Stimulation by Prostaglandin E_2 of Alkaline Secretion in the Rat Duodenum

Possible involvement of increased mucosal permeability in the stimulation by prostaglandin E_2 (PGE_2 ) of duodenal HCO_3 ^- secretion was investigated in rats. PGE_2 (0.3, 1 mg/kg. s.c.) dose-dependently increased HCO_3 ^- secretion in the duodenum with a significant elevation of transmucosal poten...

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Published in:Japanese Journal of Pharmacology 1990, Vol.53 (1), p.67-74
Main Authors: Koji TAKEUCHI, Hiromichi NIIDA, Yusuke TAKINAMI, Susumu OKABE
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container_title Japanese Journal of Pharmacology
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creator Koji TAKEUCHI
Hiromichi NIIDA
Yusuke TAKINAMI
Susumu OKABE
description Possible involvement of increased mucosal permeability in the stimulation by prostaglandin E_2 (PGE_2 ) of duodenal HCO_3 ^- secretion was investigated in rats. PGE_2 (0.3, 1 mg/kg. s.c.) dose-dependently increased HCO_3 ^- secretion in the duodenum with a significant elevation of transmucosal potential difference (PD); the PD was increased from -4.5±0.3 mV to -10.0±1.5 mV (mucosa negative) at 1 mg/kg. These responses caused by PGE_2 were abolished by sacrificing the animals with saturated KCI (i.v.). Although a significant increase of HCO_3 ^- output was observed after exposure of the mucosa to 1 M NaCI (0.5 ml), this response was accompanied by a significant reduction of PD and was not abolished after KCI injection. The mucosal permeability determined by Evans blue (1%, i.v.) was not affected by PGE_2 , while 1 M NaCI markedly elevated the amount of extravasated dye in both the luminal content and the mucosa. Stimulation of H COj output by PGE_2 was significantly mitigated by ouabain (3 mg/kg, s.c.) or prior exposure of the mucosa to 1 M NaCI. These results suggest that stimulation by PGE_2 of duodenal HCO_3 ^- secretion is not simply due to the increased mucosal permeability, but depends rather on both the Na/K ATPase activity and the intact perfusion of the organ. The HCO_3 ^- response as induced by 1 M NaCI may result from the increased permeability and is accompanied by a marked reduction of PD.
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PGE_2 (0.3, 1 mg/kg. s.c.) dose-dependently increased HCO_3 ^- secretion in the duodenum with a significant elevation of transmucosal potential difference (PD); the PD was increased from -4.5±0.3 mV to -10.0±1.5 mV (mucosa negative) at 1 mg/kg. These responses caused by PGE_2 were abolished by sacrificing the animals with saturated KCI (i.v.). Although a significant increase of HCO_3 ^- output was observed after exposure of the mucosa to 1 M NaCI (0.5 ml), this response was accompanied by a significant reduction of PD and was not abolished after KCI injection. The mucosal permeability determined by Evans blue (1%, i.v.) was not affected by PGE_2 , while 1 M NaCI markedly elevated the amount of extravasated dye in both the luminal content and the mucosa. Stimulation of H COj output by PGE_2 was significantly mitigated by ouabain (3 mg/kg, s.c.) or prior exposure of the mucosa to 1 M NaCI. These results suggest that stimulation by PGE_2 of duodenal HCO_3 ^- secretion is not simply due to the increased mucosal permeability, but depends rather on both the Na/K ATPase activity and the intact perfusion of the organ. The HCO_3 ^- response as induced by 1 M NaCI may result from the increased permeability and is accompanied by a marked reduction of PD.</description><identifier>ISSN: 0021-5198</identifier><language>jpn</language><publisher>The Japanese Pharmacological Society</publisher><ispartof>Japanese Journal of Pharmacology, 1990, Vol.53 (1), p.67-74</ispartof><woscitedreferencessubscribed>false</woscitedreferencessubscribed></display><links><openurl>$$Topenurl_article</openurl><openurlfulltext>$$Topenurlfull_article</openurlfulltext><thumbnail>$$Tsyndetics_thumb_exl</thumbnail><link.rule.ids>314,780,784,4024</link.rule.ids></links><search><creatorcontrib>Koji TAKEUCHI</creatorcontrib><creatorcontrib>Hiromichi NIIDA</creatorcontrib><creatorcontrib>Yusuke TAKINAMI</creatorcontrib><creatorcontrib>Susumu OKABE</creatorcontrib><creatorcontrib>Kyoto Pharmaceutical University</creatorcontrib><creatorcontrib>Department of Applied Pharmacology</creatorcontrib><title>Stimulation by Prostaglandin E_2 of Alkaline Secretion in the Rat Duodenum</title><title>Japanese Journal of Pharmacology</title><description>Possible involvement of increased mucosal permeability in the stimulation by prostaglandin E_2 (PGE_2 ) of duodenal HCO_3 ^- secretion was investigated in rats. PGE_2 (0.3, 1 mg/kg. s.c.) dose-dependently increased HCO_3 ^- secretion in the duodenum with a significant elevation of transmucosal potential difference (PD); the PD was increased from -4.5±0.3 mV to -10.0±1.5 mV (mucosa negative) at 1 mg/kg. These responses caused by PGE_2 were abolished by sacrificing the animals with saturated KCI (i.v.). Although a significant increase of HCO_3 ^- output was observed after exposure of the mucosa to 1 M NaCI (0.5 ml), this response was accompanied by a significant reduction of PD and was not abolished after KCI injection. The mucosal permeability determined by Evans blue (1%, i.v.) was not affected by PGE_2 , while 1 M NaCI markedly elevated the amount of extravasated dye in both the luminal content and the mucosa. Stimulation of H COj output by PGE_2 was significantly mitigated by ouabain (3 mg/kg, s.c.) or prior exposure of the mucosa to 1 M NaCI. These results suggest that stimulation by PGE_2 of duodenal HCO_3 ^- secretion is not simply due to the increased mucosal permeability, but depends rather on both the Na/K ATPase activity and the intact perfusion of the organ. 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PGE_2 (0.3, 1 mg/kg. s.c.) dose-dependently increased HCO_3 ^- secretion in the duodenum with a significant elevation of transmucosal potential difference (PD); the PD was increased from -4.5±0.3 mV to -10.0±1.5 mV (mucosa negative) at 1 mg/kg. These responses caused by PGE_2 were abolished by sacrificing the animals with saturated KCI (i.v.). Although a significant increase of HCO_3 ^- output was observed after exposure of the mucosa to 1 M NaCI (0.5 ml), this response was accompanied by a significant reduction of PD and was not abolished after KCI injection. The mucosal permeability determined by Evans blue (1%, i.v.) was not affected by PGE_2 , while 1 M NaCI markedly elevated the amount of extravasated dye in both the luminal content and the mucosa. Stimulation of H COj output by PGE_2 was significantly mitigated by ouabain (3 mg/kg, s.c.) or prior exposure of the mucosa to 1 M NaCI. These results suggest that stimulation by PGE_2 of duodenal HCO_3 ^- secretion is not simply due to the increased mucosal permeability, but depends rather on both the Na/K ATPase activity and the intact perfusion of the organ. The HCO_3 ^- response as induced by 1 M NaCI may result from the increased permeability and is accompanied by a marked reduction of PD.</abstract><pub>The Japanese Pharmacological Society</pub></addata></record>
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title Stimulation by Prostaglandin E_2 of Alkaline Secretion in the Rat Duodenum
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