Abstract

Skeletal maturation can be delayed by reducing the exposure to estrogens, either by halting pubertal development through administering a GnRH analogue (GnRHa), or by blocking the conversion of androgens to estrogens through an aromatase inhibitor (AI). These agents have been investigated in children with growth disorders (off-label), either alone or in combination with recombinant human growth hormone (rhGH). GnRHa is effective in attaining a normal adult height (AH) in the treatment of children with central precocious puberty, but its effect in short children with normal timing of puberty is equivocal. If rhGH-treated children with growth hormone deficiency or those who were born small-for-gestational age are still short at pubertal onset, co-treatment with a GnRHa for 2-3 years increases AH. A similar effect was seen by adding rhGH to GnRHa treatment of children with central precocious puberty with a poor AH prediction and by adding rhGH plus GnRHa to children with congenital adrenal hyperplasia with a poor predicted adult height on conventional treatment with gluco- and mineralocorticoids. In girls with idiopathic short stature and relatively early puberty, rhGH plus GnRHa increases AH. Administration of letrozole to boys with constitutional delay of growth puberty may increase AH, and rhGH plus anastrozole may increase AH in boys with growth hormone deficiency or idiopathic short stature, but the lack of data on attained AH and potential selective loss-of-follow-up in several studies precludes firm conclusions. GnRHas appear to have a good overall safety profile, while for aromatase inhibitors conflicting data have been reported.

Highlights

  • There are three therapeutic approaches to increase adult height (AH) for a child with a growth disorder

  • Experiments of nature have suggested that keeping the estrogen exposure low in adolescence might delay skeletal maturation and increase AH, which has led to clinical studies on the efficacy and safety of two forms of medication aimed at reducing estrogen exposure, i.e. gonadotropin-releasing hormone (GnRH) analogues (GnRHas) and aromatase inhibitors (AIs)

  • I believe that the cumulative observations of published reports on the use of GnRH analogue (GnRHa) for different specific conditions may still lead to general conclusions on their efficacy in growth disorders

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Summary

INTRODUCTION

There are three therapeutic approaches to increase adult height (AH) for a child with a growth disorder. I believe that the cumulative observations of published reports (mainly offering a low grade of evidence when assessed separately) on the use of GnRHas for different specific conditions may still lead to general conclusions on their efficacy in growth disorders. This implies that a detailed analysis of strengths and weaknesses of all published data is warranted, followed by a general assessment.

The Effect of a GnRH Analogue Alone
Design
Safety of GnRHas in Childhood and Adolescence
THE EFFECT OF AROMATASE INHIBITORS
The effect of Aromatase Inhibitors in Girls
Safety of Aromatase Inhibitors in Childhood and Adolescence
Findings
DISCUSSION AND CONCLUSION
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