Mapping drug resistance genes in Plasmodium falciparum by genome-wide association.

Tim J C Anderson
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引用次数: 64

Abstract

When alleles conferring drug resistance spread through a population of malaria parasites, they leave characteristic "scars" in the parasite genome. Flanking neutral polymorphisms "hitchhike" to high frequency with the resistance mutation, generating deep valleys of reduced variation and broad swathes of elevated linkage disequilibrium around the resistance locus. We can systematically search the genome for these scars by genotyping polymorphic marker loci at intervals throughout the genome of P. falciparum, and use them as signposts for locating drug resistance genes. In this review I outline the rational behind this approach to genetic mapping. I describe key features of P. falciparum population biology, such as recombination rate, inbreeding, and selection intensity that influence the size of genomic regions affected by selection and the choice of study population. I discuss suitable genetic markers, study designs, and statistical approaches to data analysis. Finally, to demonstrate the utility of the approach I describe two proof-of-principle studies documenting patterns of genetic variability around known drug resistance genes.

恶性疟原虫耐药基因全基因组关联图谱研究。
当赋予耐药性的等位基因在疟原虫种群中传播时,它们会在疟原虫基因组中留下特有的“伤疤”。侧翼中性多态性与抗性突变“搭便车”到高频率,在抗性位点周围产生减少变异的深谷和广泛的连锁不平衡升高。我们可以通过在整个恶性疟原虫基因组中每隔一段时间对多态性标记位点进行基因分型,系统地搜索这些疤痕,并将其作为定位耐药基因的路标。在这篇综述中,我概述了这种遗传作图方法背后的原因。我描述了恶性疟原虫种群生物学的关键特征,如重组率、近亲繁殖和选择强度,这些特征会影响受选择和研究种群选择影响的基因组区域的大小。我讨论了合适的遗传标记、研究设计和数据分析的统计方法。最后,为了证明该方法的实用性,我描述了两个原理证明研究,记录了已知耐药基因周围的遗传变异模式。
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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