Complex analysis of multiple single nucleotide polymorphisms as putative risk factors of tooth agenesis in the Hungarian population.

[oligodontia]

The role was studied of multiple single nucleotide polymorphisms in tooth agenesis in the Hungarian population using a complex approach .Eight SNPs , PAX 9 -912 C /T , PAX 9 -1031 A /G , MSX 1 3755 A /G , FGFR 1 T /C rs 881301 , IRF 6 T /C rs 764093 , AXIN 2 -8150 A /G , AXIN 2 -8434 A /G and AXIN 2 -30224 C /T , were studied in 192 hypodontia and 17 oligodontia cases and in 260 healthy volunteers . Case-control analysis was performed to test both allelic and genotypic associations as well as associations at the level of haplotypes . Multivariate exploratory Bayesian network-based multi-level analysis of relevance (BN-BMLA ) as well as logistic regression analysis were performed .Conventional statistics showed that PAX 9 SNP -912 C /T and the MSX 1 SNP changed the incidence of hypodontia , although after Bonferroni correction for multiple hypothesis testing , the effects were only borderline tendencies . Using a statistical analysis better suited for handling multiple hypotheses , the BN-BMLA , PAX 9 SNPs clearly showed a synergistic effect . This was confirmed by other multivariate analyses and it remained significant after corrections for multiple hypothesis testing (p < 0 .0025 ). The PAX 9 -1031 -A-PAX 9 -912 -T haplotype was the most relevant combination causing hypodontia . Interaction was weaker between PAX 9 and MSX 1 , while other SNPs had no joint effect on hypodontia .This complex analysis shows the important role of PAX 9 and MSX 1 SNPs and of their interactions in tooth agenesis , while IRF 6 , FGFR 1 and AXIN 2 SNPs had no detectable role in the Hungarian population . These results also reveal that risk factors in hypodontia need to be identified in various populations , since there is considerable variability among them .