Title of article
In vitro and in vivo activities of C-terminally truncated PTH peptides reveal a disconnect between cAMP signaling and functional activity
Author/Authors
Richard J. Murrills، نويسنده , , Jeanne J. Matteo، نويسنده , , Rachelle L. Samuel، نويسنده , , Jennifer L. Andrews، نويسنده , , Bheem M. Bhat، نويسنده , , Valerie E. Coleburn، نويسنده , , Yogendra P. Kharode، نويسنده , , Frederick J. Bex، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2004
Pages
10
From page
1263
To page
1272
Abstract
There is considerable evidence implicating the cAMP-signaling pathway in the anabolic action of PTH; and to date, all PTH and PTHrp peptides that stimulate cyclic AMP are active in animal models of osteogenesis. We have tested two C-terminally truncated peptides, PTH(1–29) and a modified PTH(1–21) (MPTH(1–21)), in in vitro and in vivo assays of PTH action. Each of the C-terminally truncated peptides was of low nanomolar potency in assays of receptor binding and cAMP stimulation. However, when we tested these peptides for functional response in Saos-2 cells stably transfected with a cyclic AMP response element (CRE) reporter, the C-terminally truncated peptides were two to four times less potent than would be expected from their binding and cAMP-stimulating properties. Furthermore, PTH(1–29), although active, was approximately 20-fold less potent than PTH(1–34) in a rat model of osteogenesis while MPTH(1–21) was inactive. The relative lack of activity of these peptides in vivo suggests that while activation of the cAMP pathway may be important for the anabolic effect of PTH fragments, it is not, of itself, predictive of their in vivo activity.
Keywords
osteoblasts , PTH/PTHrP , G-protein signaling , CRE , bone mineral density
Journal title
Bone
Serial Year
2004
Journal title
Bone
Record number
495435
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