Dec 15.

Abstract

The mouse-virulent RH strain of Toxoplasma gondii is generally considered to have lost its cyst-forming capacity, and conversion of RH tachyzoites into cysts in non-immune mice has previously been shown exclusively following early treatment with sulfadiazine (SDZ). We here describe the development of tissue cysts in mice infected with RH strain parasites and treated with atovaquone (ATO) combined with pyrrolidine dithiocarbamate (PDTC). Groups of Swiss-Webster mice infected intraperitoneally (i.p.) with 10(2) RH tachyzoites were treated with 5, 25 and 100 mg of ATO/kg per day alone or combined with PDTC at 250 mg/kg per day from day 1 postinfection (p.i.) for 14 days. A total of 19 mice survived the 6-week observation period. Of these, brain cysts were recovered in nine (47%), with burdens ranging from 50 to 3120 (mean +/- S.D. = 622 +/- 963). All cyst-harboring mice had high specific IgG antibody levels (1:10,240-1:40,960, corresponding to 500-2000 IU/ml), as did one mouse in which cysts were not demonstrated, which was therefore included in the group of mice with residual infection. Bioassay performed to test the infectivity of these cysts produced acute lethal toxoplasmosis following i.p. inoculation in all instances (100%), and importantly, following peroral inoculation in four (29%). The recovered tachyzoites were highly infectious. In addition, significantly elevated interferon gamma (IFN-gamma) in the treated mice which developed residual infection compared with any group of infection-free (treated or subinoculated) mice, indicates immunological control of the parasite in the latent form. In conclusion, early treatment of mice infected with T. gondii RH tachyzoites with ATO and PDTC induces conversion into tissue cysts, thus providing a new model for studying the mechanism(s) of T. gondii stage conversion.

摘要

刚地弓形虫的小鼠强毒株RH通常被认为已丧失形成包囊的能力,此前已证明,仅在早期用磺胺嘧啶(SDZ)治疗后,RH速殖子才能在非免疫小鼠体内转化为包囊。我们在此描述了感染RH株寄生虫并用阿托伐醌(ATO)联合吡咯烷二硫代氨基甲酸盐(PDTC)治疗的小鼠组织包囊的发育情况。将感染10²个RH速殖子的瑞士-韦伯斯特小鼠腹腔注射(i.p.),从感染后第1天(p.i.)开始,每天单独给予5、25和100 mg/kg的ATO,或与每天250 mg/kg的PDTC联合使用,持续14天。共有19只小鼠在6周的观察期内存活。其中,9只(47%)小鼠的脑中发现了包囊,包囊数量在50至3120个之间(平均值±标准差=622±963)。所有带有包囊的小鼠都有高特异性IgG抗体水平(1:10240 - 1:40960,相当于500 - 2000 IU/ml),有一只未发现包囊的小鼠也是如此,因此该小鼠被纳入残留感染小鼠组。为测试这些包囊的感染性进行的生物测定表明,腹腔接种后所有实例(100%)均引发急性致死性弓形虫病,重要的是,经口接种后有4只(29%)引发该病。回收的速殖子具有高度传染性。此外,与任何一组未感染(治疗或未接种)小鼠相比,发生残留感染的治疗小鼠中干扰素γ(IFN-γ)显著升高,这表明对潜伏形式的寄生虫有免疫控制作用。总之,用ATO和PDTC对感染刚地弓形虫RH速殖子的小鼠进行早期治疗可诱导其转化为组织包囊,从而为研究刚地弓形虫阶段转化机制提供了一个新模型。

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