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配子体动力学和药物在降低间日疟传播潜能中的作用。

Gametocyte dynamics and the role of drugs in reducing the transmission potential of Plasmodium vivax.

机构信息

Global Health Division, Menzies School of Health Research, Charles Darwin University, Darwin 0811, Australia.

出版信息

J Infect Dis. 2013 Sep 1;208(5):801-12. doi: 10.1093/infdis/jit261. Epub 2013 Jun 12.

Abstract

BACKGROUND

Designing interventions that will reduce transmission of vivax malaria requires knowledge of Plasmodium vivax gametocyte dynamics.

METHODS

We analyzed data from a randomized controlled trial in northwestern Thailand and 2 trials in Papua, Indonesia, to identify and compare risk factors for vivax gametocytemia at enrollment and following treatment.

RESULTS

A total of 492 patients with P. vivax infections from Thailand and 476 patients (162 with concurrent falciparum parasitemia) from Indonesia were evaluable. Also, 84.3% (415/492) and 66.6% (209/314) of patients with monoinfection were gametocytemic at enrollment, respectively. The ratio of gametocytemia to asexual parasitemia did not differ between acute and recurrent infections (P = .48 in Thailand, P = .08 in Indonesia). High asexual parasitemia was associated with an increased risk of gametocytemia during follow-up in both locations. In Thailand, the cumulative incidence of gametocytemia between day 7 and day 42 following dihydroartemisinin + piperaquine (DHA + PIP) was 6.92% vs 29.1% following chloroquine (P < .001). In Indonesia, the incidence of gametocytemia was 33.6% following artesunate + amodiaquine (AS + AQ), 7.42% following artemether + lumefantrine, and 6.80% following DHA + PIP (P < .001 for DHA + PIP vs AS + AQ).

CONCLUSIONS

P. vivax gametocyte carriage mirrors asexual-stage infection. Prevention of relapses, particularly in those with high asexual parasitemia, is likely the most important strategy for interrupting P. vivax transmission.

摘要

背景

设计降低间日疟传播的干预措施需要了解间日疟原虫配子体动力学。

方法

我们分析了来自泰国西北部的一项随机对照试验和印度尼西亚巴布亚的 2 项试验的数据,以确定并比较在入组时和治疗后发生间日疟配子体血症的风险因素。

结果

共有来自泰国的 492 例间日疟感染患者和来自印度尼西亚的 476 例患者(162 例伴有同期恶性疟原虫寄生虫血症)可进行评估。此外,分别有 84.3%(415/492)和 66.6%(209/314)的单纯感染患者在入组时具有配子体血症。急性和复发性感染之间的配子体血症与无性体寄生虫血症的比值无差异(泰国 P =.48,印度尼西亚 P =.08)。高无性体寄生虫血症与两地随访期间配子体血症的风险增加相关。在泰国,二氢青蒿素+哌喹(DHA+PIP)后第 7 天至第 42 天的配子体血症累积发生率为 6.92%,而氯喹后为 29.1%(P<0.001)。在印度尼西亚,青蒿琥酯+阿莫地喹(AS+AQ)后配子体血症的发生率为 33.6%,青蒿素+甲氟喹后为 7.42%,DHA+PIP 后为 6.80%(DHA+PIP 与 AS+AQ 相比,P<0.001)。

结论

间日疟原虫配子体携带与无性体感染相吻合。预防复发,特别是对高无性体寄生虫血症患者,可能是阻断间日疟传播的最重要策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d954/3733516/71c867326008/jit26101.jpg

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