FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W320653501> ?p ?o ?g. }

• W320653501 abstract "The non-steroid anti-inflammatory drugs inhibit cyclo-oxygenase and therefore the biosynthesis of prostaglandins, and it has been proposed that this biochemical intervention is the basis not only of their therapeutic activity but also contributes to their gastrointestinal side-effects. Since endogenous prostaglandins may exert mucosal protective actions, inhibition of cyclo-oxygenase by aspirin-like drugs would be expected to lead to gastric damage. The clinically-used anti-inflammatory compounds reduce prostaglandin levels in the experimental inflammatory exudate, but also inhibit prostacyclin formation in gastric tissue and induce gastric damage. In contrast, anti-inflammatory doses of sodium salicylate and an experimental drug BW755C (3-amino-1m-(trifluoromethyl)-phenyl-2-pyrazoline) fail to inhibit gastric mucosal prostacyclin formation (but do reduce prostaglandin levels in the inflammatory exudate) and cause only minimal gastric damage, supporting the relationship between production of gastric erosions and the inhibition of mucosal prostacyclin production. Anti-inflammatory doses of BW755C also fail to inhibit prostaglandin formation in the small intestine. Furthermore, studies on homogenates of gastric mucosa and ileum show that sodium salicylate, paracetamol and BW755C are only weak inhibitors of gastric mucosal cyclo-oxygenase in vitro. The development of nonsteroid anti-rheumatic drugs which have minimal action on prostaglandin production by the gastro-intestinal tract and exhibit reduced gastrointestinal toxicity, thus appears to be a feasible proposition." @default.
• W320653501 created "2016-06-24" @default.
• W320653501 creator A5059382959 @default.
• W320653501 creator A5066244229 @default.
• W320653501 date "1984-01-01" @default.
• W320653501 modified "2023-10-17" @default.
• W320653501 title "A Biochemical Basis for the Gastrointestinal Toxicity of Non-steroid Antirheumatoid Drugs" @default.
• W320653501 cites W1606919860 @default.
• W320653501 cites W1615012936 @default.
• W320653501 cites W1968795152 @default.
• W320653501 cites W1971804850 @default.
• W320653501 cites W1976592336 @default.
• W320653501 cites W1980197284 @default.
• W320653501 cites W2008574207 @default.
• W320653501 cites W2021623724 @default.
• W320653501 cites W2030111072 @default.
• W320653501 cites W2041735424 @default.
• W320653501 cites W2045428552 @default.
• W320653501 cites W2054229509 @default.
• W320653501 cites W2059903366 @default.
• W320653501 cites W2090746672 @default.
• W320653501 cites W2144821133 @default.
• W320653501 cites W2173164476 @default.
• W320653501 cites W2331956767 @default.
• W320653501 cites W2407170352 @default.
• W320653501 cites W2415650039 @default.
• W320653501 cites W3150791457 @default.
• W320653501 cites W4301042056 @default.
• W320653501 cites W4319694 @default.
• W320653501 doi "https://doi.org/10.1007/978-3-642-69132-4_54" @default.
• W320653501 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/6440513" @default.
• W320653501 hasPublicationYear "1984" @default.
• W320653501 type Work @default.
• W320653501 sameAs 320653501 @default.
• W320653501 citedByCount "48" @default.
• W320653501 countsByYear W3206535012012 @default.
• W320653501 countsByYear W3206535012016 @default.
• W320653501 countsByYear W3206535012018 @default.
• W320653501 crossrefType "book-chapter" @default.
• W320653501 hasAuthorship W320653501A5059382959 @default.
• W320653501 hasAuthorship W320653501A5066244229 @default.
• W320653501 hasConcept C185592680 @default.
• W320653501 hasConcept C2777628954 @default.
• W320653501 hasConcept C2779134981 @default.
• W320653501 hasConcept C2779422922 @default.
• W320653501 hasConcept C2780664492 @default.
• W320653501 hasConcept C2781128415 @default.
• W320653501 hasConcept C2781443798 @default.
• W320653501 hasConcept C55493867 @default.
• W320653501 hasConcept C71924100 @default.
• W320653501 hasConcept C98274493 @default.
• W320653501 hasConceptScore W320653501C185592680 @default.
• W320653501 hasConceptScore W320653501C2777628954 @default.
• W320653501 hasConceptScore W320653501C2779134981 @default.
• W320653501 hasConceptScore W320653501C2779422922 @default.
• W320653501 hasConceptScore W320653501C2780664492 @default.
• W320653501 hasConceptScore W320653501C2781128415 @default.
• W320653501 hasConceptScore W320653501C2781443798 @default.
• W320653501 hasConceptScore W320653501C55493867 @default.
• W320653501 hasConceptScore W320653501C71924100 @default.
• W320653501 hasConceptScore W320653501C98274493 @default.
• W320653501 hasLocation W3206535011 @default.
• W320653501 hasLocation W3206535012 @default.
• W320653501 hasOpenAccess W320653501 @default.
• W320653501 hasPrimaryLocation W3206535011 @default.
• W320653501 hasRelatedWork W1489354008 @default.
• W320653501 hasRelatedWork W1968795152 @default.
• W320653501 hasRelatedWork W2011946737 @default.
• W320653501 hasRelatedWork W2021120688 @default.
• W320653501 hasRelatedWork W2089221066 @default.
• W320653501 hasRelatedWork W2112293469 @default.
• W320653501 hasRelatedWork W2217019466 @default.
• W320653501 hasRelatedWork W2420775688 @default.
• W320653501 hasRelatedWork W320653501 @default.
• W320653501 hasRelatedWork W2183249986 @default.
• W320653501 isParatext "false" @default.
• W320653501 isRetracted "false" @default.
• W320653501 magId "320653501" @default.
• W320653501 workType "book-chapter" @default.