Abstract
An increasing number of genetic variants involved in dyslexia development were discovered during the last years, yet little is known about the molecular functional mechanisms of these SNPs. In this study we investigated whether dyslexia candidate SNPs have a direct, disease-specific effect on local expression levels of the assumed target gene by using a differential allelic expression assay. In total, 12 SNPs previously associated with dyslexia and related phenotypes were suitable for analysis. Transcripts corresponding to four SNPs were sufficiently expressed in 28 cell lines originating from controls and a family affected by dyslexia. We observed a significant effect of rs600753 on expression levels of DYX1C1 in forward and reverse sequencing approaches. The expression level of the rs600753 risk allele was increased in the respective seven cell lines from members of the dyslexia family which might be due to a disturbed transcription factor binding sites. When considering our results in the context of neuroanatomical dyslexia-specific findings, we speculate that this mechanism may be part of the pathomechanisms underlying the dyslexia-specific brain phenotype. Our results suggest that allele-specific DYX1C1 expression levels depend on genetic variants of rs600753 and contribute to dyslexia. However, these results are preliminary and need replication.
| Original language | English |
|---|---|
| Journal | Genetics and Molecular Biology |
| Volume | 41 |
| Issue number | 1 |
| Pages (from-to) | 41-49 |
| Number of pages | 9 |
| ISSN | 1415-4757 |
| DOIs | |
| Publication status | Published - 01.01.2018 |
Funding
We would like to thank all members of the Legas-creen consortium for their support during this study. The consortium consists of: Prof. Dr. Dr. h.c. Angela D. Frie-derici, Prof. Dr. Frank Emmrich, Dr. Jens Brauer, Dr. Arndt Wilcke, Dr. Nicole Neef, Prof. Dr. Dr. Johannes Boltze, Dr. Michael Skeide, Dr. Holger Kirsten, Dr. Gesa Schaadt, Dr. Bent Müller, Dr. Indra Kraft, Ivonne Czepezauer, and Liane Dörr. The Legascreen Project is funded by the Fraun-hofer Society and the Max-Planck-Society as a project within the framework of the “Pakt für Forschung und Innovation”. The authors are grateful to Prof. Dr. Svante Pääbo, Birgit Nickel and Prof. Dr. Frank Albert for providing material and expert support regarding cell culture experiments.
Research Areas and Centers
- Academic Focus: Biomedical Engineering
