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Improving the Power of Rare-Variant Association Tests by a Position-Dependent Kernel Approach

Publikation: Beitrag in Buch/Bericht/KonferenzbandKonferenzbeitragBegutachtung

Abstract

Current high-throughput sequencing technologies have allowed for an easy and cost-efficient identification of rare single-nucleotide variations (SNVs), many of which have already been proven to be associated with diseases or complex traits. Despite these successes, genomewide association studies involving rare variants remain statistically challenging. Classical single-SNV association studies particularly suffer from poor statistical power, as the potentially large number of SNVs often leads to poor significance upon false discovery rate (FDR) correction. To overcome these difficulties, approaches have been proposed that do not consider all SNVs individually; instead, they group SNVs and perform tests on those groups. This can either be done by grouping SNVs that are in the same genomic region of interest (e.g. the same transcript or exon) or by windowing along each chromosome. The choice of the groups/windows is crucial: FDR correction does not pose a serious problem if there are large, and consequently fewer, windows, but the local tests have poor power for large windows. If smaller windows, and consequently a larger number thereof, are chosen, the local tests perform well, but FDR correction nullifies this advantage. For more see http://www.bioinf.jku.at/publications/2012/HGV2012_Bodenhofer.pdf
OriginalspracheEnglisch
TitelHGV 2012 Proceedings
Seitenumfang1
PublikationsstatusVeröffentlicht - 2012

Wissenschaftszweige

  • 106013 Genetik
  • 106041 Strukturbiologie
  • 102 Informatik
  • 101029 Mathematische Statistik
  • 102001 Artificial Intelligence
  • 101004 Biomathematik
  • 102015 Informationssysteme
  • 102018 Künstliche Neuronale Netze
  • 106002 Biochemie
  • 106023 Molekularbiologie
  • 305 Andere Humanmedizin, Gesundheitswissenschaften
  • 106005 Bioinformatik

JKU-Schwerpunkte

  • Computation in Informatics and Mathematics
  • Nano-, Bio- and Polymer-Systems: From Structure to Function

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