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relapse 复燃;复发;重现;(使)再次陷入 Papua New Guinea 巴布亚新几内亚 Plasmodium vivax 间日疟原虫 contribute significantly to 对……有显著贡献;显著促成;对……作用重大 disease 疾病;弊端;不安

Relapses contribute significantly to the risk of Plasmodium vivax infection and disease in Papua New Guinean children 1-5 years of age.

机构信息

Papua New Guinea Institute of Medical Research, Madang, Papua New Guinea.

出版信息

J Infect Dis. 2012 Dec 1;206(11):1771-80. doi: 10.1093/infdis/jis580. Epub 2012 Sep 10.

Abstract

BACKGROUND

Plasmodium vivax forms long-lasting hypnozoites in the liver. How much they contribute to the burden of P. vivax malaria in children living in highly endemic areas is unknown.

METHODS

In this study, 433 Papua New Guinean children aged 1-5 years were Randomized to receive artesunate (7 days) plus primaquine (14 days), artesunate alone or no treatment and followed up actively for recurrent Plasmodium infections and disease for 40 weeks.

RESULTS

Treatment with artesunate-primaquine reduced the risk of P. vivax episodes by 28% (P = .042) and 33% (P = .015) compared with the artesunate and control arms, respectively. A significant reduction was observed only in the first 3 months of follow-up (artesunate-primaquine vs control, -58% [P = .004]; artesunate-primaquine vs artesunate, -49% [P = .031]) with little difference thereafter. Primaquine treatment also reduced the risk of quantitative real-time polymerase chain reaction- and light microscopy-positive P. vivax reinfections by 44% (P < .001) and 67% (P < .001), respectively. Whereas primaquine treatment did not change the risk of reinfection with Plasmodium falciparum, fewer P. falciparum clinical episodes were observed in the artesunate-primaquine arm.

CONCLUSIONS

Hypnozoites are an important source of P. vivax infection and contribute substantially to the high burden of P. vivax disease observed in young Papua New Guinean children. Even in highly endemic areas with a high risk of reinfection, antihypnozoite treatment should be given to all cases with parasitologically confirmed P. vivax infections.

摘要

背景

间日疟原虫在肝脏中形成持久的休眠子。在高度流行地区生活的儿童中,休眠子对间日疟原虫疟疾负担的贡献有多大尚不清楚。

方法

本研究中,433 名巴布亚新几内亚儿童(年龄 1-5 岁)被随机分为接受青蒿琥酯(7 天)加伯氨喹(14 天)、青蒿琥酯单药或不治疗,并在 40 周内积极随访复发性疟原虫感染和疾病。

结果

与青蒿琥酯和对照组相比,青蒿琥酯-伯氨喹治疗分别降低了 28%(P =.042)和 33%(P =.015)的间日疟原虫发作风险。仅在随访的前 3 个月观察到显著降低(青蒿琥酯-伯氨喹与对照组相比,-58% [P =.004];青蒿琥酯-伯氨喹与青蒿琥酯相比,-49% [P =.031]),此后差异较小。伯氨喹治疗还降低了定量实时聚合酶链反应和显微镜阳性间日疟原虫再感染的风险,分别为 44%(P <.001)和 67%(P <.001)。虽然伯氨喹治疗并未改变恶性疟原虫感染的再感染风险,但青蒿琥酯-伯氨喹组观察到的恶性疟原虫临床发作次数较少。

结论

休眠子是间日疟原虫感染的重要来源,对巴布亚新几内亚年轻儿童中观察到的高负担的间日疟原虫疾病有很大贡献。即使在高度流行地区再感染风险很高的情况下,也应给予所有寄生虫学证实的间日疟原虫感染病例抗休眠子治疗。

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