An LRP8 Variant Is Associated with Familial and Premature Coronary Artery Disease and Myocardial Infarction

Shen, Gong-Qing; Li, Lin; Girelli, Domenico; Seidelmann, Sara B.; Rao, Shaoqi; Fan, Chun; Park, Jeong Euy; Xi, Quansheng; Li, Jing; Hu, Yan; Olivieri, Oliviero; Marchant, Kandice; Barnard, John; Corrocher, Roberto; Elston, Robert C.; Cassano, June; Henderson, Susan; Hazen, Stanley L.; Plow, Edward F.; Topol, Eric J.; Wang, Qing Kenneth

doi:10.1086/521581

Cited by 77 publications

(92 citation statements)

References 30 publications

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“…There is greater cardiovascular disease risk associated with the apoE4 allele vs. apoE3, and also with the ApoER2 variant ApoER2-R952Q, and there is evidence that the increased disease predisposition may be related to mechanisms other than changes in lipid status (3)(4)(5)(6)(7)(8)(9). How ApoER2 and its interactive actions with apoE potentially influence the behavior of endothelial cells, which are critically involved in vascular health and disease, has been unknown.…”

Section: Discussionmentioning

confidence: 99%

“…The LRP8 gene, which encodes ApoER2, is a major gene locus for premature atherosclerosis and acute myocardial infarction identified in four independent human populations. In particular, homozygous carriers of the ApoER2-R952Q variant have a twofold increased risk of these conditions (3)(4)(5). ApoER2-R952Q also has an additive effect with apoE4, with the combined genotype QQ/E4 showing a 3.9-fold greater susceptibility to cardiovascular disease (5).…”

mentioning

confidence: 99%

“…ApoER2-R952Q also has an additive effect with apoE4, with the combined genotype QQ/E4 showing a 3.9-fold greater susceptibility to cardiovascular disease (5). ApoER2 polymorphism-associated risk is independent of cholesterol levels (3)(4)(5), and although apoE4 may impact LDL abundance (2), there is also evidence that apoE4-associated risk goes well beyond changes in lipoprotein status (6)(7)(8)(9). Whereas there is considerable understanding of the biology of the apoE-ApoER2 tandem in the central nervous system and in Alzheimer's disease (10), the basis for the cardiovascular impact of the receptor and apoE variants remains unclear.…”

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confidence: 99%

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Genetic variants of ApoE and ApoER2 differentially modulate endothelial function

Ulrich

Konaniah

Herz³

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

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It is poorly understood why there is greater cardiovascular disease risk associated with the apolipoprotein E4 (apoE) allele vs. apoE3, and also greater risk with the LRP8/apolipoprotein E receptor 2 (ApoER2) variant ApoER2-R952Q. Little is known about the function of the apoE-ApoER2 tandem outside of the central nervous system. We now report that in endothelial cells apoE3 binding to ApoER2 stimulates endothelial NO synthase (eNOS) and endothelial cell migration, and it also attenuates monocyte-endothelial cell adhesion. However, apoE4 does not stimulate eNOS or endothelial cell migration or dampen cell adhesion, and alternatively it selectively antagonizes apoE3/ApoER2 actions. The contrasting endothelial actions of apoE4 vs. apoE3 require the N-terminal to C-terminal interaction in apoE4 that distinguishes it structurally from apoE3. Reconstitution experiments further reveal that ApoER2-R952Q is a loss-of-function variant of the receptor in endothelium. Carotid artery reendothelialization is decreased in ApoER2 −/− mice, and whereas adenoviraldriven apoE3 expression in wild-type mice has no effect, apoE4 impairs reendothelialization. Moreover, in a model of neointima formation invoked by carotid artery endothelial denudation, ApoER2 −/− mice display exaggerated neointima development. Thus, the apoE3/ ApoER2 tandem promotes endothelial NO production, endothelial repair, and endothelial anti-inflammatory properties, and it prevents neointima formation. In contrast, apoE4 and ApoER2-R952Q display dominant-negative action and loss of function, respectively. Thus, genetic variants of apoE and ApoER2 impact cardiovascular health by differentially modulating endothelial function.

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Section: Discussionmentioning

confidence: 99%

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confidence: 99%

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confidence: 99%

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Genetic variants of ApoE and ApoER2 differentially modulate endothelial function

Ulrich

Konaniah

Herz³

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

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“…Furthermore, a VLDLR deficiency increased intimal thickening after vascular injury and increased necrosis in atherosclerotic lesions (32). In addition, an apoER2 variant has been shown to increase the risk of atherosclerotic coronary artery disease (33). These observations imply that the pro-atherogenic effect of VLDLR (possibly apoER2) arising from the lipoprotein uptake function of macrophages may be counterbalanced by their anti-atherogenic effects, such as conversion of macrophages from a proinflammatory to an anti-inflammatory phenotype (31) and the inhibition of macrophage death in atherosclerotic lesions (32).…”

Section: Discussionmentioning

confidence: 99%

Up-regulation of ATP Binding Cassette Transporter A1 Expression by Very Low Density Lipoprotein Receptor and Apolipoprotein E Receptor 2

Chen

Guo

Okoro

et al. 2012

Journal of Biological Chemistry

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Background: VLDLR and apoER2 are receptors for reelin and apoE. Results: Reelin or apoE3 induced macrophage ABCA1 expression and increased cholesterol efflux. Down-regulation of VLDLR, apoER2, or inhibition of Dab1, PI3K, PKC and Sp1 attenuated reelin-or apoE3-induced ABCA1 expression. Conclusion: Activation of VLDLR-and apoER2-mediated signaling up-regulates ABCA1 expression. Significance: Up-regulation of ABCA1 expression is a novel function of VLDLR and apoER2.

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“…Our GeneQuest cohort with premature and familial CAD and MI has been previously described (Shen et al 2007c;Wang et al 2004). Briefly, over a five year span, patients were recruited by cardiologists and data coordinators in the Department of Cardiovascular Medicine at Cleveland Clinic and 10 other collaborating institutions.…”

Section: Ascertainment Of Patientsmentioning

confidence: 99%

Four SNPS on Chromosome 9p21 Confer Risk to Premature, Familial CAD and MI in an American Caucasian Population (GeneQuest)

Abdullah

Shen

et al. 2008

Annals of Human Genetics

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SummaryGenome-wide association studies have separately identified four single nucleotide polymorphisms (SNPs) on chromosome 9p21 that confer susceptibility to coronary artery disease (CAD) and myocardial infarction (MI). This study presents the first analysis of these SNPs (rs10757274, rs2383206, rs2383207, and rs10757278) in a premature, familial CAD/MI population (GeneQuest). We performed a case-control analysis of the GeneQuest Caucasian population with 310 cases with premature CAD and MI (average age at onset of 40.3 ± 5.1) and 560 non-CAD controls to determine if these SNPs are associated with risk of CAD using both the population-based and family-based association study designs. The four SNPs are significantly associated with premature and familial MI and CAD in the GeneQuest Caucasian population (allelic P = 6.61 × 10 −7 to 1.87 × 10 −8 ). Sib-TDT analysis showed that three of the four SNPs could confer significant susceptibility to premature CAD and MI. These results indicate that the four SNPs on chromosome 9p21 are also associated with premature, familial CAD.

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An LRP8 Variant Is Associated with Familial and Premature Coronary Artery Disease and Myocardial Infarction

Cited by 77 publications

References 30 publications

Genetic variants of ApoE and ApoER2 differentially modulate endothelial function

Genetic variants of ApoE and ApoER2 differentially modulate endothelial function

Up-regulation of ATP Binding Cassette Transporter A1 Expression by Very Low Density Lipoprotein Receptor and Apolipoprotein E Receptor 2

Four SNPS on Chromosome 9p21 Confer Risk to Premature, Familial CAD and MI in an American Caucasian Population (GeneQuest)

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