TY - JOUR
T1 - Polymorphic haplotypes of CRELD1 differentially predispose Down syndrome and euploids individuals to atrioventricular septal defect
AU - Ghosh, Priyanka
AU - Bhaumik, Pranami
AU - Ghosh, Sujoy
AU - Ozbek, Umut
AU - Feingold, Eleanor
AU - Maslen, Cheryl
AU - Sarkar, Biswanath
AU - Pramanik, Vishmadeb
AU - Biswas, Priyanka
AU - Bandyopadhyay, Biswajit
AU - Dey, Subrata Kumar
PY - 2012/11
Y1 - 2012/11
N2 - To explore the role of CRELD1 variants on congenital heart defects, we sequenced the entire reading frame of CRELD1 in the samples from Kolkata and adjoining areas. Nearly, 400 participants were included in the genetic association study and they were stratified as Down syndrome (DS) with atrioventricular septal defect (AVSD), DS without AVSD, euploid with AVSD, and euploid without AVSD. A significant association was found between AVSD and three polymorphisms, namely rs9878047 (c.1049-129T>C), rs3774207 (c.1119C>T), and rs73118372 (c.1136T>C) among the Down syndrome and euploid individuals. The polymorphism rs73118372, involves a transition (c.1136T>C) that leads to change in amino acid methionine to threonine which alters protein secondary structure as confirmed by the bioinformatics software SOPMA. In addition, two haplotypes, C-T-C and C-T-T, in the order of loci rs9878047-rs3774207-rs73118372 were associated with incidence of AVSD among euploid and Down syndrome, with a slightly higher odds ratio in the later group. We hypothesize that these haplotypes increase the risk of AVSD, and the susceptibility is exacerbated in DS, possibly due to the trisomy 21 genetic background. Moreover, we report for the first time on an interaction between the mutant alleles of rs3774207 and rs73118372 which could disrupt the delicate balance between different CRELD1 isoforms.
AB - To explore the role of CRELD1 variants on congenital heart defects, we sequenced the entire reading frame of CRELD1 in the samples from Kolkata and adjoining areas. Nearly, 400 participants were included in the genetic association study and they were stratified as Down syndrome (DS) with atrioventricular septal defect (AVSD), DS without AVSD, euploid with AVSD, and euploid without AVSD. A significant association was found between AVSD and three polymorphisms, namely rs9878047 (c.1049-129T>C), rs3774207 (c.1119C>T), and rs73118372 (c.1136T>C) among the Down syndrome and euploid individuals. The polymorphism rs73118372, involves a transition (c.1136T>C) that leads to change in amino acid methionine to threonine which alters protein secondary structure as confirmed by the bioinformatics software SOPMA. In addition, two haplotypes, C-T-C and C-T-T, in the order of loci rs9878047-rs3774207-rs73118372 were associated with incidence of AVSD among euploid and Down syndrome, with a slightly higher odds ratio in the later group. We hypothesize that these haplotypes increase the risk of AVSD, and the susceptibility is exacerbated in DS, possibly due to the trisomy 21 genetic background. Moreover, we report for the first time on an interaction between the mutant alleles of rs3774207 and rs73118372 which could disrupt the delicate balance between different CRELD1 isoforms.
KW - Atrioventricular septal defect
KW - CRELD1
KW - Down syndrome
KW - Single nucleotide polymorphism
KW - Splicing
UR - http://www.scopus.com/inward/record.url?scp=84867872114&partnerID=8YFLogxK
U2 - 10.1002/ajmg.a.35626
DO - 10.1002/ajmg.a.35626
M3 - Article
C2 - 22987595
AN - SCOPUS:84867872114
SN - 1552-4825
VL - 158 A
SP - 2843
EP - 2848
JO - American Journal of Medical Genetics, Part A
JF - American Journal of Medical Genetics, Part A
IS - 11
ER -