Abstract
Substitution of arginine for glycine at position 120 in native 22-kDa human growth hormone (hGH) results in an analogue, G120R, which is unable to dimerize the GH receptor and is widely used to probe the molecular mechanism of action of hGH. When acting on human GH receptors, G120R antagonizes several biological effects of hGH, but is itself inactive as an agonist. It has been reported that this mutant also antagonizes hGH activation of the rat or human prolactin (PRL) receptor in cell-based assays, with no agonist activity. We have now tested this mutant in a sensitive MTT (3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide)-ESTA (eluted stain assay) bioassay using rat PRL receptors in the Nb2 cell line. We confirm that G120R acts as an efficient antagonist of native hGH, but show that it can also act as an agonist to generate intracellular signals leading to metabolic activation and proliferation of Nb2 cells. We have demonstrated an unusual sensitivity to the presence of zinc (Zn2+). In the absence of added Zn2+, G120R shows weak but full agonist activity in the bioassay, and this can be blocked by co-incubation with recombinant hGH-binding protein. G120R can therefore be utilized to discriminate between the molecular mechanisms of hGH interactions with its somatogenic and lactogenic receptors. Future studies with G120R in the rat may need to take account of its significant agonist effects on PRL receptors.
Highlights
Substitution of arginine for glycine at position 120 in native 22·kDa human growth hormone results in an analogue, G120R, which is unable to dimerize the GH receptor and is widely used to probe the molecular mechanism of action of hGH
We report that G120R stimulates Nb2 cells in the MTT-ESTA bioassay." We have characterized its actions, both as an agonist and an antagonist, and shown that discrepancies with previous reports may be explained by the unexpected sensitivity of the G120RJrPRL receptor interaction to zinc (Zn2 +)
The Effect of the hGH Analogue G120R on Nb2 Cells-In the absence of added Zn2 +, dose-related stimulation ofNb2 cells by G120R was observed over the concentration range 0.28-142 nM, with an EC 50 of 1.27 nM (Fig. 1)
Summary
Vol 270, No 16, Issue of April 21, pp. 9222-9226, 1995 Printed in U.S.A. G120R, a Human Growth Hormone Antagonist, Shows Zinc-dependent Agonist and Antagonist Activity on Nb2 Cells*. Substitution of arginine for glycine at position 120 in native 22·kDa human growth hormone (hGH) results in an analogue, G120R, which is unable to dimerize the GH receptor and is widely used to probe the molecular mechanism of action of hGH. It has been reported that this mutant antagonizes hGH activation of the rat or human prolactin (PRL) receptor in cell-based assays, with no agonist activity. G120R can bind normally via site 1 to the first receptor, it is thought that recruitment of the second receptor, and receptor dimerization, is blocked by the arginine substitution at the critical position in site 2 This would account for both the failure of G120R to act as an agonist and its ability to antagonize wild-type hGH. A oo... 40 x oc 30 o -4=;~~:!im;::;:;:;&I~ii=;:;:m;;=;::;:;;;::;:;m;;:;:;:;iii':;:;:;:;~
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