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A common variant in CCDC93 protects against myocardial infarction and cardiovascular mortality by regulating endosomal trafficking of low-density lipoprotein receptor

Authors :
Rimbert, Antoine
Dalila, Nawar
Wolters, Justina C.
Huijkman, Nicolette
Smit, Marieke
Kloosterhuis, Niels
Riemsma, Marijn
Van Der Veen, Ydwine
Singla, Amika
Van Dijk, Freerk
Frikke-Schmidt, Ruth
Burstein, Ezra
Tybjærg-Hansen, Anne
Van De Sluis, Bart
Kuivenhoven, Jan Albert
Rimbert, Antoine
Dalila, Nawar
Wolters, Justina C.
Huijkman, Nicolette
Smit, Marieke
Kloosterhuis, Niels
Riemsma, Marijn
Van Der Veen, Ydwine
Singla, Amika
Van Dijk, Freerk
Frikke-Schmidt, Ruth
Burstein, Ezra
Tybjærg-Hansen, Anne
Van De Sluis, Bart
Kuivenhoven, Jan Albert
Source :
Rimbert , A , Dalila , N , Wolters , J C , Huijkman , N , Smit , M , Kloosterhuis , N , Riemsma , M , Van Der Veen , Y , Singla , A , Van Dijk , F , Frikke-Schmidt , R , Burstein , E , Tybjærg-Hansen , A , Van De Sluis , B & Kuivenhoven , J A 2020 , ' A common variant in CCDC93 protects against myocardial infarction and cardiovascular mortality by regulating endosomal trafficking of low-density lipoprotein receptor ' , European Heart Journal , vol. 41 , no. 9 , pp. 1040-1053 .
Publication Year :
2020

Abstract

Aims Genome-wide association studies have previously identified INSIG2 as a candidate gene for plasma low-density lipoprotein cholesterol (LDL-c). However, we suspect a role for CCDC93 in the same locus because of its involvement in the recycling of the LDL-receptor (LDLR). Methods and results Characterization of the INSIG2 locus was followed by studies in over 107 000 individuals from the general population, the Copenhagen General Population Study and the Copenhagen City Heart Study, for associations of genetic variants with plasma lipids levels, with risk of myocardial infarction (MI) and with cardiovascular mortality. CCDC93 was furthermore studied in cells and mice. The lead variant of the INSIG2 locus (rs10490626) is not associated with changes in the expression of nearby genes but is a part of a genetic block, which excludes INSIG2. This block includes a coding variant in CCDC93 p.Pro228Leu, which is in strong linkage disequilibrium with rs10490626 (r2 > 0.96). In the general population, separately and combined, CCDC93 p.Pro228Leu is dose-dependently associated with lower LDL-c (P-trend 2.5 ×10-6 to 8.0 ×10-9), with lower risk of MI (P-trend 0.04-0.002) and lower risk of cardiovascular mortality (P-trend 0.005-0.004). These results were validated for LDL-c, risk of both coronary artery disease and MI in meta-analyses including from 194 000 to >700 000 participants. The variant is shown to increase CCDC93 protein stability, while overexpression of human CCDC93 decreases plasma LDL-c in mice. Conversely, CCDC93 ablation reduces LDL uptake as a result of reduced LDLR levels at the cell membrane. Conclusion This study provides evidence that a common variant in CCDC93, encoding a protein involved in recycling of the LDLR, is associated with lower LDL-c levels, lower risk of MI and cardiovascular mortality.

Details

Database :
OAIster
Journal :
Rimbert , A , Dalila , N , Wolters , J C , Huijkman , N , Smit , M , Kloosterhuis , N , Riemsma , M , Van Der Veen , Y , Singla , A , Van Dijk , F , Frikke-Schmidt , R , Burstein , E , Tybjærg-Hansen , A , Van De Sluis , B & Kuivenhoven , J A 2020 , ' A common variant in CCDC93 protects against myocardial infarction and cardiovascular mortality by regulating endosomal trafficking of low-density lipoprotein receptor ' , European Heart Journal , vol. 41 , no. 9 , pp. 1040-1053 .
Notes :
application/pdf, English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1322752890
Document Type :
Electronic Resource