Choice of transcripts and software has a large effect on variant annotation

Davis J McCarthy; Peter Humburg; Alexander Kanapin; Manuel A Rivas; Kyle Gaulton; Jean-Baptiste Cazier; Peter Donnelly

doi:10.1186/gm543

Choice of transcripts and software has a large effect on variant annotation

Genome Med. 2014 Mar 31;6(3):26. doi: 10.1186/gm543. eCollection 2014.

Authors

Davis J McCarthy¹, Peter Humburg², Alexander Kanapin², Manuel A Rivas², Kyle Gaulton², Jean-Baptiste Cazier³, Peter Donnelly¹

Affiliations

¹ Department of Statistics, University of Oxford, South Parks Road, Oxford, UK ; Wellcome Trust Centre for Human Genetics, University of Oxford, Roosevelt Drive, Oxford, UK.
² Wellcome Trust Centre for Human Genetics, University of Oxford, Roosevelt Drive, Oxford, UK.
³ Department of Oncology, University of Oxford, Roosevelt Drive, Oxford, UK.

PMID: 24944579
PMCID: PMC4062061
DOI: 10.1186/gm543

Abstract

Background: Variant annotation is a crucial step in the analysis of genome sequencing data. Functional annotation results can have a strong influence on the ultimate conclusions of disease studies. Incorrect or incomplete annotations can cause researchers both to overlook potentially disease-relevant DNA variants and to dilute interesting variants in a pool of false positives. Researchers are aware of these issues in general, but the extent of the dependency of final results on the choice of transcripts and software used for annotation has not been quantified in detail.

Methods: This paper quantifies the extent of differences in annotation of 80 million variants from a whole-genome sequencing study. We compare results using the RefSeq and Ensembl transcript sets as the basis for variant annotation with the software Annovar, and also compare the results from two annotation software packages, Annovar and VEP (Ensembl's Variant Effect Predictor), when using Ensembl transcripts.

Results: We found only 44% agreement in annotations for putative loss-of-function variants when using the RefSeq and Ensembl transcript sets as the basis for annotation with Annovar. The rate of matching annotations for loss-of-function and nonsynonymous variants combined was 79% and for all exonic variants it was 83%. When comparing results from Annovar and VEP using Ensembl transcripts, matching annotations were seen for only 65% of loss-of-function variants and 87% of all exonic variants, with splicing variants revealed as the category with the greatest discrepancy. Using these comparisons, we characterised the types of apparent errors made by Annovar and VEP and discuss their impact on the analysis of DNA variants in genome sequencing studies.

Conclusions: Variant annotation is not yet a solved problem. Choice of transcript set can have a large effect on the ultimate variant annotations obtained in a whole-genome sequencing study. Choice of annotation software can also have a substantial effect. The annotation step in the analysis of a genome sequencing study must therefore be considered carefully, and a conscious choice made as to which transcript set and software are used for annotation.

Abstract

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