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本文引用的文献

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DNA polymorphism adjacent to human apoprotein A-1 gene: relation to hypertriglyceridaemia.人类载脂蛋白A-1基因附近的DNA多态性:与高甘油三酯血症的关系。
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Estimation of linkage disequilibrium in randomly mating populations.随机交配群体中连锁不平衡的估计。
Heredity (Edinb). 1974 Oct;33(2):229-39. doi: 10.1038/hdy.1974.89.
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The use of measured genotype information in the analysis of quantitative phenotypes in man. II. The role of the apolipoprotein E polymorphism in determining levels, variability, and covariability of cholesterol, betalipoprotein, and triglycerides in a sample of unrelated individuals.
Am J Med Genet. 1987 Jul;27(3):567-82. doi: 10.1002/ajmg.1320270310.
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The general relationship between average effect and average excess.
Genet Res. 1987 Feb;49(1):69-70. doi: 10.1017/s0016672300026756.
5
Molecular population genetics of the alcohol dehydrogenase gene region of Drosophila melanogaster.黑腹果蝇乙醇脱氢酶基因区域的分子群体遗传学
Genetics. 1986 Dec;114(4):1165-90. doi: 10.1093/genetics/114.4.1165.
6
A study of DNA polymorphisms around the human apolipoprotein AI gene in hyperlipidaemic and normal individuals.高脂血症患者和正常人载脂蛋白AI基因周围DNA多态性的研究。
Clin Genet. 1985 Oct;28(4):296-306. doi: 10.1111/j.1399-0004.1985.tb00403.x.
7
Deoxyribonucleic acid polymorphism in the apolipoprotein A-1-C-III gene cluster. Association with hypertriglyceridemia.载脂蛋白A-1-C-III基因簇中的脱氧核糖核酸多态性。与高甘油三酯血症的关联。
J Clin Invest. 1985 Sep;76(3):1090-5. doi: 10.1172/JCI112062.
8
A cladistic analysis of phenotypic associations with haplotypes inferred from restriction endonuclease mapping. I. Basic theory and an analysis of alcohol dehydrogenase activity in Drosophila.基于限制性内切酶图谱推断的单倍型与表型关联的分支系统分析。I. 基本理论及果蝇乙醇脱氢酶活性分析
Genetics. 1987 Oct;117(2):343-51. doi: 10.1093/genetics/117.2.343.

基于限制性内切酶图谱推断的单倍型与表型关联的分支分析。II. 自然种群分析。

A cladistic analysis of phenotype associations with haplotypes inferred from restriction endonuclease mapping. II. The analysis of natural populations.

作者信息

Templeton A R, Sing C F, Kessling A, Humphries S

机构信息

Department of Biology, Washington University, St. Louis, Missouri 63130.

出版信息

Genetics. 1988 Dec;120(4):1145-54. doi: 10.1093/genetics/120.4.1145.

DOI:10.1093/genetics/120.4.1145
PMID:3147219
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1203577/
Abstract

Genes that code for products involved in the physiology of a phenotype are logical candidates for explaining interindividual variation in that phenotype. We present a methodology for discovering associations between genetic variation at such candidate loci (assayed through restriction endonuclease mapping) with phenotypic variation at the population level. We confine our analyses to DNA regions in which recombination is very rare. In this case, the genetic variation at the candidate locus can be organized into a cladogram that represents the evolutionary relationships between the observed haplotypes. Any mutation causing a significant phenotypic effect should be imbedded within the same historical structure defined by the cladogram. We showed, in the first paper of this series, how to use the cladogram to define a nested analysis of variance (NANOVA) that was very efficient at detecting and localizing phenotypically important mutations. However, the NANOVA of haplotype effects could only be applied to populations of homozygous genotypes. In this paper, we apply the quantitative genetic concept of average excess to evaluate the phenotypic effect of a haplotype or group of haplotypes stratified and contrasted according to the nested design defined by the cladogram. We also show how a permutational procedure can be used to make statistical inferences about the nested average excess values in populations containing heterozygous as well as homozygous genotypes. We provide two worked examples that investigate associations between genetic variation at or near the Alcohol dehydrogenase (Adh) locus and Adh activity in Drosophila melanogaster, and associations between genetic variation at or near some apolipoprotein loci and various lipid phenotypes in a human population.

摘要

编码参与某一表型生理过程产物的基因,是解释该表型个体间差异的合理候选基因。我们提出了一种方法,用于发现此类候选基因座处的遗传变异(通过限制性内切酶图谱分析)与群体水平上的表型变异之间的关联。我们将分析局限于重组非常罕见的DNA区域。在这种情况下,候选基因座处的遗传变异可以组织成一个分支图,该图代表了观察到的单倍型之间的进化关系。任何引起显著表型效应的突变都应包含在由分支图定义的相同历史结构内。在本系列的第一篇论文中,我们展示了如何使用分支图来定义一种嵌套方差分析(NANOVA),这种分析在检测和定位具有重要表型意义的突变方面非常有效。然而,单倍型效应的NANOVA只能应用于纯合基因型群体。在本文中,我们应用平均超额的数量遗传概念,来评估根据分支图定义的嵌套设计进行分层和对比的单倍型或单倍型组的表型效应。我们还展示了如何使用一种置换程序,对包含杂合和纯合基因型的群体中的嵌套平均超额值进行统计推断。我们提供了两个实例,分别研究了果蝇中乙醇脱氢酶(Adh)基因座或其附近的遗传变异与Adh活性之间的关联,以及人类群体中某些载脂蛋白基因座或其附近的遗传变异与各种脂质表型之间的关联。