Article ID | Journal | Published Year | Pages | File Type |
---|---|---|---|---|
2779400 | Bone | 2012 | 9 Pages |
We performed a genetic association study of rare variants and single nucleotide polymorphisms (SNPs) of UCMA/GRP and OPTN genes, in French-Canadian patients with Paget's disease of bone (PDB) and in healthy controls from the same population. We reproduced the variant found in the UCMA/GRP basal promoter and tested its functionality using in vitro transient transfection assays. Interestingly, this SNP rs17152980 appears to affect the transcription level of UCMA/GRP. In addition, we have identified five rare genetic variants in UCMA/GRP gene, four of them being population-specific, although none were found to be associated with PDB. Six Tag SNPs of UCMA/GRP gene were associated with PDB, particularly the SNP rs17152980 (uncorrected P = 3.8 × 10− 3), although not significant after Bonferroni's correction. More importantly, we replicated the strong and statistically significant genetic association of two SNPs of the OPTN gene, the rs1561570 (uncorrected P = 5.7 × 10− 7) and the rs2095388 (uncorrected P = 4.9 × 10− 3), with PDB. In addition, we identified a very rare variant found to be located close to the basal promoter of the OPTN gene, at − 232 bp from its distal transcription start site. Furthermore, depending on the type of allele present (G or A), the binding of several important nuclear factors such as the vitamin D or the retinoic acid receptors is predicted to be altered at this position, suggesting a significant effect in the regulation of transcription of the OPTN gene. In conclusion, we identified a functional SNP located in the basal promoter of the UCMA/GRP gene which provided a weak genetic association with PDB. In addition, we replicated the strong genetic association of two already known SNPs of the OPTN gene, with PDB in a founder effect population. We also identified a very rare variant in the promoter of OPTN, and through bioinformatic analysis, identified putative transcription factor binding sites likely to affect OPTN gene transcription.
► A SNP of the basal promoter of UCMA/GRP gene, rs17152980, was weakly associated with Paget's disease of bone. ► This SNP is located in a binding site for the transcription factor Sox2. ► This SNP has a functional effect on the transcriptional activity of the UCMA/GRP gene. ► The association of two SNPs of the OPTN gene with PDB was replicated in a founder effect population. ► A very rare variant close to OPTN basal promoter was identified.