TY  - JOUR
A1  - Robinson, Peter
A1  - Köhler, Sebastian
A1  - Oellrich, Anika
A1  - Sanger Mouse Genetics Project
A1  - Wang, Kai
A1  - Mungall, Chris
A1  - Lewis, Suzanna E
A1  - Washington, Nicole
A1  - Bauer, Sebastian
A1  - Seelow, Dominik Seelow
A1  - Krawitz, Peter
A1  - Gilissen, Christian
A1  - Haendel, Melissa
A1  - Smedley, Damian
T1  - Improved exome prioritization of disease genes through cross species phenotype comparison
Y1  - 2013/10/25 
JF  - Genome Research 
JO  - Genome Research 
DO  - 10.1101/gr.160325.113 
SP  - gr.160325.113 
UR  - http://genome.cshlp.org/content/early/2013/10/25/gr.160325.113.abstract 
N2  - Numerous new disease-gene associations have been identified by whole-exome sequencing studies in the last few years. However, many cases remain unsolved due to the sheer number of candidate variants remaining after common filtering strategies such as removing low quality and common variants and those deemed unlikely to be pathogenic (non-coding, not affecting splicing, synonymous or missense mutations annotated as non-pathogenic by prediction algorithms). The observation that each of our genomes contains about 100 genuine loss of function variants with ~20 genes completely inactivated makes identification of the causative mutation problematic when using these strategies alone. In some cases it may be possible to use multiple affected individuals, linkage data, identity-by-descent inference, de novo heterozygous mutations from trio analysis, or prior knowledge of affected pathways to narrow down to the causative variant. In cases where this is not possible or has proven unsuccessful we propose using the wealth of genotype to phenotype data that already exists from model organism studies to assess the potential impact of these exome variants. Here, we introduce PHenotypic Interpretation of Variants in Exomes (PHIVE), an algorithm that integrates the calculation of phenotype similarity between human diseases and genetically modified mouse models with evaluation of the variants according to allele frequency, pathogenicity and mode of inheritance approaches in our Exomiser tool. Large-scale validation of PHIVE analysis using 100,000 exomes containing known mutations demonstrated a substantial improvement (up to 54.1 fold) over purely variant-based (frequency and pathogenicity) methods with the correct gene recalled as the top hit in up to 83% of samples, corresponding to an area under the ROC curve of over 95%. We conclude that incorporation of phenotype data can play a vital role in translational bioinformatics and propose that exome sequencing projects should systematically capture clinical phenotypes to take advantage of the strategy presented here. 
ER  -