| Literature DB >> 20826553 |
Robert Keers1, Cristian Bonvicini, Catia Scassellati, Rudolf Uher, Anna Placentino, Caterina Giovannini, Marcella Rietschel, Neven Henigsberg, Dejan Kozel, Ole Mors, Wolfgang Maier, Joanna Hauser, Daniel Souery, Julien Mendlewicz, Christine Schmäl, Astrid Zobel, Erik R Larsen, Aleksandra Szczepankiewicz, Zrnka Kovacic, Amanda Elkin, Ian Craig, Peter McGuffin, Anne E Farmer, Katherine J Aitchison, Massimo Gennarelli.
Abstract
There is substantial inter-individual variation in response and adverse reactions to antidepressants, and genetic variation may, in part, explain these differences. GNB3 encodes the β3 subunit of the G protein complex, which is involved in the downstream signalling cascade following monoamine receptor activation. A functional polymorphism in this gene (C825T) has been associated with response to antidepressants. Several lines of evidence suggest that GNB3 moderates improvement in the neurovegetative symptoms of depression (such as sleep and appetite) and related adverse reactions independently of change in core mood symptoms. We here report analysis of data from GENDEP, a part-randomized pharmacogenomic trial, on the outcome of 811 subjects with major depression undergoing treatment with either escitalopram or nortriptyline in which the C825T SNP and three further SNPs in GNB3 were genotyped. The TT genotype was significantly associated with a superior response to nortriptyline and these effects were specific to improvements in neurovegetative symptoms. In addition, the same genotype predicted fewer incidents of treatment-emergent insomnia and greater weight gain on the same drug. Our results are consistent with previous associations with GNB3 and emphasize the importance of signalling genes in antidepressant response.Entities:
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Year: 2010 PMID: 20826553 DOI: 10.1177/0269881110376683
Source DB: PubMed Journal: J Psychopharmacol ISSN: 0269-8811 Impact factor: 4.153