Global assessment of partial artemisinin resistance: Multicenter trial across Kenya, Peru, and Thailand in patients with uncomplicated Plasmodium falciparum malaria.

IF 4.8 2区医学 Q1 INFECTIOUS DISEASES

International Journal of Infectious Diseases Pub Date : 2025-07-02 DOI:10.1016/j.ijid.2025.107971

B Andagalu, E Smith, S Durand, H O Valdivia, I Onyango, M Spring, V Pattaraporn, G C Baldeviano, E Majid, S Sriwichai, J Cummings, L Tapia, H Akala, P Gosi, C Cabezas, D Juma, S Wongararunkochakorn, M Sihuincha, C Chaisatit, L Chebon, W Kuntawunginn, A Halbach, C Kodchakorn, C Thamnurak, C Praditpol, P Saingam, K A Edgel, D Saunders, A Cheruiyot, I Chuang, E Milgotina, P Fernandes, A G Lescano, N Boonyalai, E Kamau, B M Forshey, S Cinkovich, D Bethell, K Jongsakul, M Fukuda

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引用次数: 0

Abstract

Introduction: Artemisinin-resistant Plasmodium falciparum challenges the effectiveness of all artemisinin-based combination therapies.

Methods: We conducted a clinical study in Peru, Kenya, and Thailand between June 2013 and November 2015 in subjects treated with three standard doses of artesunate followed by two doses of mefloquine. The primary endpoint was parasite clearance half-life (PC_1/2) during the 72-hour period of treatment. Secondary endpoints included clinical outcome at 42 days, detection of kelch13 (K13) mutations, pharmacokinetics and pharmacodynamics.

Results: The mean PC_1/2 was higher in the Thai (4.1 hours) than Peruvian (2h) or Kenyan cohorts (2.2h) (p<0.0001). Higher PC_1/2 was partially explained by K13 mutations in 13 (28%) of 46 Thai subjects, including WHO validated and candidate mutations. Twelve (26%) Thai cohort subjects had PC_1/2≥5h with parasites from nine subjects carrying K13 mutations. There was an overall 42-day cure rate of 100% across all subjects.

Conclusions: This is the first concurrent evaluation of artemisinin resistance across three continents. The presence of 11% Thai subjects that satisfied WHO criteria for drug resistance establishes this area as endemic. Longer PC_1/2 found in wildtype and candidate K13 mutant infections within the Thai cohort require further investigation to identify alternative mechanisms of resistance.

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部分青蒿素耐药的全球评估：肯尼亚、秘鲁和泰国非并发症恶性疟原虫疟疾患者的多中心试验。

导论：耐青蒿素恶性疟原虫对所有以青蒿素为基础的联合疗法的有效性构成挑战。方法：2013年6月至2015年11月，我们在秘鲁、肯尼亚和泰国进行了一项临床研究，受试者分别服用了三剂量的青蒿琥酯和两剂量的甲氟喹。主要终点是72小时治疗期间的寄生虫清除半衰期（PC1/2）。次要终点包括42天的临床结果、kelch13 （K13）突变检测、药代动力学和药效学。结果：泰国人的平均PC1/2（4.1小时）高于秘鲁人（2小时）或肯尼亚人（2.2小时）（p1/2的部分原因是46名泰国受试者中有13名（28%）的K13突变，包括WHO验证的突变和候选突变）。12名（26%）泰国队列受试者PC1/2≥5h，来自9名携带K13突变的受试者的寄生虫。所有受试者的42天总体治愈率为100%。结论：这是首次同时对三大洲的青蒿素耐药性进行评估。11%的泰国受试者符合世卫组织耐药标准，确定该地区为流行地区。在泰国队列中的野生型和候选K13突变体感染中发现的更长的PC1/2需要进一步研究以确定替代的耐药机制。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

International Journal of Infectious Diseases 医学-传染病学

CiteScore

18.90

自引率

2.40%

发文量

1020

审稿时长

30 days

期刊介绍： International Journal of Infectious Diseases (IJID) Publisher: International Society for Infectious Diseases Publication Frequency: Monthly Type: Peer-reviewed, Open Access Scope: Publishes original clinical and laboratory-based research. Reports clinical trials, reviews, and some case reports. Focuses on epidemiology, clinical diagnosis, treatment, and control of infectious diseases. Emphasizes diseases common in under-resourced countries.