par Woussen Colle, Marie-Claire 
;Lingier, Pierre ;Vertongen, Pascale ;Vandermeers-Piret, Marie-Claire ;Vandermeers, André ;Robberecht, Patrick
Référence Peptides, 15, 5, page (869-874)
Publication Publié, 1994
;Lingier, Pierre ;Vertongen, Pascale ;Vandermeers-Piret, Marie-Claire ;Vandermeers, André ;Robberecht, Patrick Référence Peptides, 15, 5, page (869-874)
Publication Publié, 1994
Article révisé par les pairs
| Résumé : | A radioimmunoassay of human pancreastatin was developed using a rabbit antiserum that selectively recognized the C-terminal amidated end of the peptide, and it was used for the identification of the molecular forms of pancreastatin in human gut (stomach, duodenum, small intestine, colon) and endocrine tumor extracts (liver metastasis of a gastrinoma and a medullary carcinoma of thyroid, one nonsecreting pancreatic tumor, one recurrence of a gut carcinoid, one vipoma and one insulinoma). In all gut extracts, a gel filtration chromatography revealed the presence of three peaks of pancreastatin-like immunoreactivity. The predominant form eluted with an apparent molecular weight higher than that of pancreastatin. This form was also predominant in the endocrine tumors analyzed, except in the insulinoma, where a lower molecular weight form predominated. The high molecular form was further purified from a liver metastasis of a gastrinoma. The pancreastatin- like immunoreactivity eluted in all the chromatographical systems (reverse- phase, ion exchange) as a single peak that was finally purified to homogeneity and sequenced. The sequence of the first 29 N-terminal amino acids was obtained unambiguously and corresponded to the sequence 210-238 of chromogranin A. Considering the selectivity of the assay used for peptide identification, this major form was identified as the fragment 210-301 of chromogranin A. It is likely that the predominant form of pancreastatin in human gut extracts and noninsular tumors is a 92 amino acid peptide. |
