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Examine the association between polymorphisms in the AKT1 and AKTIP genes and late-onset depression (LOD). Major depressive disorder is one of the most prevalent neuropsychiatric diseases. LOD is a disorder that starts after 65 years old. AKT1 is a downstream enzyme that has been implicated in the pathogenesis of neurotransmitter-related disorders, such as depression. The identification of a novel AKT1-binding protein (AKTIP) was pointed as an important new target. AKTIP binds directly to AKT1, enhancing the phosphorylation of regulatory sites, and this modulation are affected by AKT1 activation. The association of AKT1 and AKTIP polymorphisms with depressive symptoms was not investigated in LOD. Genotype tagSNPs in the AKT1 and AKTIP in LOD patients and controls. An academic medical center. Sample composed by 190 outpatients with LOD and 77 healthy individuals. The participants were evaluated using Diagnostic and Statistical Manual IV criteria, MINI-PLUS and the Geriatric Depression Scale. Our findings suggested an association between the tagSNP rs3730358 homozygous A/A (p = 0.006) and LOD. A strong association of allele A and increased association for LOD was demonstrated with tagSNP rs3730358 (p-value = 0.003). Limitation include composition of our control group, where the exclusion criteria generated a kind of super-healthy older group what might have produced a hidden stratification when compared with the LOD. This study is the first one to establish the association of the AKT1/AKTIP genes and LOD, and further studies are necessary to clarify the functional role of these proteins. Copyright © 2013 John Wiley & Sons, Ltd.

Citation

Patricia Araújo Pereira, Maria Aparecida Camargos Bicalho, Edgar Nunes de Moraes, Leandro Malloy-Diniz, Isadora Cristine Reis Sguizzato Bozzi, Rodrigo Nicolato, Daniela Rosa Valadão, Debora Marques Miranda, Marco Aurélio Romano-Silva. Genetic variant of AKT1 and AKTIP associated with late-onset depression in a Brazilian population. International journal of geriatric psychiatry. 2014 Apr;29(4):399-405

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PMID: 24022875

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