Comparative Inhibition of the GH/IGF-I Axis Obtained With Either the Targeted Secretion Inhibitor SXN101959 or the Somatostatin Analog Octreotide in Growing Male Rats

Author:

Somm Emmanuel1,Bonnet Nicolas2,Zizzari Philippe3,Tolle Virginie3,Toulotte Audrey1,Jones Richard4,Epelbaum Jacques3,Martinez Alberto4,Hüppi Petra S.1,Aubert Michel L.1

Affiliation:

1. Division of Development and Growth (E.S., A.T., P.S.H., M.L.A.), University of Geneva School of Medicine, 1211 Geneva 14, Switzerland

2. Department of Paediatrics, and Division of Bone Diseases (N.B.), University of Geneva School of Medicine, 1211 Geneva 14, Switzerland; Department of Rehabilitation and Geriatrics, University of Geneva School of Medicine, 1211 Geneva 14, Switzerland

3. Unité Mixte de Recherche 894 Institut National de la Santé et de la Recherche Médicale (P.Z., V.T., J.E.), Centre de Psychiatrie et Neurosciences, Université Paris Descartes, Sorbonne Paris Cité Paris, France

4. Syntaxin Ltd (R.J., A.M.), Abingdon OX14 3YS, United Kingdom

Abstract

Abnormally high GH/IGF-I levels, most often caused by adenomas arising from pituitary somatotrophs, generate deleterious effects. We recently described a targeted secretion inhibitor (SXN101742) comprising a GHRH domain and the endopeptidase domain of botulinum toxin serotype D (GHRH-light chain endopeptidase type D domain [LC/D] associated to a heavy chain translocation domain [HN]) able to down-regulate the GH/IGF-I axis. In the present study, we compared the effect of a single iv bolus of a related molecule developed for clinical studies (SXN101959, 1 mg/kg) with a sc infusion of the somatostatin analog octreotide (SMS201–995, 10 μg/kg·h) to lower GH/IGF-I activity in growing male rats. Ten days after administration of SXN101959 or initiation of the octreotide infusion, body and pituitary weights, body length, GH peaks, and IGF-I production were reduced by both treatments but to a greater extent with SXN101959. In contrast to unaltered GH gene expression and increased GH storage in pituitaries from octreotide-treated rats, the inhibition of GH secretion was associated with a collapse of both GH mRNA and protein level in pituitaries from SXN101959-treated rats, in line with a specific decrease in hypothalamic GHRH production, not observed with octreotide. SXN101959 did not induce major apoptotic events in anterior pituitary and exhibited a reversible mode of action with full recovery of somatotroph cell functionality 30 days after treatment. Octreotide infusion permanently decreased ghrelin levels, whereas SXN101959 only transiently attenuated ghrelinemia. Both treatments limited bone mass acquisition and altered specifically tissues development. In conclusion, SXN101959 exerts a powerful and reversible inhibitory action on the somatotropic axis. Specific features of SXN101959, including long duration of action coupled to a strong inhibition of pituitary GH synthesis, represent advantages when treating overproduction of GH.

Publisher

The Endocrine Society

Subject

Endocrinology

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