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首页> 外文期刊>Acta tropica: Journal of Biomedical Sciences >Rapid increase in resistance of Plasmodium falciparum to chloroquine-Fansidar in Uganda and the potential of amodiaquine-Fansidar as a better alternative.
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Rapid increase in resistance of Plasmodium falciparum to chloroquine-Fansidar in Uganda and the potential of amodiaquine-Fansidar as a better alternative.

机译:在乌干达,恶性疟原虫对氯喹-范西达的耐药性迅速增加,而氨二喹-范西达有可能成为更好的替代品。

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摘要

Combinations of chloroquine (CQ) and sulfadoxine-pyrimethamine (SP) [CQSP] as the first line agents in Uganda have replaced CQ monotherapy. The idea of the combination is to delay the development of malaria resistance to either drug when used alone. We compared the clinical, parasitological and molecular findings of two studies with treatment arms of CQSP, amodiaquine (AQ) plus SP (AQSP) both done in 2003 with a study done 1 year earlier (2002) using SP alone. There was a notable decrease in adequate clinical response (ACR) by day 14 from 92.7% with SP to 80% with the combination CQSP, a year later. AQSP combination was found to have the best effect (94.3% ACR). There were no early treatment failures in the AQSP group. However, treatment failures were recorded at 20% on day 14 and 43% on day 28 for CQSP treatment and 5.7% by day 14 and 28.8% by day 28 in the AQSP group. The number of mutations that are associated with SP resistance increased from 2002 to 2003 at all loci monitored, from 83.8 to 100% atcodon 108, 58.7 to 76% at codon 59 in the DHFR gene, and from 58.8 to 86% at codon 437 and 33 to 43% at codon 540 in the DHPS gene. We conclude that there has been a rapid development of resistance since the introduction of the new policy guidelines. AQSP was found to be a superior drug combination compared to CQSP and could be used as a low cost alternative at the moment.
机译:作为乌干达的第一线药物,氯喹(CQ)和磺胺多辛-乙胺嘧啶(SP)[CQSP]的组合已取代了CQ单药治疗。组合使用的想法是延迟单独使用时对两种药物的疟疾抵抗力的发展。我们比较了使用CQSP治疗组的两项研究的临床,寄生虫学和分子生物学发现:阿莫地喹(AQ)加SP(AQSP),两者均于2003年完成,而一年前(2002年)仅使用SP进行了研究。到第14天,适当的临床反应(ACR)从SP的92.7%显着降低到一年后的CQSP组合的80%。发现AQSP组合具有最佳效果(94.3%ACR)。 AQSP组没有早期治疗失败。但是,对于AQSP组,CQSP治疗的治疗失败记录为第14天的20%和第28天的43%,第14天的5.7%和第28天的28.8%。在2002年至2003年期间,在所有受监测的基因座上,与SP抗性相关的突变数量均增加了,从DHFR基因的第98位密码子从83.8%增加到100%,在第59位密码子从58.7%提高到76%,在第437位密码子从58.8%增加到86% DHPS基因中第540位密码子占33%至43%。我们得出的结论是,自从引入新的政策准则以来,抵抗运动迅速发展。与CQSP相比,发现AQSP是一种更好的药物组合,目前可以用作低成本的替代品。

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