首页> 外文期刊>Acta tropica: Journal of Biomedical Sciences >Genetic polymorphisms of candidate markers and in vitro susceptibility of Plasmodium falciparum isolates from Thai-Myanmar border in relation to clinical response to artesunate-mefloquine combination
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Genetic polymorphisms of candidate markers and in vitro susceptibility of Plasmodium falciparum isolates from Thai-Myanmar border in relation to clinical response to artesunate-mefloquine combination

机译:泰缅边境恶性疟原虫分离株候选标记的遗传多态性及其对青蒿琥酯-甲喹喹组合临床反应的敏感性

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摘要

The genetic polymorphisms of the candidate markers of antimalariaS drug resistance pfcrt, pfmdrl,pfatp6, and pfmrpl were investigated in relationship with in vitro susceptibility of Plasmodium falciparum isolates and clinical response following artesunate (AS)-mefloquine (MQ) combination in 21 and 27 samples obtained from patients with recrudescence and adequate clinical response, respectively. MQ.(21.0 vs. 49.9 nM) and AS (1.6 vs. 2.8 nM) IC50 values (concentrations that inhibit parasite growth by 50%) were significantly higher in isolates collected from patients with recrudescence. Furthermore, a significantly higher MQ.IC50 was found in isolates from patients with recrudescence that carried pfmrpl mutations at amino acid residues 191Y, 437A, and 876V. For AS sensitivity, a significant association was also detected in isolates from patients with recrudescence that carried gene mutations at amino acid residues 437A and 876V. MQ. IC50 of the isolates with recrudescence which carried >4 pfmdrl gene copies was significantly higher than that carrying only one gene copy. In addition, a significantly higher proportion of isolates carrying one gene copy was detected in the group with adequate clinical response compared with recrudescence. Results from this limited sample size suggested the potential link between pfmdrl gene copy number and pfmrpl gene mutation, in vitro parasite susceptibility, and AS-MQ. treatment response.
机译:在21和27个样品中,研究了抗疟疾候选药物pfcrt,pfmdrl,pfatp6和pfmrpl的候选标记的遗传多态性与恶性疟原虫分离株的体外药敏性以及青蒿琥酯(AS)-甲氟喹(MQ)联合使用后的临床反应之间的关系。分别从复发性和有足够临床反应的患者中获得。从复发患者收集的分离物中,MQ。(21.0 vs. 49.9 nM)和AS(1.6 vs. 2.8 nM)IC50值(抑制寄生虫生长50%的浓度)显着更高。此外,在复发患者的分离株中发现了更高的MQ.IC50,该分离株在191Y,437A和876V氨基酸残基处携带pfmrpl突变。对于AS敏感性,还从复发患者的分离物中检测到显着关联,这些患者在437A和876V氨基酸残基处携带基因突变。 MQ。携带> 4 pfmdrl基因拷贝的复发性分离株的IC50显着高于仅携带一个基因拷贝的IC50。此外,与复发相比,在具有足够临床反应的组中检测到携带一种基因拷贝的分离株比例明显更高。该有限样本量的结果表明,pfmdrl基因拷贝数与pfmrpl基因突变,体外寄生虫敏感性和AS-MQ之间存在潜在的联系。治疗反应。

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