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首页> 外文期刊>Malaria Journal >Genetic mutations in Plasmodium falciparum and Plasmodium vivax dihydrofolate reductase (DHFR) and dihydropteroate synthase (DHPS) in Vanuatu and Solomon Islands prior to the introduction of artemisinin combination therapy
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Genetic mutations in Plasmodium falciparum and Plasmodium vivax dihydrofolate reductase (DHFR) and dihydropteroate synthase (DHPS) in Vanuatu and Solomon Islands prior to the introduction of artemisinin combination therapy

机译:在引入青蒿素联合疗法之前,瓦努阿图和所罗门群岛的恶性疟原虫和间日疟原虫二氢叶酸还原酶(DHFR)和二氢蝶呤合酶(DHPS)发生了基因突变。

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Background Plasmodium falciparum and Plasmodium vivax are endemic in Vanuatu and the Solomon Islands. While both countries have introduced artemether-lumefantrine (AL) as first-line therapy for both P. falciparum and P. vivax since 2008, chloroquine and sulphadoxine-pyrimethamine (SP) were used as first-line therapy for many years prior to the introduction of AL. Limited data are available on the extent of SP resistance at the time of policy change. Methods Blood spots were obtained from epidemiological surveys conducted on Tanna Island, Tafea Province, Vanuatu and Temotu Province, Solomon Islands in 2008. Additional samples from Malaita Province, Solomon Islands were collected as part of an AL therapeutic efficacy study conducted in 2008. Plasmodium vivax and P. falciparum dhfr and dhps genes were sequenced to detect nucleotide polymorphisms. Results All P. falciparum samples analysed (n =114) possessed a double mutant pfdhfr allele (C59R/S108N). Additionally, mutation A437G in pfhdps was detected in a small number of samples 2/13, 1/17 and 3/26 from Tanna Island, Vanuatu and Temotu and Malaita Provinces Solomon Islands respectively. Mutations were also common in pvdhfr from Tanna Island, Vanuatu, where 33/51 parasites carried the double amino acid substitution S58R/S117N, while in Temotu and Malaita Provinces, Solomon Islands 32/40 and 39/46 isolates carried the quadruple amino acid substitution F57L/S58R/T61M/S117T in DHFR respectively. No mutations in pvdhps (n =108) were detected in these three island groups. Conclusion Prior to the introduction of AL, there was a moderate level of SP resistance in the P. falciparum population that may cause SP treatment failure in young children. Of the P. vivax isolates, a majority of Solomon Islands isolates carried quadruple mutant pvdhfr alleles while a majority of Vanuatu isolates carried double mutant pvdhfr alleles. This suggests a higher level of SP resistance in the P. vivax population in Solomon Islands compared to the sympatric P. falciparum population and there is a higher level of SP resistance in P. vivax parasites from Solomon Islands than Vanuatu. This study demonstrates that the change of treatment policy in these countries from SP to ACT was timely. The information also provides a baseline for future monitoring.
机译:背景恶性疟原虫和间日疟原虫在瓦努阿图和所罗门群岛流行。自2008年以来,两国都已将蒿甲醚-氟美特林(AL)用作恶性疟原虫和间日疟原虫的一线治疗药物,但在引入之前,氯喹和磺胺多辛-乙胺嘧啶(SP)一直被用作一线治疗药物的AL。有关政策更改时SP抵抗程度的有限数据。方法从2008年在所罗门群岛的塔菲亚省,塔菲亚省,瓦努阿图和特默图省进行的流行病学调查中获得血斑。作为2008年进行的AL治疗功效研究的一部分,从所罗门群岛的马莱塔省收集了其他标本。对恶性疟原虫dhfr和dhps基因进行测序,以检测核苷酸多态性。结果分析的所有恶性疟原虫样品(n = 114)均具有双突变pfdhfr等位基因(C59R / S108N)。此外,分别从塔纳岛,瓦努阿图和特莫图和马拉塔伊省所罗门群岛的少量样品2 / 13、1 / 17和3/26中检测到pfhdps中的A437G突变。在瓦努阿图塔纳岛的pvdhfr中,突变也很常见,那里的33/51寄生虫带有双氨基酸取代S58R / S117N,而在特默图和马拉塔伊省,所罗门群岛的32/40和39/46分离株进行了四倍氨基酸取代。 DHFR中的F57L / S58R / T61M / S117T。在这三个岛群中未检测到pvdhps突变(n = 108)。结论在引入AL之前,恶性疟原虫人群中SP抵抗力处于中等水平,可能导致幼儿SP治疗失败。在间日疟原虫分离株中,大多数所罗门群岛分离株带有四个突变体pvdhfr等位基因,而大多数瓦努阿图分离株带有双重突变体pvdhfr等位基因。这表明与同胞恶性疟原虫相比,所罗门群岛间日疟原虫种群对SP的抵抗力更高,所罗门群岛的间日疟原虫寄生虫对SP的抵抗力高于瓦努阿图。这项研究表明,这些国家从SP到ACT的治疗政策改变是及时的。该信息还为将来的监视提供了基准。

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