Effect of GHS-R deletion on growth, pulsatile GH secretion and meal pattern in male and female mice

Author:

Labarthe Alexandra,Zizzari Philippe,Fiquet Oriane,Lebrun Nicolas,Veldhuis Johannes D.,Roelfsema Ferdinand,Chauveau Christophe,Bohlooly-Y Mohammad,Epelbaum Jacques,Tolle VirginieORCID

Abstract

Introduction. While the vast majority of research investigating the role of ghrelin or its receptor, GHS-R1a, on growth, feeding and metabolism has been conducted in male rodents, very little is known about sex differences in this system. Furthermore, the role of GHS-R1a signaling in the control of pulsatile GH secretion and its link with growth or metabolic parameters has never been characterized. Methods. We assessed the sex-specific contribution of GHS-R1a signaling on the activity of the GH/IGF-1 axis, metabolic parameters and feeding behavior in adolescent (5-6 weeks old) or adult (10-19 weeks old) GHS-R KO (Ghsr-/-) and WT (Ghsr+/+) male and female mice. Results. Adult Ghsr-/- male and female mice displayed deficits in weight and linear growth that was correlated with reduced GH pituitary contents in males only. GHS-R1a deletion was associated with reduced meal frequency and increased meal intervals, as well as reduced hypothalamic GHRH and NPY mRNA in males, not females. In adult, GH release from Ghsr-/- mice pituitary explants ex vivo was reduced independently of the sex. However, in vivo pulsatile GH secretion decreased in adult but not adolescent Ghsr-/- females, while in males, GHS-R1a deletion was associated with reduction in pulsatile GH secretion during adolescence exclusively. In males, linear growth did not correlate with pulsatile GH secretion, but rather with ApEn, a measure that reflects irregularity of the rhythmic secretion. Fat mass, plasma leptin concentrations or ambulatory activity did not predict differences in GH secretion. Discussion/Conclusion. These results point to a sex-dependent dimorphic effect of GHS-R1a signaling to modulate pulsatile GH secretion and meal pattern in mice with different compensatory mechanisms occuring in the hypothalamus of adult males and females after GHS-R1a deletion. Altogether, we show that GHS-R1a signaling plays a more critical role in the regulation of pulsatile GH secretion during adolescence in males and adulthood in females.

Publisher

S. Karger AG

Subject

Cellular and Molecular Neuroscience,Endocrine and Autonomic Systems,Endocrinology,Endocrinology, Diabetes and Metabolism

Reference55 articles.

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