Study Report

Reference
Citation | Kanellopoulos, 2011 PubMed |
Full Info | Kanellopoulos, D., Gunning, F.M., Morimoto, S.S., Hoptman, M.J., Murphy, C.F., Kelly, R.E., Glatt, C., Lim, K.O. and Alexopoulos, G.S. (2011) Hippocampal volumes and the brain-derived neurotrophic factor val66met polymorphism in geriatric major depression. Am J Geriatr Psychiatry, 19, 13-22.
|

Study
Hypothesis or Background |
structural abnormalities in the hippocampus have been implicated in the pathophysiology of major depressive disorder (MDD). The brain-derived neurotrophic factor (BDNF) val66met polymorphism may contribute to these abnormalities and therefore confer vulnerability to MDD. This study examined whether there is a relationship among BDNF genotype, hippocampal volumes, and MDD in older adults.
|
Sample Information | thirty-three older adults with MDD and 23 psychiatrically normal comparison subjects were studied. |
Method Detail | Structural magnetic resonance imaging analysis was used to quantify hippocampal volumes. A repeated-measures analysis of covariance examined the relationships among BDNF val66met (val/val, met carrier), diagnosis (depressed, nondepressed), and hippocampal volumes (right, left). Age, gender, education, and whole brain volume were included as covariates. |
Method Keywords | magnetic resonance imaging (MRI); genotyping |
Result | elderly MDD BDNF val/val homozygotes had significantly higher right hippocampal volumes compared with nondepressed val/val subjects. However, there was no difference between the depressed and healthy nondepressed met carriers. In addition, depressed met carriers had an earlier age of onset of depressive illness than val/val homozygotes, but age of onset did not moderate the relationship between hippocampal volumes and MDD diagnosis. |
Conclusions | these results provide preliminary evidence of a neuroprotective role of the val/val genotype, suggesting that neurotrophic factor production protects against pathophysiological processes triggered by depression in older adults with later age of onset of MDD. The BDNF val66met polymorphism may play a salient role in structural alterations of the hippocampus in older adults with MDD. |

Relationships reported by
Kanellopoulos, 2011
Component A Approved Name (Name in Paper) |
Component A Type |
Component B Approved Name (Name in Paper) |
Component B Type |
Statistical Result |
Relationship Description |
Result Category (Positive/Negative)) |
MDD
|
syndrome |
Hippocampus (hippocampal volumes) |
brain morphology and function |
|
elderly MDD BDNF val/val homozygotes had significantly higher right hippocampal volumes compared with nondepressed val/val subjects. |
Positive
|
Hippocampus (hippocampal volumes)
|
brain morphology and function |
BDNF (BDNF) |
gene |
|
elderly MDD BDNF val/val homozygotes had significantly higher right hippocampal volumes compared with nondepressed val/val subjects. |
Positive
|
MDD
|
syndrome |
BDNF (BDNF) |
gene |
|
elderly MDD BDNF val/val homozygotes had significantly higher right hippocampal volumes compared with nondepressed val/val subjects. In addition, depressed met carriers had an earlier age of onset of depressive illness than val/val homozygotes |
Positive
|