Plasmodium ovale spp dhfr mutations associated with reduced susceptibility to pyrimethamine in sub-Saharan Africa: a retrospective genetic epidemiology and functional study

IF 20.9 1区 生物学 Q1 INFECTIOUS DISEASES
Valentin Joste PharmD , Romain Coppée PhD , Justine Bailly MSc , Yann Rakotoarivony BSc , Francine Ghislaine Toko Tchokoteu BSc , Shany Achache BSc , Bruno Pradines PhD , Gilles Cottrell PhD , Prof Frédéric Ariey PhD , Nimol Khim PhD , Jean Popovici PhD , Prof Toshihiro Mita PhD , Mirjam Groger PhD , Prof Michael Ramharter MD , Timothy Egbo PhD , Dennis W Juma MSc , Hoseah Akala PhD , Prof Sandrine Houzé PhD , Jérôme Clain PhD , Rella Zoleko-Manego
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引用次数: 0

Abstract

Background

Mutations in the Plasmodium falciparum dhfr gene confer resistance to pyrimethamine, which is widely used for malaria chemoprevention in Africa. We aimed to evaluate the frequency and evolution of dhfr mutations in Plasmodium ovale spp in Africa and their functional consequences, which are incompletely characterised.

Methods

We analysed dhfr mutations and their frequencies in P ovale spp isolates collected between Feb 1, 2004, and Aug 31, 2023, from the French National Malaria Reference Centre collection and from field studies in Benin, Gabon, and Kenya. Genetic patterns of positive selection were investigated. Full-length recombinant wild-type and mutant DHFR enzymes from both P ovale curtisi and P ovale wallikeri were expressed in bacteria to test whether the most common mutations reduced pyrimethamine susceptibility.

Findings

We included 518 P ovale spp samples (314 P ovale curtisi and 204 P ovale wallikeri). In P ovale curtisi, Ala15Ser-Ser58Arg was the most common dhfr mutation (39%; 124 of 314 samples). In P ovale wallikeri, dhfr mutations were less frequent, with Phe57Leu-Ser58Arg reaching 17% (34 of 204 samples). These two mutants were the most prevalent in central and east Africa and were fixed in Kenyan isolates. We detected six and four other non-synonymous mutations, representing 8% (24 isolates) and 2% (five isolates) of the P ovale curtisi and P ovale wallikeri isolates, respectively. Whole-genome sequencing and microsatellite analyses revealed reduced genetic diversity around the mutant pocdhfr and powdhfr genes. The mutant DHFR proteins showed structural changes at the pyrimethamine binding site in-silico, confirmed by a 4-times increase in pyrimethamine half-maximal inhibitory concentration in an Escherichia coli growth assay for the Phe57Leu-Ser58Arg mutant and 50-times increase for the Ala15Ser-Ser58Arg mutant, compared with the wild-type counterparts.

Interpretation

The widespread use of sulfadoxine–pyrimethamine for malaria chemoprevention might have exerted fortuitous selection pressure for dhfr mutations in P ovale spp. This calls for closer monitoring of dhfr and dhps mutations in P ovale spp.

Funding

French Ministry of Health, Agence Nationale de la Recherche, and Global Emerging Infections Surveillance branch of the Armed Forces Health Surveillance Division.

撒哈拉以南非洲卵形疟原虫 dhfr 突变与嘧啶敏感性降低有关:一项回顾性遗传流行病学和功能研究。
背景:恶性疟原虫 dhfr 基因突变会产生对嘧啶的抗药性,嘧啶在非洲被广泛用于疟疾化学预防。我们的目的是评估非洲卵形疟原虫中 dhfr 基因突变的频率和进化情况,以及它们的功能性后果:我们分析了 2004 年 2 月 1 日至 2023 年 8 月 31 日期间从法国国家疟疾参考资料中心以及贝宁、加蓬和肯尼亚的实地研究中收集的卵形疟原虫分离株中的 dhfr 突变及其频率。对正向选择的遗传模式进行了研究。在细菌中表达了来自卵形库蒂西疟原虫和卵形瓦利克氏疟原虫的全长重组野生型和突变型DHFR酶,以检测最常见的突变是否会降低嘧啶敏感性:我们纳入了 518 个卵形目动物样本(314 个 P ovale curtisi 和 204 个 P ovale wallikeri)。在柯蒂斯卵形虫中,Ala15Ser-Ser58Arg是最常见的dhfr突变(39%;314个样本中有124个)。在 P ovale wallikeri 中,dhfr 突变较少,Phe57Leu-Ser58Arg 突变占 17%(204 个样本中的 34 个)。这两种突变在非洲中部和东部最为普遍,在肯尼亚的分离物中也固定存在。我们还检测到 6 个和 4 个其他非同义突变,分别占 P ovale curtisi 和 P ovale wallikeri 分离物的 8%(24 个分离物)和 2%(5 个分离物)。全基因组测序和微卫星分析表明,突变的 pocdhfr 和 powdhfr 基因周围的遗传多样性减少。在大肠杆菌生长试验中,与野生型相比,Phe57Leu-Ser58Arg 突变体的嘧霉胺半最大抑制浓度增加了 4 倍,Ala15Ser-Ser58Arg 突变体的嘧霉胺半最大抑制浓度增加了 50 倍:解释:广泛使用磺胺乙胺嘧啶进行疟疾化学预防可能对卵球菌中的dhfr突变产生了偶然的选择压力,因此需要更密切地监测卵球菌中的dhfr和dhps突变:经费来源:法国卫生部、国家研究署和武装部队健康监测处全球新发感染监测分部。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Lancet Microbe
Lancet Microbe Multiple-
CiteScore
27.20
自引率
0.80%
发文量
278
审稿时长
6 weeks
期刊介绍: The Lancet Microbe is a gold open access journal committed to publishing content relevant to clinical microbiologists worldwide, with a focus on studies that advance clinical understanding, challenge the status quo, and advocate change in health policy.
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