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利福平对间日疟原虫疟疾的抗疟作用。

Antimalarial effects of rifampin in Plasmodium vivax malaria.

作者信息

Pukrittayakamee S, Viravan C, Charoenlarp P, Yeamput C, Wilson R J, White N J

机构信息

Hospital for Tropical Diseases, Faculty of Tropical Medicine, Mahidol University, Bangkok, Thailand.

出版信息

Antimicrob Agents Chemother. 1994 Mar;38(3):511-4. doi: 10.1128/AAC.38.3.511.

Abstract

The antimalarial effects of rifampin in 60 adults with Plasmodium vivax malaria were assessed. There were three treatment groups: rifampin (20 and 15 mg/kg of body weight per day for 1 and 4 days, respectively; n = 5); rifampin followed by primaquine (15 mg of base per day for 14 days; n = 25), and chloroquine (25 mg of base per kg over 3 days) followed by primaquine (n = 30). All patients were hospitalized till clearance of fever and parasites, and 45 patients stayed in the hospital for 1 month. Despite initial clearance of fever in all patients and a > or = 6-fold reduction in parasitemia per 48-h life cycle, rifampin alone was not effective: all five patients had subsequent R2-like parasitological responses. All patients treated with rifampin-primaquine cleared both fever and parasitemia, but the therapeutic responses were slower than those following treatment with chloroquine-primaquine. Final fever clearance times were significantly longer (mean [standard deviation] = 43 [35] versus 27 [19] h; P = 0.046), and the parasite clearance times (to 50 and 90% of admission parasite counts and to a level undetectable in a peripheral blood smear) were also significantly greater (P = 0.053 to < 0.001). However, reappearance of infection occurred in only one patient treated with rifampin-primaquine. The results of this study suggest that rifampin at the usual therapeutic doses has partial activity against blood stages of P. vivax in humans but that used alone it is insufficient for cure. Rifampin might therefore be of value in combination antimalarial therapy.

摘要

评估了利福平对60例间日疟原虫疟疾成年患者的抗疟效果。有三个治疗组:利福平组(分别按每日每公斤体重20毫克和15毫克给药,持续1天和4天;n = 5);利福平后接伯氨喹组(每日15毫克碱基,持续14天;n = 25),以及氯喹组(每公斤25毫克碱基,分3天给药)后接伯氨喹组(n = 30)。所有患者均住院至发热和寄生虫清除,45例患者住院1个月。尽管所有患者最初均退热,且每48小时生命周期内的寄生虫血症减少了≥6倍,但单用利福平无效:所有5例患者随后均出现类似R2的寄生虫学反应。所有接受利福平-伯氨喹治疗的患者均退热且寄生虫血症清除,但治疗反应比氯喹-伯氨喹治疗后慢。最终退热时间明显更长(平均值[标准差]= 43 [35] 小时对27 [19] 小时;P = 0.046),寄生虫清除时间(降至入院时寄生虫计数的50%和90%以及外周血涂片检测不到的水平)也明显更长(P = 0.053至<0.001)。然而,接受利福平-伯氨喹治疗的患者中只有1例再次出现感染。本研究结果表明,常用治疗剂量的利福平对人体间日疟原虫的血液阶段有部分活性,但单用不足以治愈。因此,利福平在联合抗疟治疗中可能有价值。

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本文引用的文献

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Antimalarial activity of rifampicin in vitro and in rodent models.利福平在体外和啮齿动物模型中的抗疟活性。
Trans R Soc Trop Med Hyg. 1993 Mar-Apr;87(2):211-6. doi: 10.1016/0035-9203(93)90497-e.
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Effects of antibiotics on Plasmodium falciparum in vitro.抗生素对恶性疟原虫的体外作用。
Am J Trop Med Hyg. 1983 Mar;32(2):221-5. doi: 10.4269/ajtmh.1983.32.221.
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Inhibition of rodent malaria in mice by rifampicin.
Nature. 1970 Jul 25;227(5256):381-2. doi: 10.1038/227381b0.
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Antimalarial effects of tetracyclines in man.
J Trop Med Hyg. 1971 Nov;74(11):238-42.

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