Título HIGH-ACTIVITY VARIANTS OF THE UMAOA POLYMORPHISM INCREASE THE RISK FOR DEPRESSION IN A LARGE PRIMARY CARE SAMPLE
Autores GUTIERREZ MARTINEZ, BLANCA , MOLINA RIVAS, ESTHER , TORRES GONZALEZ, FRANCISCO , BELLON SAAMEÑO, JUAN ANGEL , MORENO KUSTNER, BERTA , KING KING, MICHAEL , MARTINEZ GONZALEZ, LUIS JAVIER , NAZARETH, IRWIN , Martinez-Gonzalez-, Luis Javier , MARTINEZ ESPIN, ESTHER , Muñoz-García-, Maria Del Mar , MOTRICO MARTINEZ, EMMA, MARTINEZ-CAÑAVATE LOPEZ-MONTES, TERESA , LORENTE ACOSTA, JOSÉ ANTONIO , LUNA DEL CASTILLO, JUAN DE DIOS , CERVILLA BALLESTEROS, JORGE
Publicación externa Si
Medio Am. J. Med. Genet. B
Alcance Article
Naturaleza Científica
Cuartil JCR 2
Cuartil SJR 1
Impacto JCR 3.48100
Impacto SJR 1.78300
Web http://www.ncbi.nlm.nih.gov/pubmed/18626920
Fecha de publicacion 01/01/2009
ISI 000264675500012
DOI 10.1002/ajmg.b.30829
Abstract Studies on the association between the functional uMAOA Polymorphism and depression have yielded non-conclusive results up till now. One thousand two hundred twenty eight consecutive Spanish primary care attendees, participating in the PREDICT study, agreed to take part in this genetic PREDICT-Gene study. We explored the association between depression and either high-activity uMAOA alleles or genotypes. Depression was diagnosed using the Composite International Diagnostic Interview (CIDI) to establish three different depressive outcomes (ICD-10 Depressive Episode (DE), ICD-10 Severe Depressive Episode (SDE) and DSM-IV Major Depression (MD)). uMAOA genetic variation was determined by PCR amplification and subsequent electrophoresis. Crude and adjusted (gender and/or age) odds ratios, with 95% confidence intervals, were calculated for the associations between allele or genotype frequencies and all three depressive outcomes. We found associations between all three depressive phenotypes and either high-activity alleles or high-activity genotypes in both sexes. The associations were statistically significant for females but not for males. Testing the same associations on the entire sample (males and females) also yielded significant associations between depression and either high-activity alleles or high-activity genotype distribution that were independent of age and/or gender (ICD-10 DE: OR = 1.98; 95% CI: 1.42-1.77; P = 0.00002; ICD-10-SDE: OR = 2.05; 95% CI: 1.38-3.05; P = 0.0002; DSM-IV MD: OR = 1.9 1; 95% CI: (1.26-2.1); P = 0.0014). Our results provide fairly consistent evidence that high-activity variants of the MAOA promoter polymorphism confer a modestly higher risk for depression. (C) 2008 Wiley-Liss, Inc.
Palabras clave MAOA; uMAOA polymorphism; depression; association study
Miembros de la Universidad Loyola

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