Cortistatin Is Not a Somatostatin Analogue but
Stimulates Prolactin Release and Inhibits GH and
ACTH in a Gender-Dependent Fashion: Potential Role
of Ghrelin
posted on 2013-11-22, 00:00authored byJose Cordoba-Chacon, Manuel D. Gahete, Ana I. Pozo-Salas, Antonio J. Martínez-Fuentes, Luis de Lecea, Francisco Gracia-Navarro, Rhonda D. Kineman, Justo P. Castano, Raul M. Luque
Cortistatin (CST) and somatostatin (SST) evolve from a common ancestral gene and share remarkable
structural, pharmacological, and functional homologies. Although CST has been considered as a natural
SST-analogue acting through their shared receptors (SST receptors 1–5), emerging evidence indicates
that these peptides might in fact exert unique roles via selective receptors [e.g. CST, not SST, binds
ghrelin receptor growth hormone secretagogue receptor type 1a (GHS-R1a)]. To determine whether
theroleofendogenousCSTisdifferentfromSST,wecharacterizedtheendocrine-metabolicphenotype
of male/female CST null mice (cort / ) at hypothalamic-pituitary-systemic (pancreas-stomach-adrenal-
liver) levels. Also, CST effects on hormone expression/secretion were evaluated in primary pituitary
cell cultures from male/female mice and female primates (baboons). Specifically, CST exerted an unexpected
stimulatory role on prolactin (PRL) secretion, because both male/female cort / mice had
reduced PRL levels, and CST treatment (in vivo and in vitro) increased PRL secretion, which could be
blocked by a GHS-R1a antagonist in vitro and likely relates to the decreased success of female cort /
in first-litterpupcare at weaning. In contrast,CSTinhibitedGHandadrenocorticotropin-hormone axes
in a gender-dependent fashion. In addition, a rise in acylated ghrelin levels was observed in female
cort / mice, which were associated with an increase in stomach ghrelin/ghrelin O-acyl transferase
expression. Finally, CST deficit uncovered a gender-dependent role of this peptide in the regulation of
glucose-insulin homeostasis, because male, but not female, cort / mice developed insulin resistance.
The fact that these actions are not mimicked by SST and are strongly gender dependent offers new
grounds to investigate the hitherto underestimated physiological relevance of CST in the regulation of
physiological/metabolic processes.
Funding
This work was supported by Ayudas Predoctorales de Formacion en Investigacion en Salud del Fondo de Investigacion Sanitaria Grants ISCIII:FI06/00804 (to J.C.-C.) and FPU-AP20052473 (TO M.D.G.); BFU2010-19300 and CTS-5051 (to J.P.C.); and Programa Ramon y Cajal del Ministerio de Educacion y Ciencia Grants RYC-2007-00186 and JC2008-00220, BFU2008-01136/BFI (to R.M.L.).