Plasma clearance, tissue uptake and expression of pituitary peptide 23/pancreatitis-associated protein in the rat

in Journal of Endocrinology
Authors:
C Chakraborty
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S Sharma
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N Katsumata
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L J Murphy
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I C Schroedter
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M C Robertson
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R P C Shiu
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H G Friesen
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DOI:
https://doi.org/10.1677/joe.0.1450461
Volume/Issue:
Volume 145: Issue 3
Article Type:
Research Article
Page Range:
461–469
Online Publication Date:
Jun 1995
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Abstract

The secretion of peptide 23 by rat pituitary cells is stimulated by growth hormone-releasing hormone and inhibited by somatostatin. Recent cloning of the cognate cDNA for peptide 23 revealed that it is identical to pancreatitis-associated protein (PAP). In the present study, the clearance and tissue uptake of recombinant peptide 23/PAP in normal adult male rats was assessed. The plasma half-life of recombinant peptide 23/PAP was 4·8 ±1·4 (s.d.) min. Maximal accumulation of radiolabelled peptide 23/PAP was observed in the kidney, stomach, small intestine and pancreas whereas negligible uptake was seen in the liver, lung or heart. Peptide 23/PAP was detected in a variety of tissue extracts using a radioimmunoassay. Extracts of ileum contained the highest concentrations of peptide 23/PAP. In situ hybridization analysis showed that peptide 23/PAP mRNA was highly expressed in the columnar epithelial cells of ileum, jejunum and duodenum. These observations demonstrate that peptide 23/PAP, a protein previously thought to be of pituitary origin, is widely expressed in the gastrointestinal tract and that it is rapidly removed from the circulation by the kidney and by tissues which express peptide 23/PAP.

Journal of Endocrinology (1995) 145, 461–469

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Print ISSN:
0022-0795
Online ISSN:
1479-6805
Page(s):
9
Article Type:
Research Article
Print Publication Date:
01 Jan 1995
Online Publication Date:
Jun 1995