Genetic Screening of WNT4 and WNT5B in Two Populations with Deviating Bone Mineral Densities
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- 作者:Gretl Hendrickx ; Eveline Boudin ; Ellen Steenackers…
- 关键词:WNT4 ; WNT5B ; Genetics ; Bone mineral density ; Osteoporosis
- 刊名:Calcified Tissue International
- 出版年:2017
- 出版时间:March 2017
- 年:2017
- 卷:100
- 期:3
- 页码:244-249
- 全文大小:
- 刊物类别:Biomedical and Life Sciences
- 刊物主题:Biochemistry, general; Endocrinology; Orthopedics; Cell Biology;
- 出版者:Springer US
- ISSN:1432-0827
- 卷排序:100
文摘
A role for WNT4 and WNT5B in bone metabolism was indicated by genome-wide association studies (GWAS) and a Wnt4 knockout mouse model. The aim of this study was therefore to replicate and further investigate the causality between genetic variation in WNT4 and WNT5B and deviating bone mineral density (BMD) values. A WNT4 and WNT5B mutation screening was performed in patients with craniotubular hyperostosis using Sanger sequencing. Here, no putative causal mutations were detected. Moreover, a high and low BMD cohort was selected from the Odense Androgen Study population for re-sequencing. In WNT4 we detected four variants (three rare, one common), while in WNT5B we detected five variants (two rare, three common). For the common variants, no significant difference in genotype frequencies between the high and low BMD cohorts was observed. The SNPs associated with the GWAS were genotyped in these cohorts, but again no significant difference in genotype frequencies was observed. Despite the findings of the GWAS, we were not able to replicate or further verify the genetic association of polymorphisms in WNT4 and WNT5B with BMD. In order to do so, the intronic regions of both genes could be investigated more thoroughly in more extended populations (or extremes) with greater power. Future genetic and functional studies toward adjacent genes of WNT4 and WNT5B can also be interesting to figure out whether the signal from GWAS could possibly be attributed to genetic variation in these genes.