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2014年,蒿甲醚-本芴醇和青蒿琥酯-阿莫地喹在马拉维治疗非复杂性恶性疟原虫疟疾的体内疗效。

In vivo efficacy of artemether-lumefantrine and artesunate-amodiaquine for uncomplicated Plasmodium falciparum malaria in Malawi, 2014.

作者信息

Paczkowski Magdalena, Mwandama Dyson, Marthey Daniel, Luka Madalitso, Makuta Georgina, Sande John, Ali Doreen, Troell Peter, Mathanga Don P, Gutman Julie

机构信息

Malaria Branch, Division of Parasitic Diseases & Malaria, Center for Global Health, Centers for Disease Control and Prevention, 1600 Clifton Rd. NE, Mailstop A06, Atlanta, GA, 30329-4027, USA.

Malaria Alert Centre, University of Malawi College of Medicine, Blantyre, Malawi.

出版信息

Malar J. 2016 Apr 26;15:236. doi: 10.1186/s12936-016-1281-y.

Abstract

BACKGROUND

Malaria causes significant morbidity in Malawi, with an estimated 5 million cases in 2014. Artemether-lumefantrine (AL) and artesunate-amodiaquine (ASAQ) are the first- and second-line treatments for uncomplicated malaria, respectively, but emerging resistance threatens their efficacy. In order to understand whether AL and ASAQ remain efficacious for the treatment of uncomplicated Plasmodium falciparum malaria in Malawi, a therapeutic efficacy trial was conducted.

METHODS

During March-July 2014, febrile children aged 6-59 months with microscopy-confirmed uncomplicated P. falciparum malaria (1000-200,000 parasites/μL) were enrolled in a 28-day randomized in vivo efficacy trial at three sites: one each in northern (Karonga), central (Nkhotakota) and southern (Machinga) Malawi. The study was powered to estimate site-specific efficacy for AL and overall efficacy for ASAQ, with 3:1 randomization to AL or ASAQ. Blood was collected for malaria microscopy and molecular testing on days 0-3, 7, 14, 21, and 28. Recrudescence and reinfection were differentiated using polymerase chain reaction (PCR) genotyping of merozoite surface protein. The primary outcome was the PCR-corrected day 28 Kaplan-Meier cumulative success rate.

RESULTS

A total of 452 children were enrolled; 303/338 (89 %) and 98/114 (86 %) reached a study endpoint in AL and ASAQ arms, respectively. All treatment failures occurred after day 3. The day 28 uncorrected cumulative success rate was 97.1 % (95 % confidence interval [CI]: 93.9-100 %) for ASAQ and 76.8 % (95 % CI 72.1-81.5 %) for AL, with 82.5 % (95 % CI 75.4-89.7 %), 69 % (95 % CI 59.9-78.1 %), and 78.2 % (95 % CI 70.2-86.3 %) success in the northern, central, and southern regions, respectively. The day 28 PCR-corrected cumulative success rate was 99 % (95 % CI 97.2-100 %) in the ASAQ arm and 99.3 % (95 % CI 98.3-100 %) in the AL arm, with 98-100 % efficacy in each site.

CONCLUSIONS

As evidenced by the day 28 PCR-corrected cumulative success rates, both AL and ASAQ remain efficacious treatments for uncomplicated malaria in Malawi. The lower uncorrected efficacy in the AL arm compared to ASAQ may be explained by the shorter half-life of lumefantrine (3-6 days) compared to amodiaquine (9-18 days). The high reinfection rate suggests that there is a continued need to scale-up effective malaria prevention interventions.

摘要

背景

疟疾在马拉维导致了严重的发病情况,2014年估计有500万病例。蒿甲醚-本芴醇(AL)和青蒿琥酯-阿莫地喹(ASAQ)分别是单纯性疟疾的一线和二线治疗药物,但新出现的耐药性威胁到了它们的疗效。为了了解AL和ASAQ在马拉维治疗单纯性恶性疟原虫疟疾是否仍然有效,进行了一项治疗效果试验。

方法

在2014年3月至7月期间,年龄在6至59个月、经显微镜确诊为单纯性恶性疟原虫疟疾(1000 - 200,000个寄生虫/微升)的发热儿童,在马拉维北部(卡龙加)、中部(恩科塔科塔)和南部(马钦加)的三个地点参加了一项为期28天的随机体内疗效试验。该研究旨在估计AL的特定地点疗效和ASAQ的总体疗效,随机分为AL或ASAQ的比例为3:1。在第0 - 3天、7天、14天、21天和28天采集血液进行疟疾显微镜检查和分子检测。使用裂殖子表面蛋白的聚合酶链反应(PCR)基因分型来区分复发和再感染。主要结局是第28天经PCR校正的Kaplan-Meier累积成功率。

结果

共纳入452名儿童;在AL组和ASAQ组中分别有303/338(89%)和98/114(86%)达到研究终点。所有治疗失败均发生在第3天之后。第28天未校正的累积成功率,ASAQ组为97.1%(95%置信区间[CI]:93.9 - 100%),AL组为76.8%(95%CI 72.1 - 81.5%),北部、中部和南部地区的成功率分别为82.5%(95%CI 75.4 - 89.7%)、69%(95%CI 59.9 - 78.1%)和78.2%(95%CI 70.2 - 86.3%)。第28天经PCR校正的累积成功率,ASAQ组为99%(95%CI 97.2 - 100%),AL组为99.3%(95%CI 98.3 - 100%),每个地点的疗效均为98 - 100%。

结论

第28天经PCR校正的累积成功率表明,AL和ASAQ在马拉维治疗单纯性疟疾仍然有效。与ASAQ相比,AL组未校正的疗效较低,这可能是因为本芴醇的半衰期(3 - 6天)比阿莫地喹(9 - 18天)短。再感染率高表明仍需要扩大有效的疟疾预防干预措施。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fb92/4845327/5b6fc4855894/12936_2016_1281_Fig1_HTML.jpg

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