A CARBOXYL-TERMINAL PEPTIDE FROM THE PARATHYROID HORMONE-RELATED PROTEIN INHIBITS BONE-RESORPTION BY OSTEOCLASTS

被引：146

作者：

FENTON, AJ

KEMP, BE

KENT, GN

MOSELEY, JM

ZHENG, MH

ROWE, DJ

BRITTO, JM

MARTIN, TJ

NICHOLSON, GC

机构：

[1] UNIV WESTERN AUSTRALIA, FREMANTLE HOSP, DEPT MED, FREMANTLE, WA 6160, AUSTRALIA

[2] UNIV MELBOURNE, ST VINCENTS INST MED RES, FITZROY, VIC 3065, AUSTRALIA

[3] UNIV MELBOURNE, DEPT MED, FITZROY, VIC 3065, AUSTRALIA

[4] SIR CHARLES GAIRDNER HOSP, DEPT ENDOCRINOL & DIABET, NEDLANDS, WA 6009, AUSTRALIA

来源：

ENDOCRINOLOGY | 1991年 / 129卷 / 04期

关键词：

D O I：

10.1210/endo-129-4-1762

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

PTH-related protein (PTHrP) interacts, via its amino-terminal 34 residues, with PTH receptors on osteoblasts to stimulate osteoclastic bone resorption indirectly. We now report that mature hPTHrP-(1-141) (EC50, approximately 10(-11) M) and a carboxyl-terminal fragment, PTHrP-(107-139) (EC50, approximately 10(-15) M), are potent inhibitors of resorption in an isolated rat osteoclast bone resorption assay, whereas hPTHrP-(1-108) and hPTHrP-(1-34) are inactive in this respect. PTHrP-(107-139) also inhibits resorption in a rat long bone organ culture system and reduces osteoclast spreading. PTHrP-(107-139) does not act on osteoclasts via a cAMP signal transduction mechanism, but its effects may be mediated by protein kinase-C. This previously unrecognized action of PTHrP, to inhibit osteoclastic bone resorption directly, indicates that PTHrP may be a precursor of multiple biologically active peptides with differing physiological functions.

引用

页码：1762 / 1768

页数：7

共 35 条

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