A putatively functional polymorphism in the HTR2C gene is associated with depressive symptoms in white females reporting significant life stress.

dc.contributor.author

Brummett, Beverly H

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Babyak, Michael A

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Williams, Redford B

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Harris, Kathleen Mullan

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Jiang, Rong

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Kraus, William E

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Singh, Abanish

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Costa, Paul T

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Georgiades, Anastasia

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Siegler, Ilene C

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Walss-Bass, Consuelo

dc.date.accessioned

2018-10-31T18:25:40Z

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2018-10-31T18:25:40Z

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2014-01

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2018-10-31T18:25:38Z

dc.description.abstract

Psychosocial stress is well known to be positively associated with subsequent depressive symptoms. Cortisol response to stress may be one of a number of biological mechanisms that links psychological stress to depressive symptoms, although the precise causal pathway remains unclear. Activity of the x-linked serotonin 5-HTR2C receptor has also been shown to be associated with depression and with clinical response to antidepressant medications. We recently demonstrated that variation in a single nucleotide polymorphism on the HTR2C gene, rs6318 (Ser23Cys), is associated with different cortisol release and short-term changes in affect in response to a series of stress tasks in the laboratory. Based on this observation, we decided to examine whether rs6318 might moderate the association between psychosocial stress and subsequent depressive symptoms. In the present study we use cross-sectional data from a large population-based sample of young adult White men (N = 2,366) and White women (N = 2,712) in the United States to test this moderation hypothesis. Specifically, we hypothesized that the association between self-reported stressful life events and depressive symptoms would be stronger among homozygous Ser23 C females and hemizygous Ser23 C males than among Cys23 G carriers. In separate within-sex analyses a genotype-by-life stress interaction was observed for women (p = .022) but not for men (p = .471). Homozygous Ser23 C women who reported high levels of life stress had depressive symptom scores that were about 0.3 standard deviations higher than female Cys23 G carriers with similarly high stress levels. In contrast, no appreciable difference in depressive symptoms was observed between genotypes at lower levels of stress. Our findings support prior work that suggests a functional SNP on the HTR2C gene may confer an increased risk for depressive symptoms in White women with a history of significant life stress.

dc.identifier

PONE-D-14-28787

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1932-6203

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1932-6203

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https://hdl.handle.net/10161/17608

dc.language

eng

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Public Library of Science (PLoS)

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PloS one

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10.1371/journal.pone.0114451

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Humans

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Hydrocortisone

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Receptor, Serotonin, 5-HT2C

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Cross-Sectional Studies

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Stress, Psychological

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Depressive Disorder

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Sex Factors

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Genotype

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Polymorphism, Single Nucleotide

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Adult

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European Continental Ancestry Group

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United States

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Female

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Male

dc.title

A putatively functional polymorphism in the HTR2C gene is associated with depressive symptoms in white females reporting significant life stress.

dc.type

Journal article

duke.contributor.orcid

Williams, Redford B|0000-0002-8581-0648

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Jiang, Rong|0000-0003-0757-9310

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Kraus, William E|0000-0003-1930-9684

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Costa, Paul T|0000-0003-4375-1712

pubs.begin-page

e114451

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12

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School of Medicine

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Duke

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Psychiatry & Behavioral Sciences, Behavioral Medicine

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Psychiatry & Behavioral Sciences

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Clinical Science Departments

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Nursing

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School of Nursing

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Duke Cancer Institute

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Institutes and Centers

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Duke Molecular Physiology Institute

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Medicine, Cardiology

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Medicine

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Psychology and Neuroscience

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Trinity College of Arts & Sciences

pubs.publication-status

Published

pubs.volume

9

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