RALDH2 genetic variants and congenital heart disease.

The aim of the study was to investigate the role of genetic variation in the RALDH2 locus and congenital heart disease. Six different SNPs were analyzed in 101 patient-parents trios in a TDT study. None of the markers displayed any association with CHD. No single haplotype was associated with an increased risk of CHD. Analysis of the A151G polymorphism indicated that the variant produced substantial changes in mRNA structure. This variant is also localized in a putative exonic splicing enhancer (ESE). Functional splicing studies failed to reveal a significant impact of this variant and gene splicing. This methodology was applied to another mutation (G151T) found in exon 4 during the sequencing of RALDH2 gene and an increase in splicing signal was observed. We found four mutations more: rs34645259, T157G (exon 4), rs4646626 and rs35251510. In summary, no association between CHD and genetic variation at the RALDH2 locus in humans was found. Potential functional genetic variants should be further studied in order to define their real role in RA pathway disturbances. (AU)