Please use this identifier to cite or link to this item: http://hdl.handle.net/10668/10078
Title: Cortistatin Is a Key Factor Regulating the Sex-Dependent Response of the GH and Stress Axes to Fasting in Mice.
Authors: Cordoba-Chacón, José
Gahete, Manuel D
Pozo-Salas, Ana I
de Lecea, Luis
Castaño, Justo P
Luque, Raúl M
metadata.dc.subject.mesh: Adrenocorticotropic Hormone
Animals
Blood Glucose
Cells, Cultured
Corticosterone
Fasting
Female
Ghrelin
Growth Hormone
Insulin
Leptin
Male
Mice
Mice, Knockout
Neuropeptides
Pituitary Gland
Sex Factors
Stress, Physiological
Stress, Psychological
Issue Date: 13-May-2016
Abstract: Cortistatin (CORT) shares high structural and functional similarities with somatostatin (SST) but displays unique sex-dependent pituitary actions. Indeed, although female CORT-knockout (CORT-KO) mice exhibit enhanced GH expression/secretion, Proopiomelanocortin expression, and circulating ACTH/corticosterone/ghrelin levels, male CORT-KO mice only display increased plasma GH/corticosterone levels. Changes in peripheral ghrelin and SST (rather than hypothalamic levels) seem to regulate GH/ACTH axes in CORT-KOs under fed conditions. Because changes in GH/ACTH axes during fasting provide important adaptive mechanisms, we sought to determine whether CORT absence influences GH/ACTH axes during fasting. Accordingly, fed and fasted male/female CORT-KO were compared with littermate controls. Fasting increased circulating GH levels in male/female controls but not in CORT-KO, suggesting that CORT can be a relevant regulator of GH secretion during fasting. However, GH levels were already higher in CORT-KO than in controls in fed state, which might preclude a further elevation in GH levels. Interestingly, although fasting-induced pituitary GH expression was elevated in both male/female controls, GH expression only increased in fasted female CORT-KOs, likely owing to specific changes observed in key factors controlling somatotrope responsiveness (ie, circulating ghrelin and IGF-1, and pituitary GHRH and ghrelin receptor expression). Fasting increased corticosterone levels in control and, most prominently, in CORT-KO mice, which might be associated with a desensitization to SST signaling and to an augmentation in CRH and ghrelin-signaling regulating corticotrope function. Altogether, these results provide compelling evidence that CORT plays a key, sex-dependent role in the regulation of the GH/ACTH axes in response to fasting.
URI: http://hdl.handle.net/10668/10078
metadata.dc.identifier.doi: 10.1210/en.2016-1195
Appears in Collections:Producción 2020

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