The Impact of Partial and Complete Loss-of-Function Mutations in Endothelial Lipase on High-Density Lipoprotein Levels and Functionality in Humans

Author:

Singaraja Roshni R.1,Sivapalaratnam Suthesh1,Hovingh Kees1,Dubé Marie-Pierre1,Castro-Perez José1,Collins Heidi L.1,Adelman Steven J.1,Riwanto Meliana1,Manz Jasmin1,Hubbard Brian1,Tietjen Ian1,Wong Kenny1,Mitnaul Lyndon J.1,van Heek Margaret1,Lin Linus1,Roddy Thomas A.1,McEwen Jason1,Dallinge-Thie Geesje1,van Vark-van der Zee Leonie1,Verwoert Germaine1,Winther Michael1,van Duijn Cornelia1,Hofman Albert1,Trip Mieke D.1,Marais A. David1,Asztalos Bela1,Landmesser Ulf1,Sijbrands Eric1,Kastelein John J.1,Hayden Michael R.1

Affiliation:

1. From the Xenon Pharmaceuticals Inc., Burnaby, Canada (R.R.S., I.T., J.Mc., M.W.); Department of Vascular Medicine (S.S., K.H., G.D.-T., J.J.K.), Department of Cardiology (M.D.T.), Academic Medical Center, Amsterdam, the Netherlands; Montreal Heart Institute Research Center and Université de Montréal Faculté de Médecine, Montréal, Canada (M.-P.D.); Merck Research Laboratories, Rahway, NJ (J.C.-P., B.H., K.W., L.J.M., M.v.H., L.L., T.A.R.); Vascular Strategies LLC, Wynnewood, PA (H.L.C., S.J.A.);...

Abstract

Background— Endothelial lipase is a phospholipase with activity against high-density lipoprotein. Although a small number of mutations in LIPG have been described, the role of LIPG in protection against atherosclerosis is unclear. Methods and Results— We identified 8 loss-of-function (LOF) mutations in LIPG in individuals with high-density lipoprotein cholesterol. Functional analysis confirmed that most rare mutations abolish lipase activity in vitro, indicating complete LOF, whereas 2 more common mutations N396S and R476W reduce activity by ≈50%, indicating partial LOF and implying ≈50% and ≈75% remaining endothelial lipase function in heterozygous complete LOF and partial LOF mutation carriers, respectively. complete LOF mutation carriers had significantly higher plasma high-density lipoprotein cholesterol levels compared with partial LOF mutation carriers. Apolipoprotein B-depleted serum from complete LOF carriers showed significantly enhanced cholesterol efflux acceptor capacity, whereas only trends were observed in partial LOF carriers. Carriers of LIPG mutations exhibited trends toward reduced coronary artery disease in 4 independent cohorts (meta-analysis odds ratio, 0.7; P =0.04). Conclusions— Our data suggest that the impact of LIPG mutations is directly related to their effect on endothelial lipase function and support that antagonism of endothelial lipase function improves cardioprotection.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Genetics(clinical),Cardiology and Cardiovascular Medicine,Genetics

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