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首页> 外文期刊>Malaria Journal >Prevalence of the molecular marker of Plasmodium falciparum resistance to chloroquine and sulphadoxine/pyrimethamine in Benin seven years after the change of malaria treatment policy
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Prevalence of the molecular marker of Plasmodium falciparum resistance to chloroquine and sulphadoxine/pyrimethamine in Benin seven years after the change of malaria treatment policy

机译:疟疾治疗政策变化后七年七内宁七年中疟原虫对氯喹和嘧啶/吡米甲胺的分子标记

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Background In Benin, the National Malaria Control Programme (NMCP) changed the policy of malaria treatment in 2004 following increasing of failure rate of treatment with chloroquine (CQ) and sulphadoxine-pyrimethamine (SP). The objective of this study was to determinate the prevalence of Plasmodium falciparum molecular markers that are associated with resistance to CQ and SP in Benin seven years after the new policy was instituted. Methods The study was conducted in southern Benin, a region characterized by a perennial malaria transmission. Blood samples were collected in 2011 from children presenting with symptomatic and asymptomatic P. falciparum infections and living in the same area. The prevalence of critical point mutations in the genes of pfcrt (codon 76), pfmdr1 (codon 86), pfdhfr (codons, 51, 59 and 108) and pfdhps (codons 437, 540) was examined in parasite isolates by mutation-specific restriction enzyme digestion of nested PCR products. Results A high prevalence of parasites carrying point mutations in all studied targets was found: T76: 93.9% [89.8; 96.7], I51: 96.2% [92.7; 98.4], R59: 93, 9% [89.7; 96.7], N108: 97.6% [94.6; 99.2] and G437: 71.4% [64.8; 77.4]. No mutation was found at codon 540 of the pfdhps gene. The proportion of parasite isolates carrying triple mutation in the pfdhfr gene IRN (I51, R59 andN108) and quadruple mutation on the combination of pfdhfr/pfdhps IRNG (I51, R59, N108 and G437) was 91.5% [86.9; 94.9] and 65.7% [58.9; 72.1], respectively. Analysis of mutation in relation to the clinical status (symptomatic or asymptomatic) and according to age (younger or older than 10 years) showed similar very high frequencies in each category without significant difference between two groups. Conclusions These results suggest a persistence level of resistance of P. falciparum to CQ and SP, seven years after the recommendation of the change of malaria treatment policy in Benin. The distribution of mutations studied was neither related to age nor to clinical status.
机译:背景技术在贝宁,国家疟疾控制计划(NMCP)在增加氯喹(CQ)和磺基胺 - 吡米甲胺(SP)的含量后,2004年改变了2004年疟疾治疗的政策。本研究的目的是确定新政策在制定新政策后七年后与CQ和SP有关的疟原虫分子标记的患病率。方法在南贝宁进行该研究,该区域是一种特征的区域,其特征在一起,其特征在于常年疟疾传播。从患有症状和无症状P. falciparum感染并生活在同一地区的儿童,从2011年收集血样。通过突变特异性限制在寄生虫分离物中检查PFCRT(密码子76),PFMDR1(密码子86),PFDHFR(密码子,51,59和108)和PFDHPS(密码子437,540)中的临界点突变的临界率嵌套PCR产品的酶消化。结果发现,寄生虫患者患有点突变的高普遍性是:T76:93.9%[89.8; 96.7],I51:96.2%[92.7; 98.4],R59:93,9%[89.7; 96.7],N108:97.6%[94.6; 99.2]和G437:71.4%[64.8; 77.4]。在PFDHPS基因的密码子540中发现不突变。在PFDHFR基因IRN(I51,R59和N108)中携带三重突变的寄生虫分离物的比例在PFDHFR / PFDHPS IRNG(I51,R59,N108和G437)的组合上为91.5%[86.9; 94.9]和65.7%[58.9; 72.1]分别。与临床状况(症状或无症状)相关的突变分析,根据年龄(年轻或超过10年)在每类中显示出类似的非常高的频率,而两组之间的显着差异。结论这些结果表明,在贝宁疟疾治疗政策的改变后七年,七年来持续持续抗性的抗性。研究的突变分布既不与年龄有关,也不是临床地位。

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