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在加纳北部进行四年室内滞留喷洒后,对无症状恶性疟原虫感染中抗疟药物耐药标志物的评估。

Assessment of antimalarial drug resistant markers in asymptomatic Plasmodium falciparum infections after 4 years of indoor residual spraying in Northern Ghana.

作者信息

Myers-Hansen James L, Abuaku Benjamin, Oyebola Muyiwa K, Mensah Benedicta A, Ahorlu Collins, Wilson Michael D, Awandare Gordon, Koram Kwadwo A, Ngwa Alfred Amambua, Ghansah Anita

机构信息

Noguchi Memorial Institute for Medical Research, University of Ghana, Legon, Ghana.

West African Center for Cell Biology of Infectious Pathogens, University of Ghana, Legon, Ghana.

出版信息

PLoS One. 2020 Dec 7;15(12):e0233478. doi: 10.1371/journal.pone.0233478. eCollection 2020.

Abstract

BACKGROUND

Drug resistance remains a concern for malaria control and elimination. The effect of interventions on its prevalence needs to be monitored to pre-empt further selection. We assessed the prevalence of Plasmodium falciparum gene mutations associated with resistance to the antimalarial drugs: sulfadoxine-pyrimethamine (SP), chloroquine (CQ) and artemisinin combination therapy (ACTs) after the scale-up of a vector control activity that reduced transmission.

METHODS

A total of 400 P. falciparum isolates from children under five years were genotyped for seventeen single nucleotide polymorphisms (SNPs) in pfcrt, pfmdr1, pfdhfr, pfdhps and pfk13 genes using polymerase chain reaction (PCR) and high resolution melting (HRM) analysis. These included 80 isolates, each randomly selected from cross-sectional surveys of asymptomatic infections across 2010 (baseline), 2011, 2012, 2013 (midline: post-IRS) and 2014 (endline: post-IRS) during the peak transmission season, when IRS intervention was rolled out in Bunkpurugu Yunyoo (BY) District, Ghana. The proportions of isolates with drug resistant alleles were assessed over this period.

RESULTS

There were significant decreases in the prevalence of pfdhfr- I51R59N108 haplotype from 2010 to 2014, while the decline in pfdhfr/pfdhps- I51R59N108G437 during the same period was not significant. The prevalence of lumefantrine (LM), mefloquine (MQ) and amodiaquine (AQ) resistance-associated haplotypes pfmdr1-N86F184D1246 and pfmdr1-Y86Y184Y1246 showed decreasing trends (z = -2.86, P = 0.004 and z = -2.71, P = 0.007, respectively). Each of pfcrt-T76 and pfmdr1-Y86 mutant alleles also showed a declining trend in the asymptomatic reservoir, after the IRS rollout in 2014 (z = -2.87, P = 0.004 and z = -2.65, P = 0.008, respectively). Similarly, Pyrimethamine resistance mediating polymorphisms pfdhfr-N108, pfdhfr-I51 and pfdhfr-R59 also declined (z = -2.03, P = 0.042, z = -3.54, P<0.001 and z = -4.63, P<0.001, respectively), but not the sulphadoxine resistance mediating pfdhps-G437 and pfdhps-F436 (z = -0.36, P = 0.715 and z = 0.41, P = 0.684, respectively). No mutant pfk13-Y580 were detected during the study period.

CONCLUSION

The study demonstrated declining trends in the prevalence of drug resistant mutations in asymptomatic P. falciparum infections following transmission reduction after an enhanced IRS intervention in Northern Ghana.

摘要

背景

耐药性仍然是疟疾控制和消除工作中的一个问题。需要监测干预措施对其流行率的影响,以防止进一步的选择。在扩大了一项降低传播的病媒控制活动后,我们评估了与抗疟药物耐药性相关的恶性疟原虫基因突变的流行情况,这些抗疟药物包括:磺胺多辛-乙胺嘧啶(SP)、氯喹(CQ)和青蒿素联合疗法(ACTs)。

方法

使用聚合酶链反应(PCR)和高分辨率熔解(HRM)分析,对400份来自5岁以下儿童的恶性疟原虫分离株进行基因分型,检测pfcrt、pfmdr1、pfdhfr、pfdhps和pfk13基因中的17个单核苷酸多态性(SNP)。其中包括80份分离株,分别从2010年(基线)、2011年、2012年、2013年(中线:室内滞留喷洒后)和2014年(终点线:室内滞留喷洒后)的无症状感染横断面调查中随机选取,这些调查是在加纳邦库普鲁古-尤尼奥(BY)区开展室内滞留喷洒干预措施期间的传播高峰期进行的。在此期间评估了携带耐药等位基因的分离株比例。

结果

2010年至2014年期间,pfdhfr-I51R59N108单倍型的流行率显著下降,而同期pfdhfr/pfdhps-I51R59N108G437的下降不显著。与氯菊酯(LM)、甲氟喹(MQ)和阿莫地喹(AQ)耐药相关的单倍型pfmdr1-N86F184D1246和pfmdr1-Y86Y184Y1246的流行率呈下降趋势(z=-2.86,P=0.004;z=-2.71,P=0.007)。在2014年室内滞留喷洒实施后,无症状感染库中pfcrt-T76和pfmdr1-Y86突变等位基因的流行率也呈下降趋势(z=-2.87,P=0.004;z=-2.65,P=0.008)。同样,介导乙胺嘧啶耐药性的多态性pfdhfr-N108、pfdhfr-I51和pfdhfr-R59也有所下降(z=-2.03,P=0.042;z=-3.54,P<0.001;z=-4.63,P<0.001),但介导磺胺多辛耐药性的pfdhps-G437和pfdhps-F436没有下降(z=-0.36,P=0.715;z=0.41,P=0.684)。在研究期间未检测到pfk13-Y580突变。

结论

该研究表明,在加纳北部加强室内滞留喷洒干预措施降低传播后,无症状恶性疟原虫感染中耐药突变的流行率呈下降趋势。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/40f5/7721464/ce5d2f469c96/pone.0233478.g001.jpg

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