Neuropeptide Y gene polymorphisms confer risk of early-onset atherosclerosis.

dc.contributor.author

Shah, SH

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Freedman, NJ

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Zhang, L

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Crosslin, DR

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Stone, DH

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Haynes, C

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Johnson, J

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Nelson, S

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Wang, L

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Connelly, JJ

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Muehlbauer, M

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Ginsburg, GS

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Crossman, DC

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Jones, CJ

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Vance, J

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Sketch, MH

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Granger, CB

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Newgard, CB

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Gregory, SG

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Goldschmidt Clermont, PJ

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Kraus, WE

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Hauser, ER

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Cox, Gregory A

dc.coverage.spatial

United States

dc.date.accessioned

2018-02-01T19:38:51Z

dc.date.available

2018-02-01T19:38:51Z

dc.date.issued

2009-01

dc.description.abstract

Neuropeptide Y (NPY) is a strong candidate gene for coronary artery disease (CAD). We have previously identified genetic linkage to familial CAD in the genomic region of NPY. We performed follow-up genetic, biostatistical, and functional analysis of NPY in early-onset CAD. In familial CAD (GENECARD, N = 420 families), we found increased microsatellite linkage to chromosome 7p14 (OSA LOD = 4.2, p = 0.004) in 97 earliest age-of-onset families. Tagged NPY SNPs demonstrated linkage to CAD of a 6-SNP block (LOD = 1.58-2.72), family-based association of this block with CAD (p = 0.02), and stronger linkage to CAD in the earliest age-of-onset families. Association of this 6-SNP block with CAD was validated in: (a) 556 non-familial early-onset CAD cases and 256 controls (OR 1.46-1.65, p = 0.01-0.05), showing stronger association in youngest cases (OR 1.84-2.20, p = 0.0004-0.09); and (b) GENECARD probands versus non-familial controls (OR 1.79-2.06, p = 0.003-0.02). A promoter SNP (rs16147) within this 6-SNP block was associated with higher plasma NPY levels (p = 0.04). To assess a causal role of NPY in atherosclerosis, we applied the NPY1-receptor-antagonist BIBP-3226 adventitially to endothelium-denuded carotid arteries of apolipoprotein E-deficient mice; treatment reduced atherosclerotic neointimal area by 50% (p = 0.03). Thus, NPY variants associate with atherosclerosis in two independent datasets (with strong age-of-onset effects) and show allele-specific expression with NPY levels, while NPY receptor antagonism reduces atherosclerosis in mice. We conclude that NPY contributes to atherosclerosis pathogenesis.

dc.identifier

https://www.ncbi.nlm.nih.gov/pubmed/19119412

dc.identifier.eissn

1553-7404

dc.identifier.uri

https://hdl.handle.net/10161/16064

dc.language

eng

dc.publisher

Public Library of Science (PLoS)

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PLoS Genet

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10.1371/journal.pgen.1000318

dc.subject

Age of Onset

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Alleles

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Animals

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Arginine

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Atherosclerosis

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Female

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Genetic Predisposition to Disease

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Genotype

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Humans

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Linkage Disequilibrium

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Lod Score

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Male

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Mice

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Mice, Transgenic

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Middle Aged

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Neuropeptide Y

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Polymorphism, Genetic

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Receptors, Neuropeptide Y

dc.title

Neuropeptide Y gene polymorphisms confer risk of early-onset atherosclerosis.

dc.type

Journal article

duke.contributor.orcid

Shah, SH|0000-0002-3495-2830

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Freedman, NJ|0000-0002-8593-8676

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Ginsburg, GS|0000-0003-4739-9808

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Granger, CB|0000-0002-0045-3291

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Gregory, SG|0000-0002-7805-1743

duke.contributor.orcid

Kraus, WE|0000-0003-1930-9684

duke.contributor.orcid

Hauser, ER|0000-0003-0367-9189

pubs.author-url

https://www.ncbi.nlm.nih.gov/pubmed/19119412

pubs.begin-page

e1000318

pubs.issue

1

pubs.organisational-group

Basic Science Departments

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Biochemistry

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Biostatistics & Bioinformatics

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Cell Biology

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Clinical Science Departments

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Duke

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Duke Cancer Institute

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Duke Clinical Research Institute

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Duke Global Health Institute

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Duke Molecular Physiology Institute

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Institutes and Centers

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Institutes and Provost's Academic Units

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Medicine

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Medicine, Cardiology

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Medicine, Endocrinology, Metabolism, and Nutrition

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Molecular Genetics and Microbiology

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Neurology

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Neurology, MS & Neuroimmunology

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Nursing

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Pathology

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Pharmacology & Cancer Biology

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School of Medicine

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School of Nursing

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University Institutes and Centers

pubs.publication-status

Published

pubs.volume

5

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