Cysteamine-induced Duodenal Ulcer and Acid Secretion in the Rat

Kirkegaard, Preben; Poulsen, Steen Seier; Loud, F. B.; Halse, C; Christiansen, John

doi:10.3109/00365528009182225

Cited by 68 publications

(29 citation statements)

References 9 publications

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“…In contrast to with the low dose, the accumulation of gastric contents in response to the high dose of cysteamine gradually in creased, the maximum being reached at 6 hr. Since a delay in gastric emptying was already evident 1 hr after administration, this gradual accumulation appears to be due to the gradual stimulation of gastric acid secretion, as re ported by other authors (21). The maximal volume and amount of acid with the high dose of cysteamine were almost double those with the high dose of mepirizole.…”

Section: Discussionsupporting

confidence: 50%

The relationship of intraduodenal pH and delayed gastric emptying in duodenal ulceration induced by mepirizole or cysteamine in rats.

1989

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Section: Discussionsupporting

confidence: 50%

The relationship of intraduodenal pH and delayed gastric emptying in duodenal ulceration induced by mepirizole or cysteamine in rats.

1989

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“…4 The dose required, however, is 700 to 1000 mg/kg body weight or 40 to 60 times the per-kilogram body weight dose that is currently administered at any one time for the treatment of cystinosis. 1,[5][6][7] The exact mechanism by which cysteamine induces ulcerogenesis is unclear, but it likely involves gastric acid-hypersecretion 6,18 secondary to hypergastrinemia. 19 Low intraluminal pH will inhibit gastrin release through a negative feedback loop.…”

Section: Discussionmentioning

confidence: 99%

The evaluation and treatment of gastrointestinal disease in children with cystinosis receiving cysteamine

Dohil

Newbury

Sellers

et al. 2003

The Journal of Pediatrics

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Objectives Cysteamine prevents organ damage in children with cystinosis, but may cause gastrointestinal (GI) symptoms.In this study we evaluated the nature of GI disease, and the value of omeprazole in controlling GI symptoms in these children.Study design Upper GI disease was evaluated with endoscopy, gastrin levels, and acid secretion studies after oral administration of cysteamine, before and after 16 weeks of therapy with omeprazole. A symptom score was devised.Results Eleven children (mean age, 5.7 years) were studied. After cysteamine ingestion, before and after omeprazole therapy, the mean maximum acid output was significantly higher than the mean basal acid output. The maximum acid output was measured within 60 minutes of cysteamine ingestion and was reduced by omeprazole therapy (P < .01). The mean peak gastrin level was 30 minutes postcysteamine and was higher than baseline (P < .01). The initial mean symptom score (maximum score, 14) was 6.9 and fell to 0.7 (P < .0001) after 16 weeks of omeprazole therapy. At endoscopy, two children had diffuse gastric nodularity, and nearly all had cystine crystal deposits.Conclusions GI symptoms in children with cystinosis receiving cysteamine are often acid-mediated and improve with omeprazole. Cystine crystals were detected in the GI tract and may signify inadequate treatment with cysteamine. (J Pediatr 2003;143:224-30)

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“…This finding is consistent with the observations by other investigators (9) who reported the development of microscopic damage in rat duodenal epithelium 4 to 8 hr after administration of cysteamine (280 mg/ kg, p.o.). From various laboratories (22)(23)(24)(25)(26)(27) it was reported that cysteamine at the ulcerogenic dose significantly increased gastric H+ secretion within 1-4 hr in acute or chronic fistula rats, thereby suggesting the close link of increased gastric secretion in the pathogenesis. We also found that cysteamine (100 mg/kg) increased gastric H+ output by about 2-fold of the control values beginning from 2 hr after administration for the following 2 hr.…”

Section: Discussionmentioning

confidence: 99%

Effects of Indomethacin on the Duodenal Mucosa of Rats: Comparative Study with Cysteamine

Tanaka¹,

Ueki²,

Takeuchi³

et al. 1986

Japanese Journal of Pharmacology

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Abstract-Effects of indomethacin and cysteamine on the duodenal mucosa of rats were studied microscopically (using scanning electron microscopy) and also functionally.Indomethacin (5 mg/kg, s.c.) induced no microscopic damage to the duodenal epithelium for up to 6 hr after administration.Indomethacin had no effects on gastric H+ output and the amount of H+ in the duodenum, but did reduce the duodenal HCO3 secretion (both basal and 10 mM-HCI stimulated). PGE2 contents in the duodenal mucosa were markedly reduced by indomethacin for 6 hr. These results suggest that reductions of duodenal HCO3 secretion and endogenous prostaglandins per se do not impair the H+ disposal system of the duodenum and so do not damage the epithelial cells. In contrast, cysteamine (100 mg/kg, s.c.) produced microscopic damage to the duodenal epithelium as early as 2 hr later. Cysteamine significantly increased gastric H+ output and reduced duodenal HC03 secretion, resulting in an increased amount of H+ in the duodenum 3 hr later. Cysteamine had no effect on PGE2 contents in the duodenum. The time lag between damage formation and functional changes suggests that the earliest damage caused by cysteamine occurs by mechanisms other than erosive action of H+ emptied by the stomach.The increased amount of H+ may contribute to an enhancement of the initial damage.

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Cysteamine-induced Duodenal Ulcer and Acid Secretion in the Rat

Cited by 68 publications

References 9 publications

The relationship of intraduodenal pH and delayed gastric emptying in duodenal ulceration induced by mepirizole or cysteamine in rats.

The relationship of intraduodenal pH and delayed gastric emptying in duodenal ulceration induced by mepirizole or cysteamine in rats.

The evaluation and treatment of gastrointestinal disease in children with cystinosis receiving cysteamine

Effects of Indomethacin on the Duodenal Mucosa of Rats: Comparative Study with Cysteamine

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