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甲氟喹在子孢子诱导的人类疟疾中的抑制活性。

Suppressive activity of mefloquine in sporozoite-induced human malaria.

作者信息

Clyde D F, McCarthy V C, Miller R M, Hornick R B

出版信息

Antimicrob Agents Chemother. 1976 Mar;9(3):384-6. doi: 10.1128/AAC.9.3.384.

Abstract

Mefloquine hydrochloride [WR 142,490; alpha-(2-piperidyl)-2,8-bis(trifluoromethyl)-4-quinolinemethanol hydrochloride] was tested for suppressive effect on sporozoite-induced malaria in nonimmune volunteers living in an area where malaria is not naturally transmitted. Single doses of 250 mg were given at weekly intervals, 500 mg at intervals of 2 weeks and 1,000 mg at intervals of 4 weeks, to men bitten by 10 to 15 mosquitoes heavily infected with a chloroquine- and pyrimethamine-resistant strain of Plasmodium falciparum. None of the individuals so treated developed infections during the period of drug delivery or during the follow-up period of 60 days. Doses of 250 or 500 mg produced no adverse reactions; mild epigastric discomfort occurred in all three men given 1,000 mg. Sporozoite-induced P. vivax infections were suppressed by single doses of 250 mg of mefloquine given at weekly intervals, but malaria developed after completion of the course. At treatment intervals longer than 1 week, vivax malaria was not suppressed.

摘要

对居住在疟疾非自然传播地区的非免疫志愿者,测试了盐酸甲氟喹[WR 142,490;α-(2-哌啶基)-2,8-双(三氟甲基)-4-喹啉甲醇盐酸盐]对疟原虫诱导的疟疾的抑制作用。对被10至15只感染了对氯喹和乙胺嘧啶耐药的恶性疟原虫株的蚊子叮咬的男性,分别按每周一次给予250毫克单剂量、每两周一次给予500毫克单剂量以及每四周一次给予1000毫克单剂量。在给药期间或60天的随访期内,接受如此治疗的个体均未发生感染。250毫克或500毫克剂量未产生不良反应;接受1000毫克剂量的所有三名男性均出现轻度上腹部不适。每周一次给予250毫克单剂量的甲氟喹可抑制疟原虫诱导的间日疟感染,但疗程结束后疟疾仍会发生发展。在治疗间隔超过1周时,间日疟未得到抑制。

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Mefloquine for preventing malaria during travel to endemic areas.甲氟喹用于在前往疟疾流行地区旅行期间预防疟疾。
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