OBJECTIVES: Bipolar disorder is a severe mood disorder, which normally begins during adolescence or early adulthood and has a heritability of up to 80%. The largest genome-wide association analysis of bipolar disorder recently identified a new genome-wide associated variant in OZD4 (rs12576775). The aim of the present study was to further elucidate the role of this risk variant in the disease process using an imaging genetics approach. As increased amygdala and striatal responses during the processing of reward and emotion are characteristic for bipolar disorder patients, it was tested whether the risk variant has an influence on this endophenotype in healthy adolescents. METHODS: We examined the impact of the risk variant rs12576775 on functional magnetic resonance imaging data in an adolescent sample (N = 485). Differential activation between carriers of the risk allele (G-allele) and homozygous A-allele carriers in the amygdala and the striatum during a modification of the monetary incentive delay task (examining reward) and a face task (examining emotion) was analyzed. RESULTS: Carriers of the risk allele showed an increased blood oxygen level-dependent response in the amygdala during reward sensitivity (p = 0.05) and reward expectation (p < 0.05) but not during the face task. No significant group differences were found in the striatum during both reward and emotion processing. CONCLUSION: Our results indicate that the ODZ4 risk variant influences reward processing in the amygdala. Alterations in the processing of emotion may have different underlying mechanisms and need to be further examined.
OBJECTIVES:Bipolar disorder is a severe mood disorder, which normally begins during adolescence or early adulthood and has a heritability of up to 80%. The largest genome-wide association analysis of bipolar disorder recently identified a new genome-wide associated variant in OZD4 (rs12576775). The aim of the present study was to further elucidate the role of this risk variant in the disease process using an imaging genetics approach. As increased amygdala and striatal responses during the processing of reward and emotion are characteristic for bipolar disorderpatients, it was tested whether the risk variant has an influence on this endophenotype in healthy adolescents. METHODS: We examined the impact of the risk variant rs12576775 on functional magnetic resonance imaging data in an adolescent sample (N = 485). Differential activation between carriers of the risk allele (G-allele) and homozygous A-allele carriers in the amygdala and the striatum during a modification of the monetary incentive delay task (examining reward) and a face task (examining emotion) was analyzed. RESULTS: Carriers of the risk allele showed an increased blood oxygen level-dependent response in the amygdala during reward sensitivity (p = 0.05) and reward expectation (p < 0.05) but not during the face task. No significant group differences were found in the striatum during both reward and emotion processing. CONCLUSION: Our results indicate that the ODZ4 risk variant influences reward processing in the amygdala. Alterations in the processing of emotion may have different underlying mechanisms and need to be further examined.
Authors: Stéphane Jamain; Sven Cichon; Bruno Etain; Thomas W Mühleisen; Alexander Georgi; Nora Zidane; Lucie Chevallier; Jasmine Deshommes; Aude Nicolas; Annabelle Henrion; Franziska Degenhardt; Manuel Mattheisen; Lutz Priebe; Flavie Mathieu; Jean-Pierre Kahn; Chantal Henry; Anne Boland; Diana Zelenika; Ivo Gut; Simon Heath; Mark Lathrop; Wolfgang Maier; Margot Albus; Marcella Rietschel; Thomas G Schulze; Francis J McMahon; John R Kelsoe; Marian Hamshere; Nicholas Craddock; Markus M Nöthen; Frank Bellivier; Marion Leboyer Journal: PLoS One Date: 2014-08-11 Impact factor: 3.240
Authors: Martin Tesli; Karolina Kauppi; Francesco Bettella; Christine Lycke Brandt; Tobias Kaufmann; Thomas Espeseth; Morten Mattingsdal; Ingrid Agartz; Ingrid Melle; Srdjan Djurovic; Lars T Westlye; Ole A Andreassen Journal: PLoS One Date: 2015-07-29 Impact factor: 3.240