FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2041948289> ?p ?o ?g. }

• W2041948289 endingPage "1698" @default.
• W2041948289 startingPage "1689" @default.
• W2041948289 abstract "Metaphit, an acylating derivative of phencyclidine, was shown to interact with components of the dopamine nerve terminal in rat striatal tissue. This compound, previously demonstrated to be an irreversible inhibitor at the phencyclidine receptor, was shown in these experiments to irreversibly inhibit synaptosomal [3H]dopamine uptake. It also inhibited binding of [3H]methylphenidate to its recognition site, which is thought to be a subunit of the dopamine transporter. Although the inhibition was due primarily to a reduction in the binding and transport capacity of the systems studied, increases in the apparent KD of [3H]methylphenidate and the Km of [3H]dopamine were also observed. Differences in the behavior of Metaphit and phencyclidine in these dopaminergic systems compared to their effects on the NMDA receptor-linked phencyclidine receptor suggest that Metaphit may be interacting with two distinct molecular sites in the rat striatum." @default.
• W2041948289 created "2016-06-24" @default.
• W2041948289 creator A5007922126 @default.
• W2041948289 creator A5016293600 @default.
• W2041948289 creator A5065225959 @default.
• W2041948289 creator A5072565784 @default.
• W2041948289 date "1989-01-01" @default.
• W2041948289 modified "2023-10-18" @default.
• W2041948289 title "Metaphit inhibits dopamine transport and binding of [3H] methylphenidate, a proposed marker for the dopamine transport complex" @default.
• W2041948289 cites W1979921554 @default.
• W2041948289 cites W1987164572 @default.
• W2041948289 cites W2003970221 @default.
• W2041948289 cites W2018493169 @default.
• W2041948289 cites W2043813981 @default.
• W2041948289 cites W2055598466 @default.
• W2041948289 cites W2071463736 @default.
• W2041948289 cites W2086858015 @default.
• W2041948289 cites W2090996446 @default.
• W2041948289 cites W2095526078 @default.
• W2041948289 cites W2120363902 @default.
• W2041948289 cites W2168551001 @default.
• W2041948289 doi "https://doi.org/10.1016/0024-3205(89)90279-8" @default.
• W2041948289 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/2586226" @default.
• W2041948289 hasPublicationYear "1989" @default.
• W2041948289 type Work @default.
• W2041948289 sameAs 2041948289 @default.
• W2041948289 citedByCount "12" @default.
• W2041948289 crossrefType "journal-article" @default.
• W2041948289 hasAuthorship W2041948289A5007922126 @default.
• W2041948289 hasAuthorship W2041948289A5016293600 @default.
• W2041948289 hasAuthorship W2041948289A5065225959 @default.
• W2041948289 hasAuthorship W2041948289A5072565784 @default.
• W2041948289 hasConcept C118552586 @default.
• W2041948289 hasConcept C120069818 @default.
• W2041948289 hasConcept C120750228 @default.
• W2041948289 hasConcept C12554922 @default.
• W2041948289 hasConcept C137183658 @default.
• W2041948289 hasConcept C15744967 @default.
• W2041948289 hasConcept C169760540 @default.
• W2041948289 hasConcept C170493617 @default.
• W2041948289 hasConcept C185592680 @default.
• W2041948289 hasConcept C2776755682 @default.
• W2041948289 hasConcept C2777112843 @default.
• W2041948289 hasConcept C2778851735 @default.
• W2041948289 hasConcept C2780062018 @default.
• W2041948289 hasConcept C2780783007 @default.
• W2041948289 hasConcept C2909816965 @default.
• W2041948289 hasConcept C513476851 @default.
• W2041948289 hasConcept C55493867 @default.
• W2041948289 hasConcept C67018056 @default.
• W2041948289 hasConcept C86803240 @default.
• W2041948289 hasConcept C98274493 @default.
• W2041948289 hasConceptScore W2041948289C118552586 @default.
• W2041948289 hasConceptScore W2041948289C120069818 @default.
• W2041948289 hasConceptScore W2041948289C120750228 @default.
• W2041948289 hasConceptScore W2041948289C12554922 @default.
• W2041948289 hasConceptScore W2041948289C137183658 @default.
• W2041948289 hasConceptScore W2041948289C15744967 @default.
• W2041948289 hasConceptScore W2041948289C169760540 @default.
• W2041948289 hasConceptScore W2041948289C170493617 @default.
• W2041948289 hasConceptScore W2041948289C185592680 @default.
• W2041948289 hasConceptScore W2041948289C2776755682 @default.
• W2041948289 hasConceptScore W2041948289C2777112843 @default.
• W2041948289 hasConceptScore W2041948289C2778851735 @default.
• W2041948289 hasConceptScore W2041948289C2780062018 @default.
• W2041948289 hasConceptScore W2041948289C2780783007 @default.
• W2041948289 hasConceptScore W2041948289C2909816965 @default.
• W2041948289 hasConceptScore W2041948289C513476851 @default.
• W2041948289 hasConceptScore W2041948289C55493867 @default.
• W2041948289 hasConceptScore W2041948289C67018056 @default.
• W2041948289 hasConceptScore W2041948289C86803240 @default.
• W2041948289 hasConceptScore W2041948289C98274493 @default.
• W2041948289 hasIssue "18" @default.
• W2041948289 hasLocation W20419482891 @default.
• W2041948289 hasLocation W20419482892 @default.
• W2041948289 hasOpenAccess W2041948289 @default.
• W2041948289 hasPrimaryLocation W20419482891 @default.
• W2041948289 hasRelatedWork W1538801892 @default.
• W2041948289 hasRelatedWork W1592902933 @default.
• W2041948289 hasRelatedWork W1608908265 @default.
• W2041948289 hasRelatedWork W2026302172 @default.
• W2041948289 hasRelatedWork W2031008496 @default.
• W2041948289 hasRelatedWork W2041948289 @default.
• W2041948289 hasRelatedWork W2312661926 @default.
• W2041948289 hasRelatedWork W2689471436 @default.
• W2041948289 hasRelatedWork W3175711477 @default.
• W2041948289 hasRelatedWork W40745602 @default.
• W2041948289 hasVolume "45" @default.
• W2041948289 isParatext "false" @default.
• W2041948289 isRetracted "false" @default.
• W2041948289 magId "2041948289" @default.
• W2041948289 workType "article" @default.