Abstract

A common amino acid polymorphism of methylenetetrahy-drofolate reductase is associated with hyperhomocysteinemia and predisposition to cardiovascular disease. It is hypothesized that mutations of other enzymes of homocysteine metabolism may have similar impact. The focus of this study will be on two enzyme systems of homocysteine remethylation. One is methionine synthase (MS) which requires two gene products: the MS apoenzyme (deficient in cblG disorder) and a reducing system associated with MS function (cbIE disorder). The second is betaine-homocysteine methyltransferase (BHMT). The investigators have cloned cDNAs for human MS and BHMT and identified mutations and a polymorphism of the MS apoenzyme.
Their specific aims are: 1) Identify amino acid polymorphisms in the MS (cblG, cbIE) and BHMT genes (cbIE to be cloned). This will be performed by SSCP analysis for the detection of mutations from RT-PCR or genomic DNA PCR products. 2) Clone the cbIE cDNA by functional complementation or homology-based RT-PCR (used successfully for the MS cbIG cDNA cloning). The complementation method will involve transformation of an E. coli methionine auxotroph, already expressing human MS, with a human cDNA library. Successful complementation will require the cblE gene product to permit growth in methionine-free medium. The homology method makes use of conserved sequences identified between flavodoxin/flavodoxin reductase of prokaryotes and eukaryotic flavoproteins to specify degenerate oligonucleotides for RT-PCR based cloning. 3) Express polymorphisms in human cell or E. coli expression systems to assess impact of mutations. Mutant fibroblasts will be the recipient for cDNA-mediated complementation assays. Expression of cDNAs in E. coli will permit biochemical analysis of purified protein. These studies will include introducing mutations into E. coli MS for analysis in conjunction with the flavodoxin system. 4) Examine impact of polymorphisms on homocysteine and nutrient levels. Identified polymorphisms will be screened in human subjects to determine if mutations are associated with abnormal homocysteine or nutrient (folate, B12) levels. Evaluate impact of polymorphisms on cardiovascular disease. Coronary artery disease patients will be evaluated for genotype status for polymorphisms shown to be associated with altered metabolities to determine if genotype frequencies vary from control groups. These studies, will determine the importance of genotype in the metabolic causes of hyperhomocysteinemia and risk of cardiovascular disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL058955-04
Application #
6043997
Study Section
Special Emphasis Panel (ZHL1-CSR-K (M1))
Project Start
1997-08-01
Project End
2001-07-31
Budget Start
2000-08-01
Budget End
2001-07-31
Support Year
4
Fiscal Year
2000
Total Cost
$175,000
Indirect Cost

  Institution

Name
University of Calgary
Department
Type
DUNS #
207663915
City
Calgary
State
AB
Country
Canada
Zip Code
T2 1-N4

  Publications

Padmanabhan, Nisha; Jia, Dongxin; Geary-Joo, Colleen et al. (2013) Mutation in folate metabolism causes epigenetic instability and transgenerational effects on development. Cell 155:81-93
Froese, D S; Wu, X; Zhang, J et al. (2008) Restricted role for methionine synthase reductase defined by subcellular localization. Mol Genet Metab 94:68-77
Elmore, C Lee; Wu, Xuchu; Leclerc, Daniel et al. (2007) Metabolic derangement of methionine and folate metabolism in mice deficient in methionine synthase reductase. Mol Genet Metab 91:85-97
Jacques, Paul F; Bostom, Andrew G; Selhub, Jacob et al. (2003) Effects of polymorphisms of methionine synthase and methionine synthase reductase on total plasma homocysteine in the NHLBI Family Heart Study. Atherosclerosis 166:49-55
Spotila, Loretta D; Jacques, Paul F; Berger, Peter B et al. (2003) Age dependence of the influence of methylenetetrahydrofolate reductase genotype on plasma homocysteine level. Am J Epidemiol 158:871-7
Weisberg, Ilan S; Park, Eric; Ballman, Karla V et al. (2003) Investigations of a common genetic variant in betaine-homocysteine methyltransferase (BHMT) in coronary artery disease. Atherosclerosis 167:205-14
Morin, Isabelle; Platt, Robert; Weisberg, Ilan et al. (2003) Common variant in betaine-homocysteine methyltransferase (BHMT) and risk for spina bifida. Am J Med Genet A 119A:172-6
Breksa 3rd, Andrew P; Garrow, Timothy A (2002) Random mutagenesis of the zinc-binding motif of betaine-homocysteine methyltransferase reveals that Gly 214 is essential. Arch Biochem Biophys 399:73-80
Hall, D A; Vander Kooi, C W; Stasik, C N et al. (2001) Mapping the interactions between flavodoxin and its physiological partners flavodoxin reductase and cobalamin-dependent methionine synthase. Proc Natl Acad Sci U S A 98:9521-6
Brown, C A; McKinney, K Q; Kaufman, J S et al. (2000) A common polymorphism in methionine synthase reductase increases risk of premature coronary artery disease. J Cardiovasc Risk 7:197-200

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