Assessing the functional consequence of loss of function variants using electronic medical record and large-scale genomics consortium efforts

Patrick Sleiman; Jonathan Bradfield; Frank Mentch; Berta Almoguera; John Connolly; Hakon Hakonarson

doi:10.3389/fgene.2014.00105

Assessing the functional consequence of loss of function variants using electronic medical record and large-scale genomics consortium efforts

Front Genet. 2014 Apr 29:5:105. doi: 10.3389/fgene.2014.00105. eCollection 2014.

Authors

Patrick Sleiman¹, Jonathan Bradfield², Frank Mentch², Berta Almoguera², John Connolly², Hakon Hakonarson¹

Affiliations

¹ Center for Applied Genomics, Abramson Research Center, The Children's Hospital of Philadelphia Philadelphia, PA, USA ; Department of Pediatrics, Perelman School of Medicine, University of Pennsylvania Philadelphia, PA, USA.
² Center for Applied Genomics, Abramson Research Center, The Children's Hospital of Philadelphia Philadelphia, PA, USA.

Abstract

Estimates from large scale genome sequencing studies indicate that each human carries up to 20 genetic variants that are predicted to results in loss of function (LOF) of protein-coding genes. While some are known disease-causing variants or common, tolerated, LOFs in non-essential genes, the majority remain of unknown consequence. We explore the possibility of using imputed GWAS data from large biorepositories such as the electronic medical record and genomics (eMERGE) consortium to determine the effects of rare LOFs. Here, we show that two hypocholesterolemia-associated LOF mutations in the PCSK9 gene can be accurately imputed into large-scale GWAS datasets which raises the possibility of assessing LOFs through genomics-linked medical records.

Keywords: PCSK9; biorepository; eMERGE; imputation; loss of function (LOF).

Grants and funding

U01 HG006830/HG/NHGRI NIH HHS/United States