FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2004632004> ?p ?o ?g. }

• W2004632004 endingPage "13547" @default.
• W2004632004 startingPage "13538" @default.
• W2004632004 abstract "Multisubstrate adduct inhibitors (MAI) of glycinamide ribonucleotide transformylase (GAR Tfase), which incorporate key features of the folate cofactor and the beta-GAR substrate, typically exhibit K(i)'s in the picomolar range. However, these compounds have reduced bioavailability due to the incorporation of a negatively charged phosphate moiety that prevents effective cellular uptake. Thus, a folate analogue that is capable of adduct formation with the substrate on the enzyme active site could lead to a potent GAR Tfase inhibitor that takes advantage of the cellular folate transport systems. We synthesized a dibromide folate analogue, 10-bromo-10-bromomethyl-5,8,10-trideazafolic acid, that was an intermediate designed to assemble with the substrate beta-GAR on the enzyme active site. We have now determined the crystal structure of the Escherichia coli GAR Tfase/MAI complex at 1.6 A resolution to ascertain the nature and mechanism of its time-dependent inhibition. The high-resolution crystal structure clearly revealed the existence of a covalent adduct between the substrate beta-GAR and the folate analogue (K(i) = 20 microM). However, the electron density map surprisingly indicated a C10 hydroxyl in the adduct rather than a bromide and suggested that the multisubstrate adduct is not formed directly from the dibromide but proceeds via an epoxide. Subsequently, we demonstrated the in situ conversion of the dibromide to the epoxide. Moreover, synthesis of the authentic epoxide confirmed that its inhibitory, time-dependent, and cytotoxic properties are comparable to those of the dibromide. Further, inhibition was strongest when the dibromide or epoxide is preincubated with both enzyme and substrate, indicating that inhibition occurs via the enzyme-dependent formation of the multisubstrate adduct. Thus, the crystal structure revealed the successful formation of an enzyme-assembled multisubstrate adduct and highlighted a potential application for epoxides, and perhaps aziridines, in the design of efficacious GAR Tfase inhibitors." @default.
• W2004632004 created "2016-06-24" @default.
• W2004632004 creator A5010315360 @default.
• W2004632004 creator A5030990841 @default.
• W2004632004 creator A5044664321 @default.
• W2004632004 creator A5049235255 @default.
• W2004632004 creator A5056100384 @default.
• W2004632004 creator A5057047461 @default.
• W2004632004 creator A5078373008 @default.
• W2004632004 date "2001-10-18" @default.
• W2004632004 modified "2023-09-30" @default.
• W2004632004 title "Unexpected Formation of an Epoxide-Derived Multisubstrate Adduct Inhibitor on the Active Site of GAR Transformylase^," @default.
• W2004632004 doi "https://doi.org/10.1021/bi011482+" @default.
• W2004632004 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/11695901" @default.
• W2004632004 hasPublicationYear "2001" @default.
• W2004632004 type Work @default.
• W2004632004 sameAs 2004632004 @default.
• W2004632004 citedByCount "37" @default.
• W2004632004 countsByYear W20046320042012 @default.
• W2004632004 countsByYear W20046320042013 @default.
• W2004632004 countsByYear W20046320042015 @default.
• W2004632004 countsByYear W20046320042018 @default.
• W2004632004 countsByYear W20046320042023 @default.
• W2004632004 crossrefType "journal-article" @default.
• W2004632004 hasAuthorship W2004632004A5010315360 @default.
• W2004632004 hasAuthorship W2004632004A5030990841 @default.
• W2004632004 hasAuthorship W2004632004A5044664321 @default.
• W2004632004 hasAuthorship W2004632004A5049235255 @default.
• W2004632004 hasAuthorship W2004632004A5056100384 @default.
• W2004632004 hasAuthorship W2004632004A5057047461 @default.
• W2004632004 hasAuthorship W2004632004A5078373008 @default.
• W2004632004 hasConcept C108204754 @default.
• W2004632004 hasConcept C111368507 @default.
• W2004632004 hasConcept C127313418 @default.
• W2004632004 hasConcept C161790260 @default.
• W2004632004 hasConcept C178790620 @default.
• W2004632004 hasConcept C181199279 @default.
• W2004632004 hasConcept C185592680 @default.
• W2004632004 hasConcept C197957613 @default.
• W2004632004 hasConcept C2776920199 @default.
• W2004632004 hasConcept C2777289219 @default.
• W2004632004 hasConcept C41183919 @default.
• W2004632004 hasConcept C55493867 @default.
• W2004632004 hasConcept C71240020 @default.
• W2004632004 hasConceptScore W2004632004C108204754 @default.
• W2004632004 hasConceptScore W2004632004C111368507 @default.
• W2004632004 hasConceptScore W2004632004C127313418 @default.
• W2004632004 hasConceptScore W2004632004C161790260 @default.
• W2004632004 hasConceptScore W2004632004C178790620 @default.
• W2004632004 hasConceptScore W2004632004C181199279 @default.
• W2004632004 hasConceptScore W2004632004C185592680 @default.
• W2004632004 hasConceptScore W2004632004C197957613 @default.
• W2004632004 hasConceptScore W2004632004C2776920199 @default.
• W2004632004 hasConceptScore W2004632004C2777289219 @default.
• W2004632004 hasConceptScore W2004632004C41183919 @default.
• W2004632004 hasConceptScore W2004632004C55493867 @default.
• W2004632004 hasConceptScore W2004632004C71240020 @default.
• W2004632004 hasIssue "45" @default.
• W2004632004 hasLocation W20046320041 @default.
• W2004632004 hasLocation W20046320042 @default.
• W2004632004 hasOpenAccess W2004632004 @default.
• W2004632004 hasPrimaryLocation W20046320041 @default.
• W2004632004 hasRelatedWork W1550634984 @default.
• W2004632004 hasRelatedWork W1996022521 @default.
• W2004632004 hasRelatedWork W1997428826 @default.
• W2004632004 hasRelatedWork W2004632004 @default.
• W2004632004 hasRelatedWork W2010596396 @default.
• W2004632004 hasRelatedWork W2042011564 @default.
• W2004632004 hasRelatedWork W2071763012 @default.
• W2004632004 hasRelatedWork W2249621633 @default.
• W2004632004 hasRelatedWork W3022531063 @default.
• W2004632004 hasRelatedWork W3095664373 @default.
• W2004632004 hasVolume "40" @default.
• W2004632004 isParatext "false" @default.
• W2004632004 isRetracted "false" @default.
• W2004632004 magId "2004632004" @default.
• W2004632004 workType "article" @default.