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环孢素对啮齿类动物疟疾的阶段选择性抑制作用。

Stage-selective inhibition of rodent malaria by cyclosporine.

作者信息

Murphy J R, Baqar S, Baker R H, Roberts E, Nickell S P, Cole G A

机构信息

International Health Program, University of Maryland School of Medicine, Baltimore 21201.

出版信息

Antimicrob Agents Chemother. 1988 Apr;32(4):462-6. doi: 10.1128/AAC.32.4.462.

Abstract

The relative susceptibility of different developmental stages of Plasmodium berghei to cyclosporine was investigated in vivo. Within 12 h of receiving a single 25-mg/kg (body weight) dose of cyclosporine, mice with patent P. berghei infections uniformly exhibited a rapid fall in asexual parasite stages. Initially, ring forms and mature schizonts disappeared. Subsequently, trophozoites disappeared between 21 and 24 h, whereas gametocytes persisted for 36 h. In contrast, when cyclosporine was administered to mice 1 day before inoculation (100 mg/kg) with P. berghei sporozoites and for 2 consecutive days after inoculation (25 mg/kg), infections developed normally. When mice with patent infections were placed on prolonged cyclosporine therapy (25 mg/kg per day), parasitemia initially disappeared but often recrudesced. Recrudescent parasites were frequently resistant to cyclosporine (Csr). The Csr phenotype remained stable after serial passage of parasites in mice and after transmission through Anopheles stephensi mosquitoes, in which the capacity to produce oocysts was reduced. When infections of untreated mice were initiated with equal numbers of Csr and cyclosporine-susceptible (Css) parasites and then carried through two serial cycles of mosquito-to-mouse transmission without cyclosporine treatment, the Csr phenotype was lost. The results indicate that cyclosporine selectively inhibits asexual blood stages of P. berghei and favors the emergence of Csr parasites with diminished infectivity for mosquitoes.

摘要

在体内研究了伯氏疟原虫不同发育阶段对环孢素的相对敏感性。在接受单次25mg/kg(体重)剂量的环孢素后12小时内,患有伯氏疟原虫显性感染的小鼠无性寄生虫阶段均迅速减少。最初,环状体和成熟裂殖体消失。随后,滋养体在21至24小时之间消失,而配子体持续存在36小时。相比之下,当在接种伯氏疟原虫子孢子前1天给小鼠施用环孢素(100mg/kg)并在接种后连续2天(25mg/kg)给药时,感染正常发展。当患有显性感染的小鼠接受长期环孢素治疗(每天25mg/kg)时,寄生虫血症最初消失,但常常复发。复发的寄生虫通常对环孢素耐药(Csr)。在小鼠体内连续传代以及通过斯氏按蚊传播后,Csr表型保持稳定,在斯氏按蚊中产生卵囊的能力降低。当用等量的Csr和对环孢素敏感(Css)的寄生虫启动未治疗小鼠的感染,然后在不进行环孢素治疗的情况下进行两个连续的蚊媒传播周期时,Csr表型消失。结果表明,环孢素选择性抑制伯氏疟原虫的无性血液阶段,并有利于出现对蚊子感染性降低的Csr寄生虫。

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