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WR182393(一种脒腙)对猕猴体内食蟹猴疟原虫的病因预防和根治活性。

Causal prophylactic and radical curative activity of WR182393 (a guanylhydrazone) against Plasmodium cynomolgi in Macaca mulatta.

作者信息

Corcoran K D, Hansukjariya P, Sattabongkot J, Ngampochjana M, Edstein M D, Smith C D, Shanks G D, Milhous W K

机构信息

Department of Veterinary Medicine, Armed Forces Research Institute of Medical Sciences, Bangkok, Thailand.

出版信息

Am J Trop Med Hyg. 1993 Oct;49(4):473-7. doi: 10.4269/ajtmh.1993.49.473.

DOI:10.4269/ajtmh.1993.49.473
PMID:8214277
Abstract

Primaquine is the only currently available drug effective against persistent tissue stages of relapsing malaria in humans. Causal prophylactic and radical curative properties of WR182393 (a guanylhydrazone) were investigated as part of an effort to evaluate alternatives to primaquine in the rhesus monkey (Macaca mulatta)/Plasmodium cynomolgi test model. The drug was suspended in dimethylsulfoxide for intramuscular (im) injection. A pilot study indicated causal prophylactic activity in a regimen of 40 mg base/kg/day im for three days beginning the day before intravenous challenge with 1 x 10(6) P. cynomolgi sporozoites. Regimens of 31, 10, 3.1, and 0 mg base/kg/day im for three days were then tested in groups of two monkeys given a similar challenge. The two animals given 31 mg base/kg/day remained parasite-free. Average time to parasitemia for the lower dosage groups was 38, 18, and 8 days respectively. Groups of two monkeys with sporozoite-induced P. cynomolgi infections were also treated for seven days with 31, 10, 3.1, and 0 mg base/kg/day im in combination with 10 mg base/kg/day of chloroquine orally. Both monkeys given 31 mg base/kg/day did not relapse. The average time to relapse following treatment was 48, 29, and 8 days, respectively, for the lower dosage groups. Compound WR182393 is the first non-8-aminoquinoline class of drug to exhibit both causal prophylactic and radical curative properties against a relapsing primate, vivax-like malaria.

摘要

伯氨喹是目前唯一可有效对抗人类复发性疟疾持续性组织期的药物。作为在恒河猴(猕猴)/食蟹猴疟原虫试验模型中评估伯氨喹替代药物工作的一部分,对WR182393(一种脒腙)的病因性预防和根治特性进行了研究。该药物悬浮于二甲基亚砜中用于肌肉注射。一项初步研究表明,在静脉注射1×10⁶食蟹猴疟原虫子孢子前一天开始,以40毫克碱基/千克/天的剂量进行为期三天的肌肉注射方案具有病因性预防活性。然后,在两组接受类似攻击的两只猴子中测试了31、10、3.1和0毫克碱基/千克/天的剂量方案,为期三天。给予31毫克碱基/千克/天的两只动物未出现寄生虫。较低剂量组出现寄生虫血症的平均时间分别为38天、18天和8天。两组由子孢子诱导感染食蟹猴疟原虫的猴子也分别以31、10、3.1和0毫克碱基/千克/天的剂量进行为期七天的肌肉注射,并口服10毫克碱基/千克/天的氯喹。给予31毫克碱基/千克/天的两只猴子均未复发。较低剂量组治疗后复发的平均时间分别为48天、29天和8天。化合物WR182393是首个对复发性灵长类间日疟样疟疾同时具有病因性预防和根治特性的非8-氨基喹啉类药物。

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