FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2020256380> ?p ?o ?g. }

• W2020256380 endingPage "6568" @default.
• W2020256380 startingPage "6559" @default.
• W2020256380 abstract "Identity elements in tRNAs and the intracellular balance of tRNAs allow accurate selection of tRNAs by aminoacyl-tRNA synthetases. The histidyl-tRNA from Escherichia coli is distinguished by a unique G-1·C73 base pair that upon exchange with other nucleotides leads to a marked decrease in the rate of aminoacylation in vitro. G-1·C73 is also a major identity element for histidine acceptance, such that the substitution of C73 brings about mischarging by glycyl-, glutaminyl-, and leucyl-tRNA synthetases. These identity conversions mediated by the G-1·C73 base pair were exploited to isolate secondary site revertants in the histidyl-tRNA synthetase from E. coli which restore histidine identity to a histidyl-tRNA suppressor carrying U73. The revertant substitutions confer a 3−4-fold reduction in the Michaelis constant for tRNAs carrying the amber-suppressing anticodon and map to the C-terminal domain of HisRS and its interface with the catalytic core. These findings demonstrate that the histidine tRNA anticodon plays a significant role in tRNA selection in vivo and that the C-terminal domain of HisRS is in large part responsible for recognizing this trinucleotide. The kinetic parameters determined also show a small degree of anticooperativity (ΔΔG = −1.24 kcal/mol) between recognition of the discriminator base and the anticodon, suggesting that the two helical domains of the tRNA are not recognized independently. We propose that these effects substantially account for the ability of small changes in tRNA binding far removed from the site of a major determinant to bring about a complete conversion of tRNA identity." @default.
• W2020256380 created "2016-06-24" @default.
• W2020256380 creator A5023213072 @default.
• W2020256380 creator A5033892718 @default.
• W2020256380 creator A5079123564 @default.
• W2020256380 date "1996-01-01" @default.
• W2020256380 modified "2023-09-26" @default.
• W2020256380 title "A tRNA Identity Switch Mediated by the Binding Interaction between a tRNA Anticodon and the Accessory Domain of a Class II Aminoacyl-tRNA Synthetase" @default.
• W2020256380 cites W110138870 @default.
• W2020256380 cites W1562298896 @default.
• W2020256380 cites W1568949798 @default.
• W2020256380 cites W2003399248 @default.
• W2020256380 cites W2011604680 @default.
• W2020256380 cites W2083812890 @default.
• W2020256380 cites W2103947911 @default.
• W2020256380 cites W2110274263 @default.
• W2020256380 cites W2178012333 @default.
• W2020256380 cites W4213329868 @default.
• W2020256380 cites W4252889335 @default.
• W2020256380 doi "https://doi.org/10.1021/bi952889f" @default.
• W2020256380 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/8639604" @default.
• W2020256380 hasPublicationYear "1996" @default.
• W2020256380 type Work @default.
• W2020256380 sameAs 2020256380 @default.
• W2020256380 citedByCount "35" @default.
• W2020256380 countsByYear W20202563802012 @default.
• W2020256380 countsByYear W20202563802013 @default.
• W2020256380 countsByYear W20202563802016 @default.
• W2020256380 countsByYear W20202563802017 @default.
• W2020256380 countsByYear W20202563802018 @default.
• W2020256380 countsByYear W20202563802019 @default.
• W2020256380 countsByYear W20202563802021 @default.
• W2020256380 countsByYear W20202563802022 @default.
• W2020256380 countsByYear W20202563802023 @default.
• W2020256380 crossrefType "journal-article" @default.
• W2020256380 hasAuthorship W2020256380A5023213072 @default.
• W2020256380 hasAuthorship W2020256380A5033892718 @default.
• W2020256380 hasAuthorship W2020256380A5079123564 @default.
• W2020256380 hasConcept C104317684 @default.
• W2020256380 hasConcept C151238385 @default.
• W2020256380 hasConcept C153957851 @default.
• W2020256380 hasConcept C185581394 @default.
• W2020256380 hasConcept C185592680 @default.
• W2020256380 hasConcept C2778460671 @default.
• W2020256380 hasConcept C2779315393 @default.
• W2020256380 hasConcept C512185932 @default.
• W2020256380 hasConcept C515207424 @default.
• W2020256380 hasConcept C55493867 @default.
• W2020256380 hasConcept C67705224 @default.
• W2020256380 hasConcept C86803240 @default.
• W2020256380 hasConceptScore W2020256380C104317684 @default.
• W2020256380 hasConceptScore W2020256380C151238385 @default.
• W2020256380 hasConceptScore W2020256380C153957851 @default.
• W2020256380 hasConceptScore W2020256380C185581394 @default.
• W2020256380 hasConceptScore W2020256380C185592680 @default.
• W2020256380 hasConceptScore W2020256380C2778460671 @default.
• W2020256380 hasConceptScore W2020256380C2779315393 @default.
• W2020256380 hasConceptScore W2020256380C512185932 @default.
• W2020256380 hasConceptScore W2020256380C515207424 @default.
• W2020256380 hasConceptScore W2020256380C55493867 @default.
• W2020256380 hasConceptScore W2020256380C67705224 @default.
• W2020256380 hasConceptScore W2020256380C86803240 @default.
• W2020256380 hasIssue "21" @default.
• W2020256380 hasLocation W20202563801 @default.
• W2020256380 hasLocation W20202563802 @default.
• W2020256380 hasOpenAccess W2020256380 @default.
• W2020256380 hasPrimaryLocation W20202563801 @default.
• W2020256380 hasRelatedWork W1155189913 @default.
• W2020256380 hasRelatedWork W1812060039 @default.
• W2020256380 hasRelatedWork W1986670249 @default.
• W2020256380 hasRelatedWork W2000424976 @default.
• W2020256380 hasRelatedWork W2016599450 @default.
• W2020256380 hasRelatedWork W2023880708 @default.
• W2020256380 hasRelatedWork W2164783818 @default.
• W2020256380 hasRelatedWork W2467668492 @default.
• W2020256380 hasRelatedWork W2474878422 @default.
• W2020256380 hasRelatedWork W3023323281 @default.
• W2020256380 hasVolume "35" @default.
• W2020256380 isParatext "false" @default.
• W2020256380 isRetracted "false" @default.
• W2020256380 magId "2020256380" @default.
• W2020256380 workType "article" @default.