Association of COMT genotypes with S-COMT promoter methylation in growth-discordant monozygotic twins and healthy adults

Association of COMT genotypes with S-COMT promoter methylation in growth-discordant monozygotic twins and healthy adults

<p>Abstract</p> <p>Background</p> <p>Catechol-O-Methyltransferase (COMT) plays a key role in dopamine and estrogen metabolism. Recently, COMT haplotypes rather than the single polymorphism Val158Met have been reported to underlie differences in protein expression by mod...

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Main Authors: Schreiner Felix, El-Maarri Osman, Gohlke Bettina, Stutte Sonja, Nuesgen Nicole, Mattheisen Manuel, Fimmers Rolf, Bartmann Peter, Oldenburg Johannes, Woelfle Joachim
Format: Article
Language:English
Published: BMC 2011-09-01
Series:BMC Medical Genetics
Online Access:http://www.biomedcentral.com/1471-2350/12/115
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spelling doaj-53f3ea9e1a614b69813a83ebc94625bc2021-04-02T11:08:38ZengBMCBMC Medical Genetics1471-23502011-09-0112111510.1186/1471-2350-12-115Association of COMT genotypes with S-COMT promoter methylation in growth-discordant monozygotic twins and healthy adultsSchreiner FelixEl-Maarri OsmanGohlke BettinaStutte SonjaNuesgen NicoleMattheisen ManuelFimmers RolfBartmann PeterOldenburg JohannesWoelfle Joachim<p>Abstract</p> <p>Background</p> <p>Catechol-O-Methyltransferase (COMT) plays a key role in dopamine and estrogen metabolism. Recently, COMT haplotypes rather than the single polymorphism Val158Met have been reported to underlie differences in protein expression by modulating mRNA secondary structure. So far, studies investigating the epigenetic variability of the S-COMT (soluble COMT) promoter region mainly focused on phenotypical aspects, and results have been controversial.</p> <p>Methods</p> <p>We assessed S-COMT promoter methylation in saliva and blood derived DNA with regard to early pre- and postnatal growth as well as to genotype for polymorphisms rs6269, rs4633, and rs4680 (Val158Met) in 20 monozygotic twin pairs (mean age 4 years), who were discordant for intrauterine development due to severe feto-fetal-transfusion syndrome. Methylation levels of two previously reported partially methylated cytosines were determined by the quantitative SIRPH (SNuPE- IP RP HPLC) assay.</p> <p>Results</p> <p>Overall, we observed a high variability of S-COMT promoter methylation, which did not correlate with individual differences in the pre- or postnatal growth pattern. Within the twin pairs however we noted a distinct similarity that could be linked to underlying COMT genotypes. This association was subsequently confirmed in a cohort of 93 unrelated adult controls. Interestingly, 158Val-alleles were found at both ends of the epigenotypical range, which is in accordance with a recently proposed model of COMT haplotypes corresponding to a continuum of phenotypical variability.</p> <p>Conclusion</p> <p>The strong heritable component of S-COMT promoter methylation found in our study needs to be considered in future approaches that focus on interactions between COMT epigenotype and phenotype.</p> http://www.biomedcentral.com/1471-2350/12/115
collection DOAJ
language English
format Article
sources DOAJ
author Schreiner Felix
El-Maarri Osman
Gohlke Bettina
Stutte Sonja
Nuesgen Nicole
Mattheisen Manuel
Fimmers Rolf
Bartmann Peter
Oldenburg Johannes
Woelfle Joachim
spellingShingle Schreiner Felix
El-Maarri Osman
Gohlke Bettina
Stutte Sonja
Nuesgen Nicole
Mattheisen Manuel
Fimmers Rolf
Bartmann Peter
Oldenburg Johannes
Woelfle Joachim
Association of COMT genotypes with S-COMT promoter methylation in growth-discordant monozygotic twins and healthy adults
BMC Medical Genetics
author_facet Schreiner Felix
El-Maarri Osman
Gohlke Bettina
Stutte Sonja
Nuesgen Nicole
Mattheisen Manuel
Fimmers Rolf
Bartmann Peter
Oldenburg Johannes
Woelfle Joachim
author_sort Schreiner Felix
title Association of COMT genotypes with S-COMT promoter methylation in growth-discordant monozygotic twins and healthy adults
title_short Association of COMT genotypes with S-COMT promoter methylation in growth-discordant monozygotic twins and healthy adults
title_full Association of COMT genotypes with S-COMT promoter methylation in growth-discordant monozygotic twins and healthy adults
title_fullStr Association of COMT genotypes with S-COMT promoter methylation in growth-discordant monozygotic twins and healthy adults
title_full_unstemmed Association of COMT genotypes with S-COMT promoter methylation in growth-discordant monozygotic twins and healthy adults
title_sort association of comt genotypes with s-comt promoter methylation in growth-discordant monozygotic twins and healthy adults
publisher BMC
series BMC Medical Genetics
issn 1471-2350
publishDate 2011-09-01
description <p>Abstract</p> <p>Background</p> <p>Catechol-O-Methyltransferase (COMT) plays a key role in dopamine and estrogen metabolism. Recently, COMT haplotypes rather than the single polymorphism Val158Met have been reported to underlie differences in protein expression by modulating mRNA secondary structure. So far, studies investigating the epigenetic variability of the S-COMT (soluble COMT) promoter region mainly focused on phenotypical aspects, and results have been controversial.</p> <p>Methods</p> <p>We assessed S-COMT promoter methylation in saliva and blood derived DNA with regard to early pre- and postnatal growth as well as to genotype for polymorphisms rs6269, rs4633, and rs4680 (Val158Met) in 20 monozygotic twin pairs (mean age 4 years), who were discordant for intrauterine development due to severe feto-fetal-transfusion syndrome. Methylation levels of two previously reported partially methylated cytosines were determined by the quantitative SIRPH (SNuPE- IP RP HPLC) assay.</p> <p>Results</p> <p>Overall, we observed a high variability of S-COMT promoter methylation, which did not correlate with individual differences in the pre- or postnatal growth pattern. Within the twin pairs however we noted a distinct similarity that could be linked to underlying COMT genotypes. This association was subsequently confirmed in a cohort of 93 unrelated adult controls. Interestingly, 158Val-alleles were found at both ends of the epigenotypical range, which is in accordance with a recently proposed model of COMT haplotypes corresponding to a continuum of phenotypical variability.</p> <p>Conclusion</p> <p>The strong heritable component of S-COMT promoter methylation found in our study needs to be considered in future approaches that focus on interactions between COMT epigenotype and phenotype.</p>
url http://www.biomedcentral.com/1471-2350/12/115
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