Article ID Journal Published Year Pages File Type
337026 Psychoneuroendocrinology 2011 11 Pages PDF
Abstract

SummaryBackgroundCortisol controls the activity of the hypothalamic–pituitary–adrenal (HPA) axis during stress and during the circadian cycle through central mineralocorticoid (MR) and glucocorticoid receptors (GR). Changes in MR and GR functioning, therefore, may affect HPA axis activity. In this study we examined the effect of common functional MR gene variants on the cortisol awakening response (CAR), which is often disturbed in stress-related disorders like depression.MethodsCommon functional MR single nucleotide polymorphisms (SNPs; MR −2G/C and I180V) and haplotypes were tested for association with variability in the CAR in a large cohort (Netherlands Study of Depression and Anxiety, NESDA) of patients diagnosed with a lifetime major depressive disorder (MDD). Saliva cortisol measurements and genotypes could be obtained from a total of 1026 individuals, including 324 males and 702 females.ResultsThe MR −2C/C genotype was associated with an attenuated CAR increase in women (p = .03) but not in men (p = .18; p = .01 for SNP-by-sex interaction). The MR I180V SNP had no significant effect on the CAR. Additional analysis revealed that effect of the −2G/C SNP on the CAR was due to an interaction with frequent use of selective serotonin reuptake inhibitors (SSRIs). Only in subjects using SSRIs (men and women) highest total morning cortisol levels were observed in −2G/G carriers, while the CAR was completely flattened in women with the −2C/C genotype (p < .05). The results were independent of multiple potential confounders and had an effect size of r = .14–.27.ConclusionsThis study shows that the MR −2G/C SNP modulated the CAR only in the MDD patients using SSRIs, with a clear allele–dose effect in women. This suggests that effect of SSRIs on cortisol regulation depends in part on the MR genotype with possible implications for future treatment selection.

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