4.7 Article

Ranking of genome-wide association scan signals by different measures

期刊

INTERNATIONAL JOURNAL OF EPIDEMIOLOGY
卷 38, 期 5, 页码 1364-1373

出版社

OXFORD UNIV PRESS
DOI: 10.1093/ije/dyp285

关键词

Bayes factor; effect size; likelihood ratio; single nucleotide polymorphism; statistical power; statistics

资金

  1. Swedish Council for Working Life and Social Research [2007-0153]
  2. Swedish Research Council [2007-22238-47298-36]
  3. Swedish Cancer Fund [080401]
  4. Wellcome trust [WT088885/Z/09/Z]
  5. Medical Research Council [G0801056B] Funding Source: researchfish

向作者/读者索取更多资源

Background The P-value approach has been employed to prioritizing genome-wide association (GWA) scan signals, with a genome-wide significance defined by a prior P-value threshold, although this is not ideal. A rationale put forward is that the association signals rather should be expected to give less support for single nucleotide polymorphisms (SNPs) that are rare (with associated low-power tests) than for common SNPs with equivalent P-values, unless investigators believe, a priori, that rare causative variants contribute to the disease and have more pronounced effects. Methods Using data from a GWA scan for type 2 diabetes (1924 cases, 2938 controls, 393453 SNPs), we compared P-values with four alternative signal measures: likelihood ratio (1,R), Bayes factor (BF; with a specified prior distribution for true effects), 'frequentist factor' (FF; reflecting the ratio between estimated-post-data- 'power' and P-value) and probability of pronounced effect size (PrPES). Results The 19 common SNPs [minor allele frequency (MAF) among the controls > 29%] yielding strong P-value signals (P < 5 x 10(-7)) were also top ranked by the other approaches. There was a strong similarity between the P-values, LR and BF signals, in terms of ranking SNPs. In contrast, FF and PrPES signals down-weighted rare SNPs (control MAF < 10%) with low P-values. Conclusions For prioritization of signals that do not achieve compelling levels of evidence for association, the main driving force behind observed differences between the various association signals appears to be SNP MAR The statistical power afforded by follow-up samples for establishing replication should be taken into account when tailoring the signal selection strategy.

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