FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4234025924> ?p ?o ?g. }

• W4234025924 endingPage "1215" @default.
• W4234025924 startingPage "1208" @default.
• W4234025924 abstract "To investigate whether hepatobiliary transport of organic cations is under regulatory control, we studied transport of tri-n-butylmethylammonium in the isolated perfused rat liver and in isolated rat hepatocytes. Transport was investigated in the presence of modulators of the protein kinase C and the cyclic AMP second-messenger system. In the isolated perfused rat liver, it was observed that compounds modulating protein kinase C activity clearly affected the biliary excretion process of the cation tri-n-butylmethylammonium. Phorbol 12-myristate 13-acetate, a compound that directly stimulates protein kinase C, elevated the biliary excretion rate of tri-n-butylmethylammonium in a concentration-dependent manner, reaching a twofold increase at 60 nmol/L of the phorbol ester. The inactive derivative 4α-phorbol 12, 13-didecanoate (60 nmol/L) did not show any effect. Vasopressin (48 nmol/L), a receptor-mediated activator of protein kinase C, stimulated the excretion rate of the cation by about 50%. Staurosporin (1 μmol/L), an inhibitor of protein kinase C, clearly decreased the biliary excretion rate of the cation and also blocked its stimulation by phorbol 12-myristate 13-acetate. Neither phorbol 12-myristate 13-acetate nor vasopressin (at concentrations ranging from 10−9 to 10−6 mol/L) affected the initial uptake velocity of tri-n-butylmethylammonium in isolated hepatocytes and isolated perfused livers, whereas staurosporin (1 μmol/L) showed only a modest inhibition of the uptake of the cation. It is inferred that the effect of protein kinase C modulators on hepatobiliary transport of organic cations occurs at the level of carrier-mediated transport in the canalicular membrane. Because bile flow was only slightly affected by these agents, effects on biliary excretion rate of the cation are unlikely to be caused by changes in bile flow. With regard to the cyclic AMP second-messenger system, neither glucagon (concentration range of 10−9 to 10−6 mol/L), a receptormediated activator of adenylate cyclase, nor forskolin (100 μmol/L), a direct activator of adenylate cyclase and dibutyryl cyclic AMP (100 μmol/L), affected the biliary excretion rate and the hepatic uptake rate of the cation in these preparations. In conclusion, cell-to-bile transport of the organic cation tri-n-butylmethylammonium at the canalicular level is directly or indirectly regulated by protein kinase C. Neither the protein kinase C nor the cyclic AMP second-messenger systems seem to be involved in the hepatic uptake process of the cation. (HEPATOLOGY 1993;18:1208-1215)." @default.
• W4234025924 created "2022-05-12" @default.
• W4234025924 creator A5005519092 @default.
• W4234025924 date "1993-11-01" @default.
• W4234025924 modified "2023-10-16" @default.
• W4234025924 title "Modulators of the protein kinase C system influence biliary excretion of cationic drugs" @default.
• W4234025924 doi "https://doi.org/10.1016/0270-9139(93)90479-7" @default.
• W4234025924 hasPublicationYear "1993" @default.
• W4234025924 type Work @default.
• W4234025924 citedByCount "2" @default.
• W4234025924 crossrefType "journal-article" @default.
• W4234025924 hasAuthorship W4234025924A5005519092 @default.
• W4234025924 hasBestOaLocation W42340259241 @default.
• W4234025924 hasConcept C10146269 @default.
• W4234025924 hasConcept C126322002 @default.
• W4234025924 hasConcept C134018914 @default.
• W4234025924 hasConcept C163235415 @default.
• W4234025924 hasConcept C170493617 @default.
• W4234025924 hasConcept C184235292 @default.
• W4234025924 hasConcept C185592680 @default.
• W4234025924 hasConcept C195794163 @default.
• W4234025924 hasConcept C2780043322 @default.
• W4234025924 hasConcept C55493867 @default.
• W4234025924 hasConcept C71924100 @default.
• W4234025924 hasConcept C86803240 @default.
• W4234025924 hasConcept C97029542 @default.
• W4234025924 hasConceptScore W4234025924C10146269 @default.
• W4234025924 hasConceptScore W4234025924C126322002 @default.
• W4234025924 hasConceptScore W4234025924C134018914 @default.
• W4234025924 hasConceptScore W4234025924C163235415 @default.
• W4234025924 hasConceptScore W4234025924C170493617 @default.
• W4234025924 hasConceptScore W4234025924C184235292 @default.
• W4234025924 hasConceptScore W4234025924C185592680 @default.
• W4234025924 hasConceptScore W4234025924C195794163 @default.
• W4234025924 hasConceptScore W4234025924C2780043322 @default.
• W4234025924 hasConceptScore W4234025924C55493867 @default.
• W4234025924 hasConceptScore W4234025924C71924100 @default.
• W4234025924 hasConceptScore W4234025924C86803240 @default.
• W4234025924 hasConceptScore W4234025924C97029542 @default.
• W4234025924 hasIssue "5" @default.
• W4234025924 hasLocation W42340259241 @default.
• W4234025924 hasOpenAccess W4234025924 @default.
• W4234025924 hasPrimaryLocation W42340259241 @default.
• W4234025924 hasRelatedWork W1940432453 @default.
• W4234025924 hasRelatedWork W1956062754 @default.
• W4234025924 hasRelatedWork W1978255802 @default.
• W4234025924 hasRelatedWork W2011584433 @default.
• W4234025924 hasRelatedWork W2025162880 @default.
• W4234025924 hasRelatedWork W2040646620 @default.
• W4234025924 hasRelatedWork W2068240886 @default.
• W4234025924 hasRelatedWork W2102581783 @default.
• W4234025924 hasRelatedWork W2131413156 @default.
• W4234025924 hasRelatedWork W2212096471 @default.
• W4234025924 hasVolume "18" @default.
• W4234025924 isParatext "false" @default.
• W4234025924 isRetracted "false" @default.
• W4234025924 workType "article" @default.