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Family-Based Association Test Using Both Common and Rare Variants and Accounting for Directions of Effects for Sequencing Data

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  • Ren-Hua Chung
  • Wei-Yun Tsai
  • Eden R Martin

Abstract

Current family-based association tests for sequencing data were mainly developed for identifying rare variants associated with a complex disease. As the disease can be influenced by the joint effects of common and rare variants, common variants with modest effects may not be identified by the methods focusing on rare variants. Moreover, variants can have risk, neutral, or protective effects. Association tests that can effectively select groups of common and rare variants that are likely to be causal and consider the directions of effects have become important. We developed the Ordered Subset - Variable Threshold - Pedigree Disequilibrium Test (OVPDT), a combination of three algorithms, for association analysis in family sequencing data. The ordered subset algorithm is used to select a subset of common variants based on their relative risks, calculated using only parental mating types. The variable threshold algorithm is used to search for an optimal allele frequency threshold such that rare variants below the threshold are more likely to be causal. The PDT statistics from both rare and common variants selected by the two algorithms are combined as the OVPDT statistic. A permutation procedure is used in OVPDT to calculate the p-value. We used simulations to demonstrate that OVPDT has the correct type I error rates under different scenarios and compared the power of OVPDT with two other family-based association tests. The results suggested that OVPDT can have more power than the other tests if both common and rare variants have effects on the disease in a region.

Suggested Citation

  • Ren-Hua Chung & Wei-Yun Tsai & Eden R Martin, 2014. "Family-Based Association Test Using Both Common and Rare Variants and Accounting for Directions of Effects for Sequencing Data," PLOS ONE, Public Library of Science, vol. 9(9), pages 1-7, September.
  • Handle: RePEc:plo:pone00:0107800
    DOI: 10.1371/journal.pone.0107800
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    References listed on IDEAS

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    1. Iuliana Ionita-Laza & Joseph D Buxbaum & Nan M Laird & Christoph Lange, 2011. "A New Testing Strategy to Identify Rare Variants with Either Risk or Protective Effect on Disease," PLOS Genetics, Public Library of Science, vol. 7(2), pages 1-6, February.
    2. Benjamin M Neale & Manuel A Rivas & Benjamin F Voight & David Altshuler & Bernie Devlin & Marju Orho-Melander & Sekar Kathiresan & Shaun M Purcell & Kathryn Roeder & Mark J Daly, 2011. "Testing for an Unusual Distribution of Rare Variants," PLOS Genetics, Public Library of Science, vol. 7(3), pages 1-8, March.
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