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Testing for an unusual distribution of rare variants.检测罕见变异的异常分布。
PLoS Genet. 2011 Mar;7(3):e1001322. doi: 10.1371/journal.pgen.1001322. Epub 2011 Mar 3.
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A new testing strategy to identify rare variants with either risk or protective effect on disease.一种新的检测策略,用于识别对疾病具有风险或保护作用的罕见变异。
PLoS Genet. 2011 Feb 3;7(2):e1001289. doi: 10.1371/journal.pgen.1001289.
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A unified framework for multi-locus association analysis of both common and rare variants.一种用于常见和罕见变异体的多基因座关联分析的统一框架。
BMC Genomics. 2011 Jan 31;12:89. doi: 10.1186/1471-2164-12-89.
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Extending rare-variant testing strategies: analysis of noncoding sequence and imputed genotypes.扩展罕见变异测试策略:非编码序列和推断基因型分析。
Am J Hum Genet. 2010 Nov 12;87(5):604-17. doi: 10.1016/j.ajhg.2010.10.012.
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A map of human genome variation from population-scale sequencing.人类基因组变异的图谱来自于基于人群的测序。
Nature. 2010 Oct 28;467(7319):1061-73. doi: 10.1038/nature09534.
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A covering method for detecting genetic associations between rare variants and common phenotypes.一种用于检测罕见变异与常见表型之间遗传关联的覆盖方法。
PLoS Comput Biol. 2010 Oct 14;6(10):e1000954. doi: 10.1371/journal.pcbi.1000954.
7
CCRaVAT and QuTie-enabling analysis of rare variants in large-scale case control and quantitative trait association studies.大规模病例对照和数量性状关联研究中罕见变异的 CCRaVAT 和 QuTie 分析。
BMC Bioinformatics. 2010 Oct 21;11:527. doi: 10.1186/1471-2105-11-527.
8
Pooled association tests for rare variants in exon-resequencing studies.外显子重测序研究中罕见变异的合并关联分析。
Am J Hum Genet. 2010 Jun 11;86(6):832-8. doi: 10.1016/j.ajhg.2010.04.005. Epub 2010 May 13.
9
A data-adaptive sum test for disease association with multiple common or rare variants.一种用于疾病与多个常见或罕见变异关联的数据自适应总和检验。
Hum Hered. 2010;70(1):42-54. doi: 10.1159/000288704. Epub 2010 Apr 23.
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An evaluation of statistical approaches to rare variant analysis in genetic association studies.遗传关联研究中罕见变异分析的统计方法评估。
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ARIEL和AMELIA:使用下一代测序数据检测罕见变异的积累情况。

ARIEL and AMELIA: testing for an accumulation of rare variants using next-generation sequencing data.

作者信息

Asimit Jennifer L, Day-Williams Aaron G, Morris Andrew P, Zeggini Eleftheria

机构信息

Wellcome Trust Sanger Institute, Hinxton, UK.

出版信息

Hum Hered. 2012;73(2):84-94. doi: 10.1159/000336982. Epub 2012 Mar 22.

DOI:10.1159/000336982
PMID:22441326
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3477640/
Abstract

OBJECTIVES

There is increasing evidence that rare variants play a role in some complex traits, but their analysis is not straightforward. Locus-based tests become necessary due to low power in rare variant single-point association analyses. In addition, variant quality scores are available for sequencing data, but are rarely taken into account. Here, we propose two locus-based methods that incorporate variant quality scores: a regression-based collapsing approach and an allele-matching method.

METHODS

Using simulated sequencing data we compare 4 locus-based tests of trait association under different scenarios of data quality. We test two collapsing-based approaches and two allele-matching-based approaches, taking into account variant quality scores and ignoring variant quality scores. We implement the collapsing and allele-matching approaches accounting for variant quality in the freely available ARIEL and AMELIA software.

RESULTS

The incorporation of variant quality scores in locus-based association tests has power advantages over weighting each variant equally. The allele-matching methods are robust to the presence of both protective and risk variants in a locus, while collapsing methods exhibit a dramatic loss of power in this scenario.

CONCLUSIONS

The incorporation of variant quality scores should be a standard protocol when performing locus-based association analysis on sequencing data. The ARIEL and AMELIA software implement collapsing and allele-matching locus association analysis methods, respectively, that allow the incorporation of variant quality scores.

摘要

目的

越来越多的证据表明,罕见变异在某些复杂性状中发挥作用,但其分析并非易事。由于罕见变异单点关联分析的效能较低,基于位点的检验变得必要。此外,测序数据有变异质量得分,但很少被考虑在内。在此,我们提出两种纳入变异质量得分的基于位点的方法:一种基于回归的合并方法和一种等位基因匹配方法。

方法

使用模拟测序数据,我们在不同数据质量场景下比较4种基于位点的性状关联检验。我们测试了两种基于合并的方法和两种基于等位基因匹配的方法,同时考虑了变异质量得分和忽略变异质量得分的情况。我们在免费提供的ARIEL和AMELIA软件中实现了考虑变异质量的合并和等位基因匹配方法。

结果

在基于位点的关联检验中纳入变异质量得分比平等加权每个变异具有效能优势。等位基因匹配方法对一个位点中同时存在保护性和风险性变异具有稳健性,而合并方法在这种情况下效能会显著降低。

结论

在对测序数据进行基于位点的关联分析时,纳入变异质量得分应成为标准方案。ARIEL和AMELIA软件分别实现了合并和等位基因匹配的位点关联分析方法,这些方法允许纳入变异质量得分。