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首页> 外文期刊>Parasitology International >Development of an effective alternative model for in vivo hypnozoiteinduced relapse infection: A Japanese macaque (Macaca fuscata) model experimentally infected with Plasmodium cynomolgi
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Development of an effective alternative model for in vivo hypnozoiteinduced relapse infection: A Japanese macaque (Macaca fuscata) model experimentally infected with Plasmodium cynomolgi

机译:开发体内催眠素诱导的复发感染有效替代模型:用疟原虫进行实验感染的日本猕猴(猕猴属FUSCATA)模型

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摘要

In the present study, we demonstrate that the Japanese macaque (Macaca fuscata) can be used as an effective alternative in vivo model for investigating hypnozoite-induced relapsing infection caused by Plasmodium cynomolgi B strain, and that this model is comparable to the rhesus macaque model. Two female Japanese macaques (JM-1 and JM-2; aged 5 years; weighing about 4.0 kg) were used for the experiment. To produce sporozoites in mosquitoes, blood infected with P. cynomolgi B strain was collected from the donor monkey JM-1 and fed to approximately 200 mosquitoes using the standard artificial membrane feeding method. The isolated sporozoites (2 x 10(5)) were intravenously inoculated into the JM-2 monkey, and the blood stage of the parasite was detected on day 8 after the infection. Chloroquine sulfate (CQ) was intramuscularly administered at a dosage of 6.0 mg/kg into the JM-2 monkey for 6 consecutive days from day 12 onward, after which the parasites disappeared from the peripheral blood. The first relapse occurred on day 26, which was treated again with CQ. Then, the second relapse occurred on day 44, which was cured by CQ treatment followed by the administration of primaquine phosphate (PQ) at a dosage of 1.0 mg/kg/day for 15 days. The JM-2 monkey was observed until 69 days after PQ administration, and there was no relapse during the entire follow-up period. We propose that the Japanese macaque model could contribute not only to drug screening for anti-hypnozoite activity, but could also be used as a powerful tool for investigating hypnozoite biology.
机译:在本研究中,我们证明日本猕猴(Macaca FUSCATA)可以用作体内模型中的有效替代方案,用于研究由疟原虫引起的疟原虫诱导的疟原虫B株引起的复发感染,并且该模型与恒星猕猴模型相当。两只雌性日本猕猴(JM-1和JM-2;年龄5岁;重约4.0千克)用于实验。为了在蚊子中产生孢子,用P. cynomolgi B菌株的血液从供体猴JM-1收集,并使用标准人工膜进料法进料到大约200℃。将分离的孢子(2×10(5))静脉内接种到JM-2猴中,并且在感染后第8天检测寄生虫的血液阶段。将氯喹硫酸盐(CQ)以6.0mg / kg的剂量以6.0mg / kg的剂量分成JM-2猴,从第12天开始,之后寄生虫从外周血中消失。第26天发生了第一次复发,其再次用CQ治疗。然后,在第44天发生第二复发,其通过CQ处理固化,然后在1.0mg / kg /天的剂量下给予原磷酸酯(PQ),持续15天。在PQ管理后69天观察到JM-2猴,在整个后续期间没有复发。我们提出日本猕朗克模型可能不仅有助于对抗催眠素活性的药物筛查,而且还可以用作调查催眠生物学的强大工具。

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  • 来源
    《Parasitology International》 |2020年第2020期|共4页
  • 作者单位

    Dokkyo Med Univ Dept Trop Med &

    Parasitol Mibu Tochigi 3210293 Japan;

    Natl Inst Infect Dis Dept Parasitol Shinjuku Ku Tokyo Japan;

    Natl Inst Infect Dis Dept Parasitol Shinjuku Ku Tokyo Japan;

    Natl Inst Biomed Innovat Hlth &

    Nutr Tsukuba Primate Res Ctr Lab Immunoregulat &

    Vaccine Res Tsukuba Ibaraki Japan;

    Natl Inst Biomed Innovat Hlth &

    Nutr Tsukuba Primate Res Ctr Lab Immunoregulat &

    Vaccine Res Tsukuba Ibaraki Japan;

    Natl Inst Biomed Innovat Hlth &

    Nutr Tsukuba Primate Res Ctr Lab Immunoregulat &

    Vaccine Res Tsukuba Ibaraki Japan;

    Dokkyo Med Univ Dept Trop Med &

    Parasitol Mibu Tochigi 3210293 Japan;

    Nagasaki Univ Inst Trop Med NEKKEN Dept Protozool Nagasaki Japan;

    Natl Inst Biomed Innovat Hlth &

    Nutr Tsukuba Primate Res Ctr Lab Immunoregulat &

    Vaccine Res Tsukuba Ibaraki Japan;

    Dokkyo Med Univ Dept Trop Med &

    Parasitol Mibu Tochigi 3210293 Japan;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 寄生生物学;
  • 关键词

    Plasmodium cynomolgi; Japanese macaque; Hypnozoite; Relapse; Primate model;

    机译:疟原虫Cynomolgi;日本短尾猿;催眠;复发;灵长类动物模型;

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