Crossref journal-article
Springer Science and Business Media LLC
BMC Medical Genetics (297)
Abstract

Abstract Background Schizophrenia is a highly heritable complex psychiatric disorder with an underlying pathophysiology that is still not well understood. Metaanalyses of schizophrenia linkage studies indicate numerous but rather large disease-associated genomic regions, whereas accumulating gene- and protein expression studies have indicated an equally large set of candidate genes that only partially overlap linkage genes. A thorough assessment, beyond the resolution of current GWA studies, of the disease risk conferred by the numerous schizophrenia candidate genes is a daunting and presently not feasible task. We undertook these challenges by using an established clinical paradigm, the estrogen hypothesis of schizophrenia, as the criterion to select candidates among the numerous genes experimentally implicated in schizophrenia. Bioinformatic tools were used to build and priorities the signaling networks implicated by the candidate genes resulting from the estrogen selection. We identified ten candidate genes using this approach that are all active in glucose metabolism and particularly in the glycolysis. Thus, we tested the hypothesis that variants of the glycolytic genes are associated with schizophrenia or at least with gender-associated aspects of the illness. Results We genotyped 185 SNPs in three independent case-control samples of Scandinavian origin (a total of 765 patients and 1274 control subjects). Variants of the mitogen-activated protein kinase 14 gene (MAPK14) and the phosphoenolpyruvate carboxykinase 1 (PCK1) and fructose-1,6-biphosphatase (FBP1) were nominal significantly associated with schizophrenia, and several haplotypes within enolase 2 gene (ENO2) consist of the same SNP allele having elevated risk of schizophrenia. Importantly, we find no evidence of stratification due to nationality or gender. Conclusion Several gene variants in the Glycolysis were associated with schizophrenia in three independent samples. However, the findings are weak and not resistant to correction for multiple testing, which may indicate that they are either spurious or may relate to a particular subtype or aspect of the illness.

Bibliography

Olsen, L., Hansen, T., Jakobsen, K. D., Djurovic, S., Melle, I., Agartz, I., Hall, H., Ullum, H., Timm, S., Wang, A. G., Jönsson, E. G., Andreassen, O. A., & Werge, T. (2008). The estrogen hypothesis of Schizophrenia implicates glucose metabolism: Association study in three independent samples. BMC Medical Genetics, 9(1).

Authors 13
  1. Line Olsen (first)
  2. Thomas Hansen (additional)
  3. Klaus D Jakobsen (additional)
  4. Srdjan Djurovic (additional)
  5. Ingrid Melle (additional)
  6. Ingrid Agartz (additional)
  7. Haakan Hall (additional)
  8. Henrik Ullum (additional)
  9. Sally Timm (additional)
  10. August G Wang (additional)
  11. Erik G Jönsson (additional)
  12. Ole A Andreassen (additional)
  13. Thomas Werge (additional)
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Dates
Type When
Created 17 years, 3 months ago (May 21, 2008, 3:51 p.m.)
Deposited 4 years ago (Sept. 1, 2021, 6:52 a.m.)
Indexed 9 months, 2 weeks ago (Nov. 19, 2024, 11:12 a.m.)
Issued 17 years, 4 months ago (May 6, 2008)
Published 17 years, 4 months ago (May 6, 2008)
Published Online 17 years, 4 months ago (May 6, 2008)
Published Print 16 years, 9 months ago (Dec. 1, 2008)
Funders 0

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@article{Olsen_2008, title={The estrogen hypothesis of Schizophrenia implicates glucose metabolism: Association study in three independent samples}, volume={9}, ISSN={1471-2350}, url={http://dx.doi.org/10.1186/1471-2350-9-39}, DOI={10.1186/1471-2350-9-39}, number={1}, journal={BMC Medical Genetics}, publisher={Springer Science and Business Media LLC}, author={Olsen, Line and Hansen, Thomas and Jakobsen, Klaus D and Djurovic, Srdjan and Melle, Ingrid and Agartz, Ingrid and Hall, Haakan and Ullum, Henrik and Timm, Sally and Wang, August G and Jönsson, Erik G and Andreassen, Ole A and Werge, Thomas}, year={2008}, month=may }