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首页> 外文期刊>Tropical Medicine and International Health: TM and IH >Plasmodium falciparum: correlation of in vivo resistance to chloroquine and antifolates with genetic polymorphisms in isolates from the south of Lao PDR.
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Plasmodium falciparum: correlation of in vivo resistance to chloroquine and antifolates with genetic polymorphisms in isolates from the south of Lao PDR.

机译:恶性疟原虫:老挝人民民主共和国南部分离物中对氯喹和抗叶酸药物的体内抗性与遗传多态性的关系。

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摘要

Levels of drug resistance of Plasmodium falciparum strains against antimalarials have increased in Laos. In several studies, chloroquine (CQ) resistance has been associated with point mutations in the Pfcrt and pfmdr genes, and sulphadoxine/pyrimethamine (S/P) resistance with point mutations in the genes of dihydrofolate reductase (DHFR) and dihydropteroate synthetase (DHPS). We combined a study of these molecular markers with an in vivo antimalarial drug sensitivity study in Attapeu province in the south of Lao PDR. We treated 100 patients with either CQ, S/P or a combination of both. In the CQ group, Pfcrt mutations showed a very high sensitivity (100%) but a low specificity (12.5%) to predict resistance. The combination of mutations in the Pfcrt and pfmdr genes was highly specific and had a positive predictive value of 100%. Mutations in the DHPS gene showed a high correlation with the development of resistance. The prevalence of mutations in the DHFR gene, especially codon 108 Asn, was predictive with high sensitivity (100%) but low specificity. Isolates derived from patients treated with a combination of both drugs showed a high correlation between the mutation in codon 437 of DHPS gene and in vivo-resistance (odds ratio 16.00, CI). The study provides evidence for the existence of antimalarial drug resistance in the south of Lao PDR, and offers a molecular method to predict resistance.
机译:老挝恶性疟原虫菌株对抗疟药的耐药性水平有所提高。在几项研究中,氯喹(CQ)耐药与Pfcrt和pfmdr基因的点突变有关,而磺胺多辛/乙胺嘧啶(S / P)耐药与二氢叶酸还原酶(DHFR)和二氢蝶呤合成酶(DHPS)基因的点突变相关。 。我们将这些分子标记物的研究与在老挝人民民主共和国南部的Attapeu省的体内抗疟药敏感性研究相结合。我们用CQ,S / P或两者结合治疗了100例患者。在CQ组中,Pfcrt突变显示出很高的灵敏度(100%),但是低特异性(12.5%)来预测耐药性。 Pfcrt和pfmdr基因突变的组合具有很高的特异性,阳性预测值为100%。 DHPS基因的突变与耐药性的发展高度相关。 DHFR基因,特别是密码子108 Asn突变的发生率具有高灵敏度(100%)但特异性低的预测。两种药物联合治疗的患者分离株显示DHPS基因第437位密码子突变与体内抗药性高度相关(优势比16.00,CI)。该研究为老挝人民民主共和国南部存在抗疟药耐药性提供了证据,并提供了预测耐药性的分子方法。

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