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大规莫青蒿琥酯-哌喹全民服药加或不加伯氨喹方案显著降低非洲高度流行区疟疾发病率。

Large-scale Artemisinin-Piperaquine Mass Drug Administration With or Without Primaquine Dramatically Reduces Malaria in a Highly Endemic Region of Africa.

机构信息

Institute of Tropical Medicine, People's Republic of China.

Science and Technology Park, Guangzhou University of Chinese Medicine, Guangdong, People's Republic of China.

出版信息

Clin Infect Dis. 2018 Nov 13;67(11):1670-1676. doi: 10.1093/cid/ciy364.

Abstract

BACKGROUND

Mass drug administration (MDA), with or without low-dose primaquine (PMQLD), is being considered for malaria elimination programs. The potential of PMQLD to block malaria transmission by mosquitoes must be balanced against liabilities of its use.

METHODS

Artemisinin-piperaquine (AP), with or without PMQLD, was administered in 3 monthly rounds across Anjouan Island, Union of Comoros. Plasmodium falciparum malaria rates, mortality, parasitemias, adverse events, and PfK13 Kelch-propeller gene polymorphisms were evaluated.

RESULTS

Coverage of 85 to 93% of the Anjouan population was achieved with AP plus PMQLD (AP+PMQLD) in 2 districts (population 97164) and with AP alone in 5 districts (224471). Between the months of April-September in both 2012 and 2013, average monthly malaria hospital rates per 100000 people fell from 310.8 to 2.06 in the AP+PMQLD population (ratio 2.06/310.8 = 0.66%; 95% CI: 0.02%, 3.62%; P = .00007) and from 412.1 to 2.60 in the AP population (ratio 0.63%; 95% CI: 0.11%, 1.93%; P < .00001). Effectiveness of AP+PMQLD was 0.9908 (95% CI: 0.9053, 0.9991), while effectiveness of AP alone was 0.9913 (95% CI: 0.9657, 0.9978). Both regimens were well tolerated, without severe adverse events. Analysis of 52 malaria samples after MDA showed no evidence for selection of PfK13 Kelch-propeller mutations.

CONCLUSIONS

Steep reductions of malaria cases were achieved by 3 monthly rounds of either AP+PMQLD or AP alone, suggesting potential for highly successful MDA without PMQLD in epidemiological settings such as those on Anjouan. A major challenge is to sustain and expand the public health benefits of malaria reductions by MDA.

摘要

背景

大规模药物治疗(MDA),联合或不联合低剂量伯氨喹(PMQLD),正被考虑用于消除疟疾项目。PMQLD 阻断蚊子传播疟疾的潜力必须与使用它的责任相平衡。

方法

在科摩罗联盟的昂儒昂岛,每月进行三轮青蒿素-哌喹(AP),联合或不联合 PMQLD。评估恶性疟原虫疟疾发病率、死亡率、寄生虫血症、不良事件和 PfK13 Kelch-propeller 基因突变。

结果

AP+PMQLD(AP+PMQLD)在 2 个区(人口 97164)和 AP 单独在 5 个区(人口 224471)覆盖了昂儒昂岛 85%至 93%的人口。在 2012 年 4 月至 9 月和 2013 年期间,AP+PMQLD 人群的平均每月疟疾医院发病率从每 100000 人 310.8 下降到 2.06(比率 2.06/310.8=0.66%;95%CI:0.02%,3.62%;P=0.00007),AP 人群从每 100000 人 412.1 下降到 2.60(比率 0.63%;95%CI:0.11%,1.93%;P<0.00001)。AP+PMQLD 的有效性为 0.9908(95%CI:0.9053,0.9991),而 AP 单独的有效性为 0.9913(95%CI:0.9657,0.9978)。两种方案均耐受良好,无严重不良事件。MDA 后对 52 份疟疾样本的分析未显示 PfK13 Kelch-propeller 突变选择的证据。

结论

通过每月三轮的 AP+PMQLD 或 AP 单独治疗,疟疾病例急剧减少,这表明在昂儒昂等流行病学环境下,无需 PMQLD 就可以进行高度成功的 MDA。一个主要的挑战是通过 MDA 维持和扩大疟疾减少带来的公共卫生效益。

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