心理学
海马结构
萧条(经济学)
FKBP5型
西酞普兰
肿瘤科
海马体
内科学
新加坡元1
糖皮质激素
抗抑郁药
医学
临床心理学
精神科
糖皮质激素受体
宏观经济学
经济
作者
Raegan Mazurka,Simone Cunningham,Stefanie Hassel,Jane A. Foster,Nikita Nogovitsyn,Laura M. Fiori,Stephen C. Strother,Stephen R. Arnott,Benício N. Frey,Raymond W. Lam,Glenda MacQueen,Roumen Milev,Susan Rotzinger,Gustavo Turecki,Sidney H. Kennedy,Kate L. Harkness
标识
DOI:10.1016/j.euroneuro.2023.12.003
摘要
Preclinical research implicates stress-induced upregulation of the enzyme, serum- and glucocorticoid-regulated kinase 1 (SGK1), in reduced hippocampal volume. In the current study, we tested the hypothesis that greater SGK1 mRNA expression in humans would be associated with lower hippocampal volume, but only among those with a history of prolonged stress exposure, operationalized as childhood maltreatment (physical, sexual, and/or emotional abuse). Further, we examined whether baseline levels of SGK1 and hippocampal volume, or changes in these markers over the course of antidepressant treatment, would predict treatment outcomes in adults with major depression [MDD]. We assessed SGK1 mRNA expression from peripheral blood, and left and right hippocampal volume at baseline, as well as change in these markers over the first 8 weeks of a 16-week open-label trial of escitalopram as part of the Canadian Biomarker Integration Network in Depression program (MDD [n = 161] and healthy comparison participants [n = 91]). Childhood maltreatment was assessed via contextual interview with standardized ratings. In the full sample at baseline, greater SGK1 expression was associated with lower hippocampal volume, but only among those with more severe childhood maltreatment. In individuals with MDD, decreases in SGK1 expression predicted lower remission rates at week 16, again only among those with more severe maltreatment. Decreases in hippocampal volume predicted lower week 16 remission for those with low childhood maltreatment. These results suggest that both glucocorticoid-related neurobiological mechanisms of the stress response and history of childhood stress exposure may be critical to understanding differential treatment outcomes in MDD. ClinicalTrials.gov: NCT01655706 Canadian Biomarker Integration Network for Depression Study.
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