Author:
Herbert J.,Ban M.,Brown G. W.,Harris T. O.,Ogilvie A.,Uher R.,Craig T. K. J.
Abstract
BackgroundCommon genetic variants, such as the brain-derived neurotrophic factor
(BDNF) Val/66/Met polymorphism (rs6265), are known to interact with
environmental factors such as early adversity to increase the risk of
subsequent major depression. Much less is known about how they interact
with individual differences in cortisol, although these also represent a
risk for major depression.AimsTo determine whether this BDNF variant moderated the risk represented by
higher levels of morning salivary cortisol in adult women.MethodWe recruited 279 premenopausal women who were at high risk of major
depressive disorder because of either negative self-evaluation,
unsupportive core relationship or chronic subclinical symptoms of
depression or anxiety. Morning salivary cortisol was measured daily for
up to 10 days at entry. Participants were followed up for about 12 months
by telephone calls at 3–4 monthly intervals. Major depression and severe
life events were assessed through interviews at baseline and follow-up;
DNA was obtained from the saliva.ResultsThere were 53 onsets (19%) of depressive episodes during follow-up. There
was a significant U-shaped relationship between adjusted morning cortisol
levels at baseline and the probability of depression onset during
follow-up. In total, 51% experienced at least one severe life
event/difficulty, and this strongly predicted subsequent onsets of
depressive episodes. The BDNF Val/66/Met genotype was
not directly associated with onsets of depression or with cortisol
levels, but there was significant interaction between Val/66/Met and
cortisol: the association between baseline cortisol and depression was
limited to those with the Val/66/Val variant. There was no interaction
between life events and either this BDNF polymorphism or cortisol
levels.ConclusionsMorning salivary cortisol interacts with the BDNF Val/66/Met polymorphism
in predicting new depressive episodes. This paper adds to the evidence
that single gene polymorphisms interact with endogenous factors to
predict depression.
Publisher
Royal College of Psychiatrists
Subject
Psychiatry and Mental health
Cited by
26 articles.
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