Functional mineralocorticoid receptor (MR) gene variation influences the cortisol awakening response after dexamethasone
Functional mineralocorticoid receptor (MR) gene variation influences the cortisol awakening response after dexamethasone
Stress causes activation of the hypothalamic-pituitary-adrenal (HPA) axis and results in the secretion of corticosteroids, which facilitate behavioral adaptation and promote the termination of the stress response. These actions exerted by cortisol are mediated by two brain corticosteroid receptor types: the high affinity mineralocorticoid (MR) and the low affinity glucocorticoid receptor (GR). Dexamethasone is a potent GR agonist with affinity to MR. Administration of dexamethasone in the evening results in a significant suppression of the morning cortisol awakening response (CAR). Here we tested the involvement of MR variants in this effect of dexamethasone in 218 young healthy subjects (125 females, all using oral contraceptives). For this purpose we determined two single nucleotide polymorphisms (SNPs) in the MR gene, the previously described MRI180V (rs5522) and the MR-2G/C (rs2070951), which both affect in vitro the transactivational capacity of the MR in response to either cortisol or dexamethasone. Administration of a low dose dexamethasone (0.25 mg) at 2300 h resulted in a significant suppression of the cortisol awakening response (CAR). Both SNPs modulated the suppression of the CAR after dexamethasone significantly and in a sex specific manner. Suppression of the CAR was highest in the female MR-2G/C GG subjects while in male GG subjects the dexamethasone suppression of the CAR was attenuated compared to the MR-2G/C GC and CC groups. For the MRI180V, male AA subjects showed after dexamethasone a higher CAR than AG subjects while this effect was not observed in females. The SNPs had no significant influence on the CAR without prior dexamethasone treatment. The association of the CAR with functional MR gene variants only in dexamethasone treated subjects suggests the involvement of MR in dexamethasone induced suppression of morning cortisol.
mineralocorticoid receptor, genetic variation, HPA axis, dexamethasone, cortisol
339-349
van Leeuwen, Nienke
9381167a-3b81-40d1-afe2-69b3872fdecf
Kumsta, Robert
88285030-6a7c-4ef1-ba75-b78e09cd2f1e
Entringer, Sonja
f96a0401-9da9-4f00-aada-b6a3569501ba
de Kloet, Ronald
66484ff8-d07a-49c7-be0a-8d73a93f4f0f
Zitman, Frans
87ff564a-d3a1-4eb9-bf65-694d32250381
DeRijk, Roel
70e3f165-74fd-41b0-bdda-ffd391e40f9a
Wust, Stefan
ab957fa6-da2b-4718-988c-de5962fa3200
April 2010
van Leeuwen, Nienke
9381167a-3b81-40d1-afe2-69b3872fdecf
Kumsta, Robert
88285030-6a7c-4ef1-ba75-b78e09cd2f1e
Entringer, Sonja
f96a0401-9da9-4f00-aada-b6a3569501ba
de Kloet, Ronald
66484ff8-d07a-49c7-be0a-8d73a93f4f0f
Zitman, Frans
87ff564a-d3a1-4eb9-bf65-694d32250381
DeRijk, Roel
70e3f165-74fd-41b0-bdda-ffd391e40f9a
Wust, Stefan
ab957fa6-da2b-4718-988c-de5962fa3200
van Leeuwen, Nienke, Kumsta, Robert, Entringer, Sonja, de Kloet, Ronald, Zitman, Frans, DeRijk, Roel and Wust, Stefan
(2010)
Functional mineralocorticoid receptor (MR) gene variation influences the cortisol awakening response after dexamethasone.
Psychoneuroendocrinology, 35 (3), .
(doi:10.1016/j.psyneuen.2009.07.006).
Abstract
Stress causes activation of the hypothalamic-pituitary-adrenal (HPA) axis and results in the secretion of corticosteroids, which facilitate behavioral adaptation and promote the termination of the stress response. These actions exerted by cortisol are mediated by two brain corticosteroid receptor types: the high affinity mineralocorticoid (MR) and the low affinity glucocorticoid receptor (GR). Dexamethasone is a potent GR agonist with affinity to MR. Administration of dexamethasone in the evening results in a significant suppression of the morning cortisol awakening response (CAR). Here we tested the involvement of MR variants in this effect of dexamethasone in 218 young healthy subjects (125 females, all using oral contraceptives). For this purpose we determined two single nucleotide polymorphisms (SNPs) in the MR gene, the previously described MRI180V (rs5522) and the MR-2G/C (rs2070951), which both affect in vitro the transactivational capacity of the MR in response to either cortisol or dexamethasone. Administration of a low dose dexamethasone (0.25 mg) at 2300 h resulted in a significant suppression of the cortisol awakening response (CAR). Both SNPs modulated the suppression of the CAR after dexamethasone significantly and in a sex specific manner. Suppression of the CAR was highest in the female MR-2G/C GG subjects while in male GG subjects the dexamethasone suppression of the CAR was attenuated compared to the MR-2G/C GC and CC groups. For the MRI180V, male AA subjects showed after dexamethasone a higher CAR than AG subjects while this effect was not observed in females. The SNPs had no significant influence on the CAR without prior dexamethasone treatment. The association of the CAR with functional MR gene variants only in dexamethasone treated subjects suggests the involvement of MR in dexamethasone induced suppression of morning cortisol.
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Published date: April 2010
Keywords:
mineralocorticoid receptor, genetic variation, HPA axis, dexamethasone, cortisol
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Local EPrints ID: 72990
URI: http://eprints.soton.ac.uk/id/eprint/72990
ISSN: 0306-4530
PURE UUID: 6e88275c-4195-42de-9613-4523ba8e88c2
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Date deposited: 25 Feb 2010
Last modified: 13 Mar 2024 21:47
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Author:
Nienke van Leeuwen
Author:
Robert Kumsta
Author:
Sonja Entringer
Author:
Ronald de Kloet
Author:
Frans Zitman
Author:
Roel DeRijk
Author:
Stefan Wust
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