Publikation: Genome-Wide Association-, Replication-, and Neuroimaging Study Implicates HOMER1 in the Etiology of Major Depression
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Zusammenfassung
Background:
Genome-wide association studies are a powerful tool for unravelling the genetic background of complex disorders such as major depression.
Methods:
We conducted a genome-wide association study of 604 patients with major depression and 1364 population based control subjects. The top hundred findings were followed up in a replication sample of 409 patients and 541 control subjects.
Results:
Two SNPs showed nominally significant association in both the genome-wide association study and the replication samples: 1) rs9943849 (pcombined = 3.24E-6) located upstream of the carboxypeptidase M (CPM) gene and 2) rs7713917 (pcombined = 1.48E-6), located in a putative regulatory region of HOMER1. Further evidence for HOMER1 was obtained through gene-wide analysis while conditioning on the genotypes of rs7713917 (pcombined = 4.12E-3). Homer1 knockout mice display behavioral traits that are paradigmatic of depression, and transcriptional variants of Homer1 result in the dysregulation of cortical-limbic circuitry. This is consistent with the findings of our subsequent human imaging genetics study, which revealed that variation in single nucleotide polymorphism rs7713917 had a significant influence on prefrontal activity during executive cognition and anticipation of reward.
Conclusion:
Our findings, combined with evidence from preclinical and animal studies, suggest that HOMER1 plays a role in the etiology of major depression and that the genetic variation affects depression via the dysregulation of cognitive and motivational processes.
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RIETSCHEL, Marcella, Manuel MATTHEISEN, Josef FRANK, Jens TREUTLEIN, Franziska DEGENHARDT, René BREUER, Michael STEFFENS, Daniela MIER, Christine ESSLINGER, Henrik WALTER, 2010. Genome-Wide Association-, Replication-, and Neuroimaging Study Implicates HOMER1 in the Etiology of Major Depression. In: Biological Psychiatry. 2010, 68(6), pp. 578-585. ISSN 0006-3223. eISSN 1873-2402. Available under: doi: 10.1016/j.biopsych.2010.05.038BibTex
@article{Rietschel2010-09-15Genom-45696,
year={2010},
doi={10.1016/j.biopsych.2010.05.038},
title={Genome-Wide Association-, Replication-, and Neuroimaging Study Implicates HOMER1 in the Etiology of Major Depression},
number={6},
volume={68},
issn={0006-3223},
journal={Biological Psychiatry},
pages={578--585},
author={Rietschel, Marcella and Mattheisen, Manuel and Frank, Josef and Treutlein, Jens and Degenhardt, Franziska and Breuer, René and Steffens, Michael and Mier, Daniela and Esslinger, Christine and Walter, Henrik}
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<dcterms:abstract xml:lang="eng">Background:<br />Genome-wide association studies are a powerful tool for unravelling the genetic background of complex disorders such as major depression.<br /><br />Methods:<br />We conducted a genome-wide association study of 604 patients with major depression and 1364 population based control subjects. The top hundred findings were followed up in a replication sample of 409 patients and 541 control subjects.<br /><br />Results:<br />Two SNPs showed nominally significant association in both the genome-wide association study and the replication samples: 1) rs9943849 (p<sub>combined</sub> = 3.24E-6) located upstream of the carboxypeptidase M (CPM) gene and 2) rs7713917 (p<sub>combined</sub> = 1.48E-6), located in a putative regulatory region of HOMER1. Further evidence for HOMER1 was obtained through gene-wide analysis while conditioning on the genotypes of rs7713917 (p<sub>combined</sub> = 4.12E-3). Homer1 knockout mice display behavioral traits that are paradigmatic of depression, and transcriptional variants of Homer1 result in the dysregulation of cortical-limbic circuitry. This is consistent with the findings of our subsequent human imaging genetics study, which revealed that variation in single nucleotide polymorphism rs7713917 had a significant influence on prefrontal activity during executive cognition and anticipation of reward.<br /><br />Conclusion:<br />Our findings, combined with evidence from preclinical and animal studies, suggest that HOMER1 plays a role in the etiology of major depression and that the genetic variation affects depression via the dysregulation of cognitive and motivational processes.</dcterms:abstract>
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