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首页> 外文期刊>Molecular Biology and Evolution >From DNA to Fitness Differences: Sequences and Structures of Adaptive Variants of Colias Phosphoglucose Isomerase (PGI)
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From DNA to Fitness Differences: Sequences and Structures of Adaptive Variants of Colias Phosphoglucose Isomerase (PGI)

机译:从DNA到适应性差异:Colias磷酸葡萄糖异构酶(PGI)的适应性变体的序列和结构

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Colias eurytheme butterflies display extensive allozyme polymorphism in the enzyme phosphoglucose isomerase (PGI). Earlier studies on biochemical and fitness effects of these genotypes found evidence of strong natural selection maintaining this polymorphism in the wild. Here we analyze the molecular features of this polymorphism by sequencing multiple alleles and modeling their structures. PGI is a dimer with rotational symmetry. Each monomer provides a critical residue to the other monomer's catalytic center. Sequenced alleles differ at multiple amino acid positions, including cryptic charge-neutral variation, but most consistent differences among the electromorph alleles are at the charge-changing amino acid sites. Principal candidate sites of selection, identified by structural and functional analyses and by their variants' population frequencies, occur in interpenetrating loops across the interface between monomers, where they may alter subunit interactions and catalytic center geometry. Comparison to a second (and basal) species, Colias meadii, also polymorphic for PGI under natural selection, reveals one fixed amino acid difference between their PGIs, which is located in the interpenetrating loop and accompanies functional differences among their variants. We also study nucleotide variability among the PGI alleles, comparing these data to similar data from another glycolytic enzyme gene, glyceraldehyde-3-phosphate dehydrogenase. Despite extensive nonsynonymous and synonymous polymorphism at PGI in each species, the only base changes fixed between species are the two causing the amino acid replacement; this absence of synonymous fixation yields a significant McDonald-Kreitman test. Analyses of these data suggest historical population expansion. Positive peaks of Tajima's D statistic, representing regions of neutral “hitchhiking,” are found around the principal candidate sites of selection. This study provides novel views of molecular-structural mechanisms, and beginnings of historical evidence, for a long-persistent balanced enzyme polymorphism at PGI in these and perhaps other species.
机译:Colias eurytheme蝴蝶在磷酸葡萄糖异构酶(PGI)中显示出广泛的同工酶多态性。对这些基因型的生化和适应性效应的早期研究发现,有很强的自然选择证据可以在野外保持这种多态性。在这里,我们通过对多个等位基因测序并对它们的结构建模来分析这种多态性的分子特征。 PGI是具有旋转对称性的二聚体。每种单体向另一单体的催化中心提供关键残基。测序的等位基因在多个氨基酸位置不同,包括隐性电荷中性变化,但电态等位基因之间最一致的差异是在电荷变化的氨基酸位点。通过结构和功能分析及其变体的总体频率确定的主要候选候选位点,贯穿单体之间界面的互穿环中,它们可能会改变亚基相互作用和催化中心的几何形状。与第二种(和基础的)物种相比,Colias meadii也是自然选择下的PGI多态性,揭示了其PGI之间存在一个固定的氨基酸差异,该差异位于互穿环中,并伴随其变体之间的功能差异。我们还研究了PGI等位基因之间的核苷酸变异性,将这些数据与另一个糖酵解酶基因甘油醛-3-磷酸脱氢酶的相似数据进行了比较。尽管每个物种在PGI处都存在广泛的非同义和同义多态性,但物种之间唯一固定的碱基变化是引起氨基酸置换的两个碱基。缺少同义注视会产生重大的McDonald-Kreitman检验。这些数据的分析表明历史人口的增长。在选择的主要候选位点附近发现了田岛D统计量的正峰,代表中性的“搭便车”区域。这项研究为这些以及其他物种的PGI长期持久的平衡酶多态性提供了分子结构机制的新观点,以及历史证据的开端。

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