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Molecular Evidence of Increased Resistance to Anti-Folate Drugs in Plasmodium falciparum in North-East India: A Signal for Potential Failure of Artemisinin Plus Sulphadoxine-Pyrimethamine Combination Therapy

机译:在印度东北部恶性疟原虫中抗叶酸药物耐药性增强的分子证据:青蒿素加磺胺嘧啶-乙胺嘧啶联合治疗潜在失败的信号

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摘要

North-east India, being a corridor to South-east Asia, is believed to play an important role in transmitting drug resistant Plasmodium falciparum malaria to India and South Asia. North-east India was the first place in India to record the emergence of drug resistance to chloroquine as well as sulphadoxine/pyrimethamine. Presently chloroquine resistance is widespread all over the North-east India and resistance to other anti-malarials is increasing. In this study both in vivo therapeutic efficacy and molecular assays were used to screen the spectrum of drug resistance to chloroquine and sulphadoxine/pyrimethamine in the circulating P. falciparum strains. A total of 220 P. falciparum positives subjects were enrolled in the study for therapeutic assessment of chloroquine and sulphadoxine/pyrimethamine and assessment of point mutations conferring resistances to these drugs were carried out by genotyping the isolates following standard methods. Overall clinical failures in sulphadoxine/pyrimethamine and chloroquine were found 12.6 and 69.5% respectively, while overall treatment failures recorded were 13.7 and 81.5% in the two arms. Nearly all (99.0%) the isolates had mutant pfcrt genotype (76T), while 68% had mutant pfmdr-1 genotype (86Y). Mutation in dhps 437 codon was the most prevalent one while dhfr codon 108 showed 100% mutation. A total of 23 unique haplotypes at the dhps locus and 7 at dhfr locus were found while dhps-dhfr combined loci revealed 49 unique haplotypes. Prevalence of double, triple and quadruple mutations were common while 1 haplotype was found with all five mutated codons (>F/AGEGS/T) at dhps locus. Detection of quadruple mutants (51I/59R/108N/164L) in the present study, earlier recorded from Car Nicobar Island, India only, indicates the presence of high levels of resistance to sulphadoxine/pyrimethamine in north-east India. Associations between resistant haplotypes and the clinical outcomes and emerging resistance in sulphadoxine/pyrimethamine in relation to the efficacy of the currently used artemisinin combination therapy are discussed.
机译:印度东北部是通往东南亚的走廊,据信在将耐药性恶性疟原虫疟疾传播到印度和南亚方面发挥了重要作用。印度东北部是印度第一个记录对氯喹以及磺胺多辛/乙胺嘧啶产生抗药性的地方。目前,氯喹的抗药性在印度东北部广泛分布,对其他抗疟疾药的抗药性也在增加。在这项研究中,体内治疗功效和分子测定均用于筛选循环恶性疟原虫菌株对氯喹和磺胺多辛/乙胺嘧啶的耐药性谱。共有220名恶性疟原虫阳性受试者参加了研究,以进行氯喹和磺胺多辛/乙胺嘧啶的治疗性评估,并通过按照标准方法对分离物进行基因分型来评估赋予这些药物耐药性的点突变。磺胺多辛/乙胺嘧啶和氯喹的总体临床失败率分别为12.6和69.5%,而两组的总治疗失败率分别为13.7和81.5%。几乎所有菌株(99.0%)都具有突变pfcrt基因型(76T),而68%菌株具有突变pfmdr-1基因型(86Y)。 dhps 437密码子的突变是最普遍的突变,而dhfr密码子108的突变为100%。在dhps位点共有23个独特的单倍型,在dhfr位点共有7个,而dhps-dhfr组合位点揭示了49个独特的单倍型。双重,三重和四重突变的患病率很普遍,而在dhps基因座上发现了所有五个突变密码子(> F / AGEGS / T )的1个单倍型。在本研究中检测到四个突变体(51I / 59R / 108N / 164L),较早时仅从印度的汽车尼科巴岛记录,表明在印度东北部对磺胺多辛/乙胺嘧啶有较高水平的抗性。讨论了抗性单倍型与临床结果和磺胺多辛/乙胺嘧啶新出现的抗性之间的关联,这些抗性与目前使用的青蒿素联合疗法的疗效有关。

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