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印度尼西亚地区间恶性疟原虫和间日疟原虫分离株的耐药性。

Drug resistance of Plasmodium falciparum and Plasmodium vivax isolates in Indonesia.

机构信息

Graduate Program in Molecular Medicine, Faculty of Science, Mahidol University, Bangkok, 10400, Thailand.

Department of Molecular Tropical Medicine and Genetics, Faculty of Tropical Medicine, Mahidol University, Bangkok, Thailand.

出版信息

Malar J. 2022 Nov 28;21(1):354. doi: 10.1186/s12936-022-04385-2.

Abstract

This review article aims to investigate the genotypic profiles of Plasmodium falciparum and Plasmodium vivax isolates collected across a wide geographic region and their association with resistance to anti-malarial drugs used in Indonesia. A systematic review was conducted between 1991 and date. Search engines, such as PubMed, Science Direct, and Google Scholar, were used for articles published in English and Indonesian to search the literature. Of the 471 initially identified studies, 61 were selected for 4316 P. falciparum and 1950 P. vivax individual infections. The studies included 23 molecular studies and 38 therapeutic efficacy studies. K76T was the most common pfcrt mutation. K76N (2.1%) was associated with the haplotype CVMNN. By following dihydroartemisinin-piperaquine (DHA-PPQ) therapy, the mutant pfmdr1 alleles 86Y and 1034C were selected. Low prevalence of haplotype N86Y/Y184/D1246Y pfmdr1 reduces susceptibility to AS-AQ. SNP mutation pvmdr1 Y976F reached 96.1% in Papua and East Nusa Tenggara. Polymorphism analysis in the pfdhfr gene revealed 94/111 (84.7%) double mutants S108N/C59R or S108T/A16V in Central Java. The predominant pfdhfr haplotypes (based on alleles 16, 51, 59,108, 164) found in Indonesia were ANCNI, ANCSI, ANRNI, and ANRNL. Some isolates carried A437G (35.3%) or A437G/K540E SNPs (26.5%) in pfdhps. Two novel pfdhps mutant alleles, I588F/G and K540T, were associated with six pfdhps haplotypes. The highest prevalence of pvdhfr quadruple mutation (F57L/S58R/T61M/S117T) (61.8%) was detected in Papua. In pvdhps, the only polymorphism before and after 2008 was 383G mutation with 19% prevalence. There were no mutations in the pfk13 gene reported with validated and candidate or associated k13 mutation. An increased copy number of pfpm2, associated with piperaquine resistance, was found only in cases of reinfection. Meanwhile, mutation of pvk12 and pvpm4 I165V is unlikely associated with ART and PPQ drug resistance. DHA-PPQ is still effective in treating uncomplicated falciparum and vivax malaria. Serious consideration should be given to interrupt local malaria transmission and dynamic patterns of resistance to anti-malarial drugs to modify chemotherapeutic policy treatment strategies. The presence of several changes in pfk13 in the parasite population is of concern and highlights the importance of further evaluation of parasitic ART susceptibility in Indonesia.

摘要

这篇综述文章旨在研究在印度尼西亚广泛地理区域采集的恶性疟原虫(Plasmodium falciparum)和间日疟原虫(Plasmodium vivax)分离株的基因型谱及其与抗疟药物耐药性的关联。本研究进行了系统性综述,时间范围为 1991 年至当日。使用 PubMed、Science Direct 和 Google Scholar 等搜索引擎,对发表在英语和印度尼西亚语的文献进行了检索。在最初确定的 471 项研究中,有 61 项研究被选中,涉及 4316 例恶性疟原虫和 1950 例间日疟原虫个体感染。这些研究包括 23 项分子研究和 38 项治疗效果研究。K76T 是最常见的 pfcrt 突变。K76N(2.1%)与 CVMNN 单倍型相关。遵循双氢青蒿素-哌喹(DHA-PPQ)治疗后,选择了突变型 pfmdr1 等位基因 86Y 和 1034C。pfmdr1 等位基因 86Y/Y184/D1246Y 的低流行率降低了 AS-AQ 的敏感性。pvmdr1 Y976F 的 SNP 突变在巴布亚和东努沙登加拉达到 96.1%。在 pfdhfr 基因的多态性分析中,爪哇中部发现了 94/111(84.7%)双突变体 S108N/C59R 或 S108T/A16V。在印度尼西亚发现的主要 pfdhfr 单倍型(基于等位基因 16、51、59、108、164)是 ANCNI、ANCSI、ANRNI 和 ANRNL。一些分离株在 pfdhps 中携带 A437G(35.3%)或 A437G/K540E SNPs(26.5%)。两种新的 pfdhps 突变等位基因 I588F/G 和 K540T 与六个 pfdhps 单倍型相关。在巴布亚发现的 pvdhfr 四重突变(F57L/S58R/T61M/S117T)(61.8%)的流行率最高。在 pvdhps 中,2008 年前后唯一的多态性是 383G 突变,流行率为 19%。pfk13 基因没有报道与验证和候选或相关 k13 突变有关的突变。仅在再感染病例中发现与哌喹耐药相关的 pfpm2 拷贝数增加。同时,pvk12 和 pvpm4 I165V 的突变不太可能与 ART 和 PPQ 耐药性相关。DHA-PPQ 仍可有效治疗无并发症的恶性疟原虫和间日疟原虫疟疾。应认真考虑中断当地疟疾传播和抗疟药物耐药性的动态模式,以修改化学治疗政策治疗策略。寄生虫种群中 pfk13 的几种变化令人担忧,这突显了进一步评估印度尼西亚寄生虫对 ART 敏感性的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/06b8/9703795/867b53caf554/12936_2022_4385_Fig1_HTML.jpg

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