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首页> 外文期刊>The Royal Society Proceedings B: Biological Sciences >Selection strength and hitchhiking around two anti-malarial resistance genes.
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Selection strength and hitchhiking around two anti-malarial resistance genes.

机译:选择强度和搭便车周围的两个抗疟疾抗性基因。

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摘要

Neutral mutations may hitchhike to high frequency when they are situated close to sites under positive selection, generating local reductions in genetic diversity. This process is thought to be an important determinant of levels of genomic variation in natural populations. The size of genome regions affected by genetic hitchhiking is expected to be dependent on the strength of selection, but there is little empirical data supporting this prediction. Here, we compare microsatellite variation around two drug resistance genes (chloroquine resistance transporter (pfcrt), chromosome 7, and dihydrofolate reductase (dhfr), chromosome 4) in malaria parasite populations exposed to strong (Thailand) or weak selection (Laos) by anti-malarial drugs. In each population, we examined the point mutations underlying resistance and length variation at 22 (chromosome 4) or 25 (chromosome 7) microsatellite markers across these chromosomes. All parasites from Thailand carried the K76T mutation in pfcrt conferring resistance to chloroquine (CQ) and 2-4 mutations in dhfr conferring resistance to pyrimethamine. By contrast, we found both wild-type and resistant alleles at both genes in Laos. There were dramatic differences in the extent of hitchhiking in the two countries. The size of genome regions affected was smaller in Laos than in Thailand. We observed significant reduction in variation relative to sensitive parasites for 34-64kb (2-4cM) in Laos on chromosome 4, compared with 98-137kb (6-8cM) in Thailand. Similarly, on chromosome 7, we observed reduced variation for 34-69kb (2-4cM) around pfcrt in Laos, but for 195-268kb (11-16cM) in Thailand. Reduction in genetic variation was also less extreme in Laos than in Thailand. Most loci were monomorphic in a 12kb region surrounding both genes on resistant chromosomes from Thailand, whereas in Laos, even loci immediately proximal to selective sites showed some variation on resistant chromosomes. Finally, linkage disequilibrium (LD) decayed more rapidly around resistant pfcrt and dhfr alleles from Laos than from Thailand. These results demonstrate that different realizations of the same selective sweeps may vary considerably in size and shape, in a manner broadly consistent with selection history. From a practical perspective, genomic regions containing resistance genes may be most effectively located by genome-wide association in populations exposed to strong drug selection. However, the lower levels of LD surrounding resistance alleles in populations under weak selection may simplify identification of functional mutations.
机译:当中性突变位于正选择位点附近时,中性突变可能会突然发作,从而导致遗传多样性的局部降低。人们认为这一过程是自然种群中基因组变异水平的重要决定因素。受基因搭便车影响的基因组区域的大小预计将取决于选择的强度,但几乎没有经验数据支持这一预测。在这里,我们比较了通过抗药性暴露于强(泰国)或弱选择(老挝)的疟原虫种群中两个耐药基因(氯喹耐药转运蛋白(pfcrt),7号染色体和二氢叶酸还原酶(dhfr),4号染色体)周围的微卫星变异。 -疟疾药物。在每个种群中,我们检查了这些染色体上22个(染色体4)或25(染色体7)微卫星标记的抗性和长度变异的基础点突变。来自泰国的所有寄生虫均在pfcrt中带有K76T突变,赋予了对氯喹(CQ)的抗性,而dhfr的2-4个突变则赋予了对乙胺嘧啶的抗性。相比之下,我们在老挝的两个基因上都发现了野生型和抗性等位基因。两国搭便车的程度存在巨大差异。老挝受影响的基因组区域的规模小于泰国。我们观察到老挝第4号染色体上34-64kb(2-4cM)的敏感寄生虫变异相对于泰国显着降低,而泰国为98-137kb(6-8cM)。同样,在第7号染色体上,我们观察到老挝pfcrt附近34-69kb(2-4cM)的变异减少,而泰国则为195-268kb(11-16cM)。老挝的遗传变异减少也没有泰国那么极端。大多数位点在来自泰国的抗性染色体上的两个基因周围的12kb区域内是单态的,而在老挝,即使紧邻选择位点的位点也显示出抗性染色体上的一些变异。最后,老挝的抗性pfcrt和dhfr等位基因周围的连锁不平衡(LD)的衰减比泰国更快。这些结果表明,相同选择扫描的不同实现方式在大小和形状上可能会以与选择历史大致一致的方式发生很大变化。从实践的角度来看,在暴露于强烈药物选择的人群中,通过全基因组关联可以最有效地定位包含抗性基因的基因组区域。但是,在弱选择下的群体中较低水平的LD周围抗性等位基因可以简化功能突变的鉴定。

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