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Distribution of nonrandom associations between pairs of protein loci along the third chromosome of Drosophila melanogaster.

机译:沿果蝇第三条染色体的蛋白质基因对对之间的非随机关联分布。

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摘要

The within-chromosome distribution of gametic disequilibrium (GD) between protein loci, and the underlying evolutionary factors of this distribution, are still largely unknown. Here, we report a detailed study of GD between a large number of protein loci (15) spanning 87% of the total length of the third chromosome of Drosophila melanogaster in a large sample of haplotypes (600) drawn from a single natural population. We used a sign-based GD estimation method recently developed for multiallelic systems, which considerably increases both the statistical power and the accuracy of estimation of the intensity of GD. We found that strong GD between pairs of protein loci was widespread throughout the chromosome. In total, 22% of both the pairs of alleles and pairs of loci were in significant GD, with mean intensities (as measured by D' coefficients) of 0.43 and 0.31, respectively. In addition, strong GD often occurs between loci that are far apart. By way of illustration, 32% of the allele pairs in significant GD occurred within pairs of loci separated by effective frequencies of recombination (EFRs) of 15-20 cM, the mean D' value being 0.49. These observations are in sharp contrast with previous studies showing that GD between protein loci is rarely found in natural populations of outcrossing species, even between very closely linked loci. Interestingly, we found that most instances of significant interallelic GD (68%) involved functionally related protein loci. Specifically, GD was markedly more frequent between protein loci related by the functions of hormonal control, molybdenum control, antioxidant defense system, and reproduction than between loci without known functional relationship, which is indicative of epistatic selection. Furthermore, long-distance GD between functionally related loci (mean EFR 9 cM) suggests that epistatic interactions must be very strong along the chromosome. This evidence is hardly compatible with the neutral theory and has far-reaching implications for understanding the multilocus architecture of the functional genome. Our findings also suggest that GD may be a useful tool for discovering networks of functionally interacting proteins.
机译:蛋白质基因座之间配子不平衡(GD)的染色体内分布以及该分布的潜在进化因子仍然是未知的。在这里,我们报告了对来自单个自然种群的大量单倍型样本(600个)中大量蛋白质位点(15个)跨越果蝇第三个染色体总长度的87%的GD的详细研究。我们使用了最近为多等位基因系统开发的基于符号的GD估计方法,该方法大大提高了GD强度的统计功效和估计准确性。我们发现成对的蛋白质基因座之间的强GD分布在整个染色体中。总共,等位基因对和基因座对中的22%处于显着的GD中,平均强度(通过D'系数测量)分别为0.43和0.31。此外,强GD通常发生在相距较远的基因座之间。举例说明,显着GD中的等位基因对的32%发生在由有效重组频率(EFR)为15-20cM分开的基因座对中,平均D'值为0.49。这些观察结果与以前的研究形成鲜明对比,以前的研究表明,在异源物种的自然种群中,即使在非常紧密联系的基因座之间,也很少发现蛋白质基因座之间的GD。有趣的是,我们发现大多数重要的等位基因GD(68%)都涉及功能相关的蛋白质基因座。特别地,与没有已知功能关系的基因座之间的GD相比,与激素控制,钼控制,抗氧化防御系统和繁殖相关的蛋白质基因座之间的GD明显更频繁。此外,功能相关基因座之间的长距离GD(平均EFR 9 cM)表明上位性相互作用在染色体上必须非常强。该证据与中性理论几乎不相容,并且对于理解功能基因组的多基因座结构具有深远的意义。我们的发现还表明,GD可能是发现功能相互作用蛋白网络的有用工具。

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