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首页> 外文期刊>Tropical Medicine and International Health: TM and IH >Molecular genotyping in a malaria treatment trial in Uganda - unexpected high rate of new infections within 2 weeks after treatment.
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Molecular genotyping in a malaria treatment trial in Uganda - unexpected high rate of new infections within 2 weeks after treatment.

机译:乌干达一项疟疾治疗试验中的分子基因分型-治疗后2周内出乎意料的高新感染率。

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Polymerase chain reaction (PCR) genotyping of malaria parasites in drug efficacy trials helps differentiate reinfections from recrudescences. A combination therapy trial of one (n = 115) or three (n = 117) days artesunate (1AS, 3AS 4 mg/kg/day) plus sulphadoxine-pyrimethamine (SP) vs. SP alone (n = 153) was conducted in Mbarara, a mesoendemic area of western Uganda. All paired recurrent Plasmodium falciparum parasitaemias on days 7, 14, 21 and 28 post-treatment were genotyped by PCR amplification and analysis of glutamate-rich protein (glurp) and merozoite surface proteins (msp) 1 and 2 genes to distinguish recrudescent from new infections. A total of 156 (1AS = 61, 3AS = 35, SP alone = 60) of 199 paired recurrent samples were successfully analysed and were resolved as 79 recrudescences (1AS = 32, 3AS = 8, SP = 39) and 77 as new infections (1AS = 29, 3AS = 27, SP = 21). The ratios of proportions of new to recrudescent infections were 0.2, 0.9, 1.4 and 1.9 on days 7, 14, 21 and 28, respectively (P < 0.001, chi(2) test for linear trend). Unexpected high new infection rates were observed early in follow-up on days 7 [5/26 (19.2%)] and 14 [24/51 (47.1%)]. These results impact significantly on resistance monitoring and point to the value of genotyping all recurrent infections in antimalarial trials.
机译:在药物功效试验中,疟原虫的聚合酶链反应(PCR)基因分型有助于区分再感染与复发。青蒿琥酯(1AS,3AS 4 mg / kg / day)加磺胺多辛-乙胺嘧啶(SP)与单独使用SP(n = 153)进行了联合治疗试验(n = 115)或3(n = 117)天。姆巴拉拉(Mbarara),乌干达西部的中流行区。治疗后第7、14、21和28天,对所有配对的恶性疟原虫副寄生虫病均进行PCR分型并分析富含谷氨酸的蛋白质(glurp)和裂殖子表面蛋白质(msp)1和2基因,以区分新发感染和复发。共成功分析了199个配对复发样本中的156个(1AS = 61,3AS = 35,SP仅= 60),并解决了79次复发(1AS = 32、3AS = 8,SP = 39)和77例再次感染(1AS = 29,3AS = 27,SP = 21)。在第7、14、21和28天,新发感染与复发感染的比例分别为0.2、0.9、1.4和1.9(P <0.001,线性趋势的chi(2)测试)。在随访的第7天[5/26(19.2%)]和第14天[24/51(47.1%)]的早期发现意外的高新感染率。这些结果显着影响耐药性监测,并指出在抗疟疾试验中对所有复发感染进行基因分型的价值。

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