Abstract

The most important cause of death and disability in the Western world is atherosclerotic coronary artery disease (CAD) and its primary complication-acute myocardial infarction (MI). The long-term objective of this project is to define genetic pathways and molecular mechanisms for CAD and MI. The central hypothesis of this proposal is that the pathogenesis of CAD/MI involves functional mutations in key genes that perturb the complex molecular processes involved in CAD/MI. To this end, recently, in a large pedigree with autosomal dominant CAD/MI, we identified a specific MEF2A mutation (21-bp deletion) that appears to be responsible for this family's CAD/MI (Science, in press). Furthermore, we have completed a genomewide scan for susceptibility genes for CAD/MI in a well characterized U.S. cohort consisting of 1,163 affected persons in 428 multiplex families with premature CAD and MI (average age at onset: 44.4 + 9.7 years). Of eight novel significant susceptibility loci detected for MI linkage to the chromosomal region lp34-36 showed multipoint allelesharing P values of <10 -12 (LOD = 11.68). The present proposal is driven by these exciting results.
The specific aims are:
Specific Aim 1 : To map and identify a novel CAD/MI gene using single large families and model-based linkage analysis, and positional cloning. First, we will continue to validate our finding that mutations in MEF2A cause familial CAD/MI by characterizing the MEF2A knockout mice and transgenic mice for phenotype related to CAD/MI. A series of molecular and cell biological experiments are designed to explore the molecular mechanisms of the MEF2A deletion. We will also identify SNPs in MEF2A and determine whether some of the SNPs increase or decrease the risk of common complex CAD/MI by association studies. Secondly, we plan to continue to use model-based linkage analysis and positional cloning to map and identify at least one new CAD/MI gene. We have recruited three large and extended CAD/MI pedigrees that are not linked toMEF2A, and each family has statistically sufficient power (simulated LOD scores of 3.53, 7.22, and 6.62, respectively) to conduct a genomewide scan of significant linkage to CAD and MI. Furthermore, 16 families of more than four affected individuals have been identified with an average of 27 living siblings and parents per family for this study.
Specific Aim 2 : To identify the susceptibility gene for MI on the chromosomal region lp34-36, We will focus on the chromosome lp34-36 MI locus for our follow-up gene discovery effort because this is the most significant linkage identified for MI to date (LOD score of 11.68). We will perform fine mapping, identification of candidate genes, SNP identification and genotyping_ family-TDT analysis (Sibship Disequilibrium Test) as well as population-based case-control studies to determine whether a specific SNP or SNP haplotype in a candidate gene is associated with MI. The accomplishment of research objectives in this proposal has the potential to have a substantial impact on the understanding of the molecular mechanism of CAD and MI, thereby facilitating better prevention, diagnosis and therapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
1R01HL073817-01A1
Application #
6826599
Study Section
Clinical and Integrative Cardiovascular Sciences Study Section (CICS)
Program Officer
Bookman, Ebony B
Project Start
2004-08-01
Project End
2004-12-31
Budget Start
2004-08-01
Budget End
2004-12-31
Support Year
1
Fiscal Year
2004
Total Cost
$189,186
Indirect Cost

  Institution

Name
Cleveland Clinic Lerner
Department
Other Basic Sciences
Type
Schools of Medicine
DUNS #
135781701
City
Cleveland
State
OH
Country
United States
Zip Code
44195

  Publications

Shen, Gong-Qing; Girelli, Domenico; Li, Lin et al. (2013) Multi-allelic haplotype association identifies novel information different from single-SNP analysis: a new protective haplotype in the LRP8 gene is against familial and early-onset CAD and MI. Gene 521:78-81
Yang, Qinbo; Li, Lin; Chen, Qiuyun et al. (2011) Association studies of variants in MEIS1, BTBD9, and MAP2K5/SKOR1 with restless legs syndrome in a US population. Sleep Med 12:800-4
Wang, Annabel Z; Li, Lin; Zhang, Bin et al. (2011) Association of SNP rs17465637 on chromosome 1q41 and rs599839 on 1p13.3 with myocardial infarction in an American caucasian population. Ann Hum Genet 75:475-82
Liu, Jing Yu; Dai, Xiaohua; Sheng, Jiqun et al. (2008) Identification and functional characterization of a novel splicing mutation in RP gene PRPF31. Biochem Biophys Res Commun 367:420-6
Shen, Gong-Qing; Li, Lin; Girelli, Domenico et al. (2007) An LRP8 variant is associated with familial and premature coronary artery disease and myocardial infarction. Am J Hum Genet 81:780-91
Melamud, A; Shen, G-Q; Chung, D et al. (2006) Mapping a new genetic locus for X linked retinitis pigmentosa to Xq28. J Med Genet 43:e27
Wang, Qing (2005) Molecular genetics of coronary artery disease. Curr Opin Cardiol 20:182-8
Timur, A A; Driscoll, D J; Wang, Q (2005) Biomedicine and diseases: the Klippel-Trenaunay syndrome, vascular anomalies and vascular morphogenesis. Cell Mol Life Sci 62:1434-47
You, Sun-Ah; Wang, Qing (2005) Ferritin in atherosclerosis. Clin Chim Acta 357:1-16
Wang, Qing (2005) Advances in the genetic basis of coronary artery disease. Curr Atheroscler Rep 7:235-41

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