Ghrelin and obestatin modulate growth hormone‐releasing hormone release and synaptic inputs onto growth hormone‐releasing hormone neurons

Ghrelin, a natural ligand of the growth hormone secretagogue receptor (GHS‐R), is synthesized in the stomach but may also be expressed in lesser quantity in the hypothalamus where the GHS‐R is located on growth hormone‐releasing hormone (GHRH) neurons. Obestatin, a peptide derived from the same precursor as ghrelin, is able to antagonize the ghrelin‐induced increase of growth hormone (GH) secretion in vivo but not from pituitary explants in vitro . Thus, the blockade of ghrelin‐induced GH release by obestatin could be mediated at the hypothalamic level by the neuronal network that controls pituitary GH secretion. Ghrelin increased GHRH and decreased somatostatin (somatotropin‐releasing inhibitory factor) release from hypothalamic explants, whereas obestatin only reduced the ghrelin‐induced increase of GHRH release, thus indicating that the effect of ghrelin and obestatin is targeted to GHRH neurons. Patch‐clamp recordings on mouse GHRH‐enhanced green fluorescent protein neurons indicated that ghrelin and obestatin had no significant effects on glutamatergic synaptic transmission. Ghrelin decreased GABAergic synaptic transmission in 44% of the recorded neurons, an effect blocked in the presence of the GHS‐R antagonist BIM28163, and stimulated the firing rate of 78% of GHRH neurons. Obestatin blocked the effects of ghrelin by acting on a receptor different from the GHS‐R. These data suggest that: (i) ghrelin increases GHRH neuron excitability by increasing their action potential firing rate and decreasing the strength of GABA inhibitory inputs, thereby leading to an enhanced GHRH release; and (ii) obestatin counteracts ghrelin actions. Such interactions on GHRH neurons probably participate in the control of GH secretion.