A rare variant in APOC3 is associated with plasma triglyceride and VLDL levels in Europeans

Author:

Timpson Nicholas J., ,Walter Klaudia,Min Josine L.,Tachmazidou Ioanna,Malerba Giovanni,Shin So-Youn,Chen Lu,Futema Marta,Southam Lorraine,Iotchkova Valentina,Cocca Massimiliano,Huang Jie,Memari Yasin,McCarthy Shane,Danecek Petr,Muddyman Dawn,Mangino Massimo,Menni Cristina,Perry John R. B.,Ring Susan M.,Gaye Amadou,Dedoussis George,Farmaki Aliki-Eleni,Burton Paul,Talmud Philippa J.,Gambaro Giovanni,Spector Tim D.,Smith George Davey,Durbin Richard,Richards J Brent,Humphries Steve E.,Zeggini Eleftheria,Soranzo Nicole

Abstract

Abstract The analysis of rich catalogues of genetic variation from population-based sequencing provides an opportunity to screen for functional effects. Here we report a rare variant in APOC3 (rs138326449-A, minor allele frequency ~0.25% (UK)) associated with plasma triglyceride (TG) levels (−1.43 s.d. (s.e.=0.27 per minor allele (P-value=8.0 × 10−8)) discovered in 3,202 individuals with low read-depth, whole-genome sequence. We replicate this in 12,831 participants from five additional samples of Northern and Southern European origin (−1.0 s.d. (s.e.=0.173), P-value=7.32 × 10−9). This is consistent with an effect between 0.5 and 1.5 mmol l−1 dependent on population. We show that a single predicted splice donor variant is responsible for association signals and is independent of known common variants. Analyses suggest an independent relationship between rs138326449 and high-density lipoprotein (HDL) levels. This represents one of the first examples of a rare, large effect variant identified from whole-genome sequencing at a population scale.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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