氯喹用于圭亚那治疗无并发症的疟疾

J. Baird, T. Tiwari, G. J. Martin, C. Tamminga, T. Prout, J. Tjaden, P. Bravet, S. Rawlins, M. Ferrel, D. Carucci, S. Hoffman
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引用次数: 25

摘要

在圭亚那乔治城的一家公立医院,对44例有症状的经玻片确诊的疟疾患者给予标准氯喹治疗并随访28天。单纯感染恶性疟原虫(14例)、间日疟原虫(13例)、间日疟原虫(1例),或混合感染恶性疟原虫、间日疟原虫(17例),或混合感染恶性疟原虫、间日疟原虫和疟疾疟原虫(2例)。每只小鼠在第0天和第1天分别接受10 mg CQ碱/kg的监督治疗,第2天分别接受5 mg/kg的监督治疗。在入组当天(第0天),患者主诉发热(100%)、头痛(100%)、不适(94%)、肌痛(79%)、恶心(67%)、眩晕(49%)和呕吐(33%)。许多人(39%)病得只能卧床休息。在第4天,较少的受试者抱怨发烧(15%)、头痛(15%)、不适(6%)、肌痛(21%)、恶心(6%)、眩晕(24%)或呕吐(0%),尽管治疗失败的风险相对较高(>48%)。第4天,恶性疟原虫寄生虫学治疗失败的累计发生率为15%,第7天和第14天分别为33%和48%。所有间日疟原虫和疟疾疟原虫感染在第4天前消失,第7天无复发。两例间日疟原虫感染后来复发(第14或28天),但在CQ加去乙基氯喹的全血浓度不足(即<100 ng/ml)的情况下。综上所述,这些结果表明CQ对恶性疟原虫治疗失败的风险很高,但也表明圭亚那间日疟原虫对CQ的耐药性很少发生。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Chloroquine for the treatment of uncomplicated malaria in Guyana
Abstract At a public hospital in Georgetown, Guyana, 44 patients seeking treatment for symptomatic, slide-confirmed malaria were given standard chloroquine (CQ) therapy and followed for 28 days. The patients apparently had pure infections with Plasmodium falciparum (14), P. vivax (13) or P. malariae (one), or mixed infections either of P. falciparum and P. vivax (17) or of P. falciparum, P. malariae and P. vivax (two). Each received supervised treatment with 10 mg CQ base/kg on each of days 0 and 1, and 5 mg/kg on day 2. On the day of enrollment (day 0), the patients complained of fever (100%), headache (100%), malaise (94%), myalgia (79%), nausea (67%), vertigo (49%) and vomiting (33%). Many (39%) were ill enough to confine themselves to bed. On day 4, fewer of the subjects complained of fever (15%), headache (15%), malaise (6%), myalgia (21%), nausea (6%), vertigo (24%) or vomiting (0%) despite the relatively high (>48%) risk of therapeutic failure. The cumulative incidence of parasitological failure against P. falciparum was 15% at day 4, 33% at day 7 and 48% at day 14. All of the P. vivax and P. malariae infections cleared before day 4 and none recurred by day 7. Two infections with P. vivax recurred later (on day 14 or 28) but in the presence of less than adequate, whole-blood concentrations of CQ plus desethyl-chloroquine (i.e. <100 ng/ml). Taken together, the results indicate a high risk of therapeutic failure of CQ against P. falciparum but also indicate that resistance to CQ in P. vivax occurs infrequently in Guyana.
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