中非、西非和东非重症疟疾儿童抗疟药物耐药性的分子标志物

Molecular markers of anti-malarial drug resistance in Central, West and East African children with severe malaria.

作者信息

Nguetse Christian N, Adegnika Ayola Akim, Agbenyega Tsiri, Ogutu Bernhards R, Krishna Sanjeev, Kremsner Peter G, Velavan Thirumalaisamy P

机构信息

Institute of Tropical Medicine, University Tübingen, Wilhelmstrasse 27, 72074, Tübingen, Germany.

Centre de Recherches Médicales de Lambaréné, Lambaréné, Gabon.

出版信息

Malar J. 2017 May 23;16(1):217. doi: 10.1186/s12936-017-1868-y.

DOI:10.1186/s12936-017-1868-y

PMID:28535801

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5442681/

Abstract

BACKGROUND

The Plasmodium falciparum multidrug resistance 1 (PfMDR1), P. falciparum Ca-ATPase (PfATP6) and Kelch-13 propeller domain (PfK13) loci are molecular markers of parasite susceptibility to anti-malarial drugs. Their frequency distributions were determined in the isolates collected from children with severe malaria originating from three African countries.

METHODS

Samples from 287 children with severe malaria [(Gabon: n = 114); (Ghana: n = 89); (Kenya: n = 84)] were genotyped for pfmdr1, pfatp6 and pfk13 loci by DNA sequencing and assessing pfmdr1 copy number variation (CNV) by real-time PCR.

RESULTS

Pfmdr1-N86Y mutation was detected in 48, 10 and 10% in Lambaréné, Kumasi and Kisumu, respectively. At codon 184, the prevalence of the mutation was 73% in Lambaréné, 63% in Kumasi and 49% Kisumu. The S1034C and N1042D variants were absent at all three sites, while the frequency of the D1246Y mutation was 1, 3 and 13% in Lambaréné, Kumasi and Kisumu, respectively. Isolates with two pfmdr1 gene copy number predominantly harboured the N86Y wild-type allele and were mostly found in Kumasi (10%) (P < 0.0001). Among the main pfmdr1 haplotypes (NFD, NYD and YFD), NYD was associated with highest parasitaemia (P = 0.04). At the pfatp6 locus, H243Y and A623E mutations were observed at very low frequency at all three sites. The prevalence of the pfatp6 E431K variant was 6, 18 and 17% in Lambaréné, Kumasi and Kisumu, respectively. The L263E and S769N mutations were absent in all isolates. The pfk13 variants associated with artemisinin resistance in Southeast Asia were not observed. Eleven novel substitutions in the pfk13 locus occurring at low frequency were observed.

CONCLUSIONS

Artemisinins are still highly efficacious in large malaria-endemic regions though declining efficacy has occurred in Southeast Asia. The return of chloroquine-sensitive strains following the removal of drug pressure is observed. However, selection of wild-type alleles in the multidrug-resistance gene and the increased gene copy number is associated with reduced lumefantrine sensitivity. This study indicates a need to constantly monitor drug resistance to artemisinin in field isolates from malaria-endemic countries.

摘要

背景

恶性疟原虫多药耐药 1 基因（PfMDR1）、恶性疟原虫钙 - ATP 酶（PfATP6）和 Kelch - 13 螺旋桨结构域（PfK13）位点是寄生虫对抗疟药物敏感性的分子标志物。在从三个非洲国家患有严重疟疾的儿童中收集的分离株中确定了它们的频率分布。

方法

对来自 287 名患有严重疟疾的儿童的样本（[加蓬：n = 114]；[加纳：n = 89]；[肯尼亚：n = 84]）进行 pfmdr1、pfatp6 和 pfk13 位点的基因分型，采用 DNA 测序法，并通过实时 PCR 评估 pfmdr1 拷贝数变异（CNV）。

结果

在兰巴雷内、库马西和基苏木分别检测到 Pfmdr1 - N86Y 突变的比例为 48%、10%和 10%。在第 184 密码子处，该突变的流行率在兰巴雷内为 73%，在库马西为 63%，在基苏木为 49%。在所有三个地点均未检测到 S1034C 和 N1042D 变体，而 D1246Y 突变的频率在兰巴雷内、库马西和基苏木分别为 1%、3%和 13%。具有两个 pfmdr1 基因拷贝数的分离株主要携带 N86Y 野生型等位基因，且大多在库马西被发现（10%）（P < 0.0001）。在主要的 pfmdr1 单倍型（NFD、NYD 和 YFD）中，NYD 与最高的寄生虫血症相关（P = 0.04）。在 pfatp6 位点，在所有三个地点均以极低频率观察到 H243Y 和 A623E 突变。pfatp6 E431K 变体的流行率在兰巴雷内、库马西和基苏木分别为 6%、18%和 17%。在所有分离株中均未发现 L263E 和 S769N 突变。未观察到与东南亚青蒿素耐药相关的 pfk13 变体。在 pfk13 位点观察到 11 个低频出现的新替换。

结论

在疟疾流行的广大地区，青蒿素仍然高度有效，尽管在东南亚其疗效有所下降。观察到在去除药物压力后氯喹敏感菌株的出现。然而，多药耐药基因中野生型等位基因的选择以及基因拷贝数的增加与卤泛群敏感性降低有关。本研究表明需要持续监测疟疾流行国家野外分离株对青蒿素的耐药性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6ae2/5442681/45ed544f9f86/12936_2017_1868_Fig1_HTML.jpg

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中非、西非和东非重症疟疾儿童抗疟药物耐药性的分子标志物

Molecular markers of anti-malarial drug resistance in Central, West and East African children with severe malaria.

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