Pentadecapeptide BPC 157, cimetidine, ranitidine, bromocriptine, and atropine effect in cysteamine lesions in totally gastrectromized rats : A model for cytoprotective studies

Pentadecapeptide BPC 157, cimetidine, ranitidine, bromocriptine, and atropine effect in cysteamine lesions in totally gastrectromized rats : A model for cytoprotective studies

A superior effectiveness in various lesion assays was noted for the novel pentadecapeptide BPC 157, originated from human gastric juice protein (BPC) and claimed to be a cytoprotective agent. From this viewpoint, as a previously untreated experimental improvement to create an acid-free environmental...

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Veröffentlicht in:Digestive diseases and sciences 1997-05, Vol.42 (5), p.1029-1037
Hauptverfasser: SIKIRIC, P, MIKUS, D, ZORICIC, I, PERIC, J, KONJEVODA, P, PEROVIC, D, JURINA, L, HANZEVACKI, M, SEPAROVIC, J, GJURASIN, M, JADRIJEVIC, S, JELOVAC, N, SEIWERTH, S, MIKLIC, P, BULJAT, G, MAROVIC, A, GRABAREVIC, Z, RUCMAN, R, PETEK, M, JAGIC, V, TURKOVIC, B, ROTKVIC, I, MISE, S
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Anti-Ulcer Agents - pharmacology
Atropine - pharmacology
Biological and medical sciences
Bromocriptine - pharmacology
Cimetidine - pharmacology
Cysteamine - toxicity
Digestive system
Duodenal Ulcer - chemically induced
Duodenal Ulcer - prevention & control
Female
Gastrectomy
Medical sciences
Omeprazole - pharmacology
Peptide Fragments - pharmacology
Pharmacology. Drug treatments
Proteins - pharmacology
Ranitidine - pharmacology
Rats
Rats, Wistar
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Zusammenfassung:A superior effectiveness in various lesion assays was noted for the novel pentadecapeptide BPC 157, originated from human gastric juice protein (BPC) and claimed to be a cytoprotective agent. From this viewpoint, as a previously untreated experimental improvement to create an acid-free environmental for cytoprotection studies, total gastrectomy was done 24 hr before the ulcerogenic procedure. In the absence of stomach and gastric acid, the damaging effects of cysteamine (400 mg/kg subcutaneously, death 24 hr thereafter), to date thought to be an acid-related duodenal ulcerogen, and the BPC 157 cytoprotective effect (10 microg or 10 ng/kg intraperitoneally) were further challenged. BPC 157 was compared with reference agents [cimetidine (50), ranitidine (10), omeprazole (10), bromocriptine (10) and atropine (10) (mg/kg intraperitoneally, 1 hr before cysteamine] known to be also cytoprotective. In naive rats, with intact stomach, all of them showed a strong beneficial effect. Interestingly, in gastrectomized animals, the application of BPC 157 or the reference agents before cysteamine significantly prevented the otherwise severe duodenal lesion development noted in the control gastrectomized cysteamine rats. In groups without cysteamine, no lesions were noted (laparotomy, gastrectomy only, 24 or 48 hr postsurgical period), nor was lesion potentiation seen in cysteamine-treated laparotomized animals. In summary, these findings--equal damaging effect of cysteamine and equal protection of pentadecapeptide BPC 157 and reference agents in gastrectomized and rats with intact stomach--seem to be particularly relevant for a cytoprotective viewpoint. Without a stomach, the cysteamine damaging effect was convincingly defined as an essential gastric acid-independent injury (analogous to ethanol gastric lesions). Likewise, a high "cytoprotective capacity," apparently acid independent, common for all tested agents (novel pentadecapeptide BPC 157, cimetidine, ranitidine, omeprazole and atropine) could be clearly stressed.
ISSN:0163-2116
1573-2568
DOI:10.1023/A:1018893220943