Stereospecific Inhibition by Naloxone of Histamine-Stimulated Acid Secretion in Isolated Guinea Pig Parietal Cells

Kromer, W.; Schröder, Peter; Netz, Susanne

doi:10.1159/000138031

Cited by 6 publications

(3 citation statements)

References 22 publications

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“…However, in rat (Schepp & Ruoff, 1984) and human (Miederer et al 1986) parietal cells the effects of glucagon and histamine on adenylate cyclase activity were additive. Glucagon did not increase aminopyrine accumulation in rat parietal cells (Schepp & Ruoff, 1984 (Kromer, Schroder & Netz, 1984;Schepp, Schneider, Schusdziarra & Classen, 1986). The effects of these opioid peptides were blocked by (-)naloxone.…”

Section: Glucagon and Related Peptides?mentioning

confidence: 79%

“…Opioid peptides? D-Ala2-D-leu5-enkephalin and met-enkephalin produced a small enhancement of histamine-stimulated aminopyrine accumulation in parietai cells from guinea-pig and rat (Kromer, Schroder & Netz, 1984;Schepp, Schneider, Schusdziarra & Classen, 1986). The effects of these opioid peptides were blocked by (-)naloxone.…”

Section: Glucagon and Related Peptides?mentioning

confidence: 93%

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Intracellular Signalling and Regulation of Gastric Acid Secretion

Hanson

Hatt

1989

Exp Physiol

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Section: Glucagon and Related Peptides?mentioning

confidence: 79%

Section: Glucagon and Related Peptides?mentioning

confidence: 93%

Intracellular Signalling and Regulation of Gastric Acid Secretion

Hanson

Hatt

1989

Exp Physiol

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“…This might be an expression of the general distress (including marked re spiratory depression) manifested by the ani mals given these elevated doses of opioids; 20% of the rats died, in fact, with the com bined treatment of ulcerating solutions and opioids. However, bearing in mind the con tradictory literature on the effects of opioids even in the stomach [7][8][9][10], the possibility of a biphasic effect of opioids, linked to the size of dose, cannot be excluded.…”

Section: Discussionmentioning

confidence: 99%

Protection by Opioids against Gastric Lesions Caused by Necrotizing Agents

Ferri

Speroni²,

Candeletti³

et al. 1988

Pharmacology

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The synthetic opioid met-enkephalin analog [D-Ala², MePhe⁴, Met(0)⁵ol] enkephalin (DAMME) and the opiate morphine injected intraperitoneally to rats at doses of 0.5–2 and 5–20 mg/kg, respectively, showed a protective effect on gastric damage induced by oral administration of necrotizing agents (0.6 NHCl or 0.2 NNaOH solutions, 1 ml/rat). The protection was prevented by naltrexone (10 mg/kg s.c), an opioid antagonist with long-lasting activity. Histological sections of mucosal samples from animals pretreated with morphine (10 mg/kg i.p.) and DAMME (1 mg/kg i.p.) showed less alteration of the columnar epithelium, with a normal glandular structure, than untreated rats. A mediation of prostaglandins is suggested, since indomethacin (10 mg/kg s.c.) significantly reduced the protective effects of opioids.

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Opioid Peptides of The Gut

Miller

Hirning

1989

Comprehensive Physiology

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Stereospecific Inhibition by Naloxone of Histamine-Stimulated Acid Secretion in Isolated Guinea Pig Parietal Cells

Cited by 6 publications

References 22 publications

Intracellular Signalling and Regulation of Gastric Acid Secretion

Intracellular Signalling and Regulation of Gastric Acid Secretion

Protection by Opioids against Gastric Lesions Caused by Necrotizing Agents

Opioid Peptides of The Gut

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