FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2086706656> ?p ?o ?g. }

• W2086706656 endingPage "355" @default.
• W2086706656 startingPage "353" @default.
• W2086706656 abstract "Thymidine phosphorylase (TP; EC 2.4.2.4) catalyzes the reversible phosphorolysis of thymidine, deoxyuridine, and their analogues to their respective nucleobases and 2-deoxy-α-d-ribose-1-phosphate (dRib-1-P). TP is a key enzyme in the pyrimidine salvage pathways. Activity of the enzyme is crucial in angiogenesis, cancer chemotherapy, radiotherapy, and tumor imaging, Nevertheless, a complete set of kinetic parameters has never been reported for any human TP. This study describes the kinetic mechanism and regulation of native human hepatic TP. The liver is a main site of pyrimidine metabolism and contains high levels of TP. Initial velocity and product inhibition studies demonstrated that the basic mechanism of this enzyme is a sequential random bi-bi mechanism. Initial velocity studies showed an intersecting pattern, consistent with substrate-enzyme-co-substrate complex formation, and a binding pattern indicating that the binding of the substrate interferes with the binding of the co-substrate and vice versa. Estimated kinetic parameters were KThymidine = 284 ± 55, KPi = 5.8 ± 1.9, KThymine = 244 ± 69, and KdRib-1-P = 90 ± 33 μM. Thymine was a product activator, but becomes a substrate inhibitor at concentrations eight times higher than its Km. dRib-1-P was a non-competitive product inhibitor of the forward reaction. It bounded better to the Enzyme●Pi complex than the free enzyme, but had better affinity to the free enzyme than the Enzyme●Thymidine complex. In the reverse reaction, dRib-1-P enhanced the binding of thymine. The enhancement of the thymine binding along with the fact that dRib-1-P was a non-competitive product inhibitor suggests the presence of another binding site for dRib-1-P on the enzyme." @default.
• W2086706656 created "2016-06-24" @default.
• W2086706656 creator A5021638873 @default.
• W2086706656 creator A5029451572 @default.
• W2086706656 date "1988-01-01" @default.
• W2086706656 modified "2023-10-17" @default.
• W2086706656 title "Thymidine phosphorylase in human epidermal keratinocytes" @default.
• W2086706656 cites W1974384202 @default.
• W2086706656 cites W1977972494 @default.
• W2086706656 cites W1979767153 @default.
• W2086706656 cites W2003519607 @default.
• W2086706656 cites W2019251285 @default.
• W2086706656 cites W2027559664 @default.
• W2086706656 cites W2047439512 @default.
• W2086706656 cites W2072618321 @default.
• W2086706656 cites W2088360956 @default.
• W2086706656 cites W2089709035 @default.
• W2086706656 cites W2137972697 @default.
• W2086706656 cites W2333924917 @default.
• W2086706656 cites W4293247451 @default.
• W2086706656 doi "https://doi.org/10.1016/0006-2952(88)90740-x" @default.
• W2086706656 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/2449215" @default.
• W2086706656 hasPublicationYear "1988" @default.
• W2086706656 type Work @default.
• W2086706656 sameAs 2086706656 @default.
• W2086706656 citedByCount "23" @default.
• W2086706656 countsByYear W20867066562013 @default.
• W2086706656 countsByYear W20867066562014 @default.
• W2086706656 countsByYear W20867066562018 @default.
• W2086706656 countsByYear W20867066562019 @default.
• W2086706656 crossrefType "journal-article" @default.
• W2086706656 hasAuthorship W2086706656A5021638873 @default.
• W2086706656 hasAuthorship W2086706656A5029451572 @default.
• W2086706656 hasConcept C181199279 @default.
• W2086706656 hasConcept C185592680 @default.
• W2086706656 hasConcept C18903297 @default.
• W2086706656 hasConcept C2776476023 @default.
• W2086706656 hasConcept C2776735402 @default.
• W2086706656 hasConcept C2776858809 @default.
• W2086706656 hasConcept C2777108182 @default.
• W2086706656 hasConcept C2777289219 @default.
• W2086706656 hasConcept C2777648924 @default.
• W2086706656 hasConcept C2779321679 @default.
• W2086706656 hasConcept C552990157 @default.
• W2086706656 hasConcept C55493867 @default.
• W2086706656 hasConcept C71240020 @default.
• W2086706656 hasConcept C71615608 @default.
• W2086706656 hasConcept C86803240 @default.
• W2086706656 hasConceptScore W2086706656C181199279 @default.
• W2086706656 hasConceptScore W2086706656C185592680 @default.
• W2086706656 hasConceptScore W2086706656C18903297 @default.
• W2086706656 hasConceptScore W2086706656C2776476023 @default.
• W2086706656 hasConceptScore W2086706656C2776735402 @default.
• W2086706656 hasConceptScore W2086706656C2776858809 @default.
• W2086706656 hasConceptScore W2086706656C2777108182 @default.
• W2086706656 hasConceptScore W2086706656C2777289219 @default.
• W2086706656 hasConceptScore W2086706656C2777648924 @default.
• W2086706656 hasConceptScore W2086706656C2779321679 @default.
• W2086706656 hasConceptScore W2086706656C552990157 @default.
• W2086706656 hasConceptScore W2086706656C55493867 @default.
• W2086706656 hasConceptScore W2086706656C71240020 @default.
• W2086706656 hasConceptScore W2086706656C71615608 @default.
• W2086706656 hasConceptScore W2086706656C86803240 @default.
• W2086706656 hasIssue "2" @default.
• W2086706656 hasLocation W20867066561 @default.
• W2086706656 hasLocation W20867066562 @default.
• W2086706656 hasOpenAccess W2086706656 @default.
• W2086706656 hasPrimaryLocation W20867066561 @default.
• W2086706656 hasRelatedWork W1907637722 @default.
• W2086706656 hasRelatedWork W1968380675 @default.
• W2086706656 hasRelatedWork W1974384202 @default.
• W2086706656 hasRelatedWork W1978158489 @default.
• W2086706656 hasRelatedWork W1979845990 @default.
• W2086706656 hasRelatedWork W2072400918 @default.
• W2086706656 hasRelatedWork W2081084085 @default.
• W2086706656 hasRelatedWork W2093680570 @default.
• W2086706656 hasRelatedWork W2367338326 @default.
• W2086706656 hasRelatedWork W91031534 @default.
• W2086706656 hasVolume "37" @default.
• W2086706656 isParatext "false" @default.
• W2086706656 isRetracted "false" @default.
• W2086706656 magId "2086706656" @default.
• W2086706656 workType "article" @default.