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An automatic and efficient pipeline for disease gene identification through utilizing family-based sequencing data

Issue title: Frontiers in Biomedical Engineering and Biotechnology – Proceedings of the 4th International Conference on Biomedical Engineering and Biotechnology, 18–21 August 2015, Shanghai, China

Guest editors: Feng Liu, Dong-Hoon Lee, Ricardo Lagoa and Sandeep Kumar

Article type: Research Article

Authors: Song, Dandan | Li, Ning | Liao, Lejian; *

Affiliations: Beijing Engineering Research Center of High Volume Language Information Processing and Cloud Computing Applications, Beijing Lab of Intelligent Information Technology, School of Computer Science and Technology, Beijing Institute of Technology, Beijing, China

Correspondence: [*] Address for correspondence: Lejian Liao, Beijing Engineering Research Center of High Volume Language Information Processing and Cloud Computing Applications, Beijing Lab of Intelligent Information Technology, School of Computer Science and Technology, Beijing Institute of Technology, Beijing, China. Tel.: +86-1068913536; Fax: +86-1068913536; E-mail: [email protected].

Keywords: Mendelian disorders, disease gene identification, whole-exome sequencing

DOI: 10.3233/BME-151481

Journal: Bio-Medical Materials and Engineering, vol. 26, no. s1, pp. S1797-S1803, 2015

Published: 2015
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Due to the generation of enormous amounts of data at both lower costs as well as in shorter times, whole-exome sequencing technologies provide dramatic opportunities for identifying disease genes implicated in Mendelian disorders. Since upwards of thousands genomic variants can be sequenced in each exome, it is challenging to filter pathogenic variants in protein coding regions and reduce the number of missing true variants. Therefore, an automatic and efficient pipeline for finding disease variants in Mendelian disorders is designed by exploiting a combination of variants filtering steps to analyze the family-based exome sequencing approach. Recent studies on the Freeman-Sheldon disease are revisited and show that the proposed method outperforms other existing candidate gene identification methods.

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