Response of the Renal Vitamin D Endocrine System to Oxidized Parathyroid Hormone (1-34)
- 1 November 1982
- journal article
- research article
- Published by Frontiers Media SA in Experimental Biology and Medicine
- Vol. 171 (2) , 191-195
- https://doi.org/10.3181/00379727-171-41497
Abstract
Two preparations of bovine parathyroid hormone (bPTH), the natural bPTH(1-84) and the synthetic bPTH(1-34) fragment, were treated with hydrogen peroxide and assayed for the effect of such treatment on the renal vitamin D endocrine system in Japanese quail. The oxidized and untreated preparations were injected i.m. into 4-wk-old male Japanese quail, 12 h after which the kidneys were removed and homogenized. The kidney homogenates were incubated with tritiated 25-hydroxyvitamin D3[25-(OH)D3] and the production rates of 1,25-(OH)2D3 and of 24,25-(OH)2D3 were determined as indices of 25-(OH)D3-1-hydroxylase and 25-(OH)D3-24-hydroxylase activities, respectively. Both untreated bPTH(1-34) and untreated bPTH(1-84) stimulated 1-hydroxylase and suppressed 24-hydroxylase activities. Oxidation of either bPTH(1-34) or bPTH(1-84) did not eliminate these responses, while the effects of oxidation on other responses to bPTH(1-34), namely inactivation of the hypotensive and renal adenylate cyclase stimulating responses, were observed as anticipated from earlier observations. The importance of these findings is heightened when viewed in the context of previous reports that oxidation of bPTH(1-34) leaves the hypercalcemic and hypocalciuric responses intact while partially or possibly totally inactivating all other major responses studied to date. The mechanisms involved in effecting the hypercalcemic, hypocalciuric and renal 25-(OH)D3-1-hydroxylase responses to bPTH(1-34) demand structural requirements in the peptide molecule which are different from those needed to effect the hyperphosphaturic, hypophosphatemic, hypotensive, smooth muscle relaxing and renal adenylate cyclase responses.This publication has 6 references indexed in Scilit:
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