Abstract

To investigate growth hormone (GH) secretion at the transition age, retesting of all subjects who have undergone GH replacement therapy is recommended when linear growth and pubertal development are complete to distinguish between transitional and persistent GH deficiency (GHD). Early retesting of children with idiopathic and isolated GHD (i.e., before the achievement of final height and/or the adult pubertal stage) can avoid possible over-treatment. Here, we report data from our population with idiopathic and isolated GHD to encourage changes in the management and timing of retesting. We recruited 31 patients (19 males) with idiopathic GHD who received recombinant GH (rGH) for at least 2 years. All of the patients were retested at the transition age at least 3 months after rGH discontinuation. Permanent GHD was defined as a GH peak of <19 ng/mL after administration of growth hormone–releasing hormone (GHRH) + arginine as a provocative test. Permanent GHD was confirmed in only five of 31 patients (16.13%). None of these patients presented low serum insulin-like growth factor (IGF)-1 levels (<−2 standard deviation score (SDS)). Only one male patient with an IGF-1 serum level lower than −2 SDS showed a normal GH stimulation response, with a GH peak of 44.99 ng/mL. Few patients with idiopathic and isolated GHD demonstrated persistence of the deficit when retested at the transition age, suggesting that the timing of retesting should be anticipated to avoid overtreatment.

Highlights

  • The diagnosis of growth hormone deficit (GHD) during childhood represents a complex process that includes auxological and clinical parameters and is associated with neuroradiological and chemical assessments [1]

  • All patients demonstrated a subnormal response to two different provocative tests

  • The results of our study demonstrated that the majority of subjects treated with recombinant GH (rGH) during childhood for idiopathic and isolated GHD, showed a complete recovery of normal Growth hormone (GH) secretion when retested at the transition age

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Summary

Introduction

The diagnosis of growth hormone deficit (GHD) during childhood represents a complex process that includes auxological and clinical parameters and is associated with neuroradiological and chemical assessments [1]. Idiopathic GHD is defined as either isolated or with one additional hormone deficit in the absence of a defined genetic cause, structural hypothalamic–pituitary abnormalities, central nervous system tumours or a history of high-dose cranial irradiation [2]. Growth hormone (GH) replacement therapy is a cornerstone to guarantee correct growth during childhood, but it plays a significant role in maintaining the physiological body composition and metabolic homeostasis throughout life [3]. Res. Public Health 2019, 16, 307; doi:10.3390/ijerph16030307 www.mdpi.com/journal/ijerph

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