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Genetic mapping of fitness determinants across the malaria parasite?Plasmodium falciparum life cycle

机译:疟疾疟原虫生命周期中健康决定因素的遗传图谱

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Determining the genetic basis of fitness is central to understanding evolution and transmission of microbial pathogens. In human malaria parasites ( Plasmodium falciparum ), most experimental work on fitness has focused on asexual blood stage parasites, because this stage can be easily cultured, although the transmission of malaria requires both female Anopheles mosquitoes and vertebrate hosts. We explore a powerful approach to identify the genetic determinants of parasite fitness across both invertebrate and vertebrate life-cycle stages of P . falciparum . This combines experimental genetic crosses using humanized mice, with selective whole genome amplification and pooled sequencing to determine genome-wide allele frequencies and identify genomic regions under selection across multiple lifecycle stages. We applied this approach to genetic crosses between artemisinin resistant (ART-R, kelch13 -C580Y) and ART-sensitive (ART-S, kelch13 -WT) parasites, recently isolated from Southeast Asian patients. Two striking results emerge: we observed (i) a strong genome-wide skew (>80%) towards alleles from the ART-R parent in the mosquito stage, that dropped to ~50% in the blood stage as selfed ART-R parasites were selected against; and (ii) repeatable allele specific skews in blood stage parasites with particularly strong selection (selection coefficient (s) ≤ 0.18/asexual cycle) against alleles from the ART-R parent at loci on chromosome 12 containing MRP2 and chromosome 14 containing ARPS10 . This approach robustly identifies selected loci and has strong potential for identifying parasite genes that interact with the mosquito vector or compensatory loci involved in drug resistance.
机译:确定适应性的遗传基础对于了解微生物病原体的进化和传播至关重要。在人类疟疾寄生虫(恶性疟原虫)中,关于适应性的大多数实验工作都集中在无性血液阶段的寄生虫上,因为可以轻松地培养该阶段的寄生虫,尽管疟疾的传播既需要雌性按蚊也可以传播脊椎动物。我们探索了一种强大的方法来确定P的无脊椎动物和脊椎动物生命周期阶段寄生虫适应性的遗传决定因素。恶性肿瘤。这结合了使用人源化小鼠进行的实验性遗传杂交,选择性全基因组扩增和合并测序,以确定全基因组等位基因频率,并确定了跨多个生命周期阶段选择的基因组区域。我们将这种方法应用于最近从东南亚患者中分离出的青蒿素耐药性(ART-R,kelch13 -C580Y)和ART敏感性(ART-S,kelch13 -WT)寄生虫之间的遗传杂交。出现两个惊人的结果:我们观察到(i)在蚊子阶段,来自ART-R亲本的等位基因对全基因组的偏向性强(> 80%),在血液阶段由于自体ART-R寄生虫下降至〜50%被选为反对(ii)在血液阶段寄生虫中可重复的等位基因特异性偏斜,对来自MART2染色体的12号染色体和包含ARPS10的14号染色体上来自ART-R亲本的等位基因具有特别强的选择(选择系数≤0.18 /无性循环)。该方法可强有力地鉴定选定的基因座,并且具有鉴定与蚊子载体或与药物抗性有关的补偿基因座相互作用的寄生虫基因的强大潜力。

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