Use of a GH receptor antagonist (GHRA) to explore the relationship between GH and IGF-I in adults with severe GH deficiency (GHD)

Summary Objective  At diagnosis, approximately 50% of adults with severe GH deficiency (GHD) have an IGF-I within the reference range. It is unclear whether in such patients serum IGF-I levels are regulated by factors other than GH. Design and patients  We performed a double-blind, randomized, placebo-controlled, cross-over study to investigate the effect of the GH receptor antagonist – pegvisomant (20 mg daily for 14 days) on GH and IGF-I levels in three cohorts: patients with GHD and a normal IGF-I (NORMS); patients with GHD and a low IGF-I (LOWS) and healthy volunteers (CONS). Results  Pegvisomant decreased IGF-I in CONS and NORMS [158·5 (101–206) vs. 103 (77–125) µg/l, P < 0·01; 124 (81–136) vs. 95 (51–113) µg/l, P < 0·01 respectively], but not in LOWS [31 (< 31–32) vs. 34·5 (< 31–38) µg/l], and this was associated with an increase in mean 24 h GH in CONS [0·49 (0·12–0·89) to 1·38 (0·22–2·45) µg/l (P = 0·03)] and in NORMS [69 (0–320)% from 0·1 (< 0·1–0·13) to 0·17 (0·11–0·42) µg/l (P = 0·03)], but not in the LOWS. The peak GH response to arginine was increased by pegvisomant in CONS and NORMS [6·1 (0·8–9) vs. 20·4 (13·1–28·8) µg/l, P = 0·03; 0·4 (0·1–0·5) vs. 0·5 (0·3–0·6) µg/l, respectively], but not in LOWS. Conclusions  These data indicate that patients with severe GHD with a normal IGF-I are able to increase GH secretion in response to a pegvisomant-induced fall in IGF-I, whereas those with low IGF-I levels are unable to increase GH secretion. Therefore circulating IGF-I appears to be GH-independent in GHD patients with a low IGF-I, but remains partially GH-dependant in GHD patients with a normal IGF-I.