2017 年塞内加尔南部地区治疗失败患者中与耐药性相关的恶性疟原虫遗传标记。

International journal of molecular epidemiology and genetics Pub Date : 2024-06-15 eCollection Date: 2024-01-01 DOI:10.62347/RWLA6562
Magatte Ndiaye, Malick Diouf, Moufid Mhamadi, Aicha Djigal, Isaac A Manga, Coumba Sene, Souleye Lelo, Cheikh B Fall, Khadime Sylla, Babacar Faye
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引用次数: 0

摘要

青蒿素综合疗法(ACT)是最有效的抗疟疗法。针对东南亚地区出现的青蒿素综合疗法抗药性疟原虫,世界卫生组织(WHO)建议对青蒿素综合疗法和其他抗疟药物的疗效进行持续监测。为了满足这一需求,我们在 2017 年进行了一项为期 42 天的药物疗效试验,评估青蒿琥酯加阿莫地喹(ASAQ)、蒿甲醚加鲁胺蒽醌(AL)和双氢青蒿素加哌喹(DHAPQ)对单纯恶性疟原虫疟疾的疗效,期间收集了疟疾患者的干血斑。在患者首次服用 ACT 之前的第 0 天以及出现复发性寄生虫血症的任何一天采集血样。对原生动物表面蛋白1(MSP1)和原生动物表面蛋白2(MSP2)等遗传标记进行了基因分型,以区分复发和再感染病例。此外,还利用 PCR 单特异性寡核苷酸探针结合-ELISA 平台(PCR-SSOP-ELISA)和 PCR-RFLP 技术分别鉴定了与氯喹和阿莫地喹耐药性相关的 Pfcrt 72-76 突变单倍型和 Pfmdr1_86Y 等位基因。在参与研究的 320 名患者中,只有 43 人(13.43%)复发。经 PCR 校正后,我们的分析显示有 13 名患者复发感染,其中 ASAQ 组 8 人,AL 组 5 人,DHAPQ 组无。值得注意的是,没有观察到早期治疗失败(治疗头 3 天内),所有复发都发生在第 21 天到第 42 天之间。Pfcrt 野生型单倍型 CVMNK 和 Pfmdr N86 等位基因的流行率分别为 67.03% 和 97.70%。相比之下,突变型 CVIET 和 86Y 的发病率分别为 32.97% 和 2.3%。CVMNK 野生单倍型的高流行率表明寄生虫对氯喹仍然敏感,而 86Y 突变体的低流行率表明阿莫地喹仍然有效。此外,表现出 CVIET 和 86Y 组合的菌株发生率较低,这表明使用多种抗疟药对抗药性控制很有价值。值得注意的是,复发病例中没有一例携带 86Y 突变或 86Y 和 CVIET 组合。
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P. falciparum genetic markers associated with drug resistance from patients with treatment failure in the Southern part of Senegal in 2017.

Artemisinin Combination Therapies (ACT) stand as the most potent antimalarial treatments. In response to the emergence of ACT-resistant malaria parasites in Southeast Asia, the World Health Organization (WHO) has recommended continuous monitoring of the effectiveness of ACT and other antimalarials. To address this need, we collected dried blood spots from malaria patients during a 42-days drug efficacy trial evaluating the efficacy of Artesunate plus Amodiaquine (ASAQ), Artemether Plus Lumefantrine (AL) and Dihydroarthemisinine plus Piperaquine (DHAPQ) on simple P. falciparum malaria in 2017. Blood samples were collected on Day 0, prior to the patients' initial ACT dose, and on any days of recurrent parasitemia. Genetic markers such as Merozoite Surface Protein 1 (MSP1) and Merozoite Surface Protein 2 (MSP2) were genotyped to differentiate between recrudescence and re-infestation cases. Furthermore, PCR Single Specific Oligonucleotide Probes combined with-ELISA platform (PCR-SSOP-ELISA) and PCR-RFLP techniques were used to identify Pfcrt 72-76 mutant haplotype and Pfmdr1_86Y allele associated with chloroquine and amodiaquine resistance, respectively. Out of the 320 patients enrolled in the study, only 43 (13.43%) experienced relapses. Upon PCR correction, our analysis revealed that recrudescent infections affected 13 patients, with 8 in the ASAQ group, 5 in the AL group, and none in the DHAPQ group. Notably, no early treatment failures (within the first 3 days of treatment) were observed, and all recurrences occurred between Day 21 and Day 42. The prevalence of the Pfcrt wild-type haplotype CVMNK and Pfmdr N86 allele was 67.03% and 97.70%, respectively. In contrast, the mutant types CVIET and 86Y were found at 32.97% and 2.3%, respectively. The high prevalence of the CVMNK wild haplotype suggests that the parasites remain sensitive to chloroquine, while the low prevalence of the 86Y mutants indicates continued effectiveness of amodiaquine. Furthermore, the low prevalence of strains exhibiting the combination of CVIET and 86Y suggests that the use of multiple antimalarials is valuable for resistance control. Notably, none of the relapse cases carried the 86Y mutation or the combination of 86Y and CVIET.

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