FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W1609043222> ?p ?o ?g. }

• W1609043222 endingPage "16937" @default.
• W1609043222 startingPage "16929" @default.
• W1609043222 abstract "Abstract Information on cation occlusion sites of renal NA,K-ATPase has been obtained by comparing the ability of competitive Na-like antagonists (David, P., Mayan, H., Cohen, H., Tal, D. M., and Karlish, S. J. D. (1992) J. Biol. Chem. 267, 1141-1149) with that of transported alkali metal cations to protect against covalent modification and structural perturbations of the protein. Sodium antagonists include p- or m-xylylenebisguanidium, guanidinium ions, and ethylenediamine. Experiments with proteoliposomes reconstituted with Na,K-ATPase demonstrate that p-xylylenebisguanidium has pronounced selectivity for the cytoplasmic surface. Tryptic digestion of Na,K-ATPase leading to membranes, a specifically truncated enzyme with intact cation occlusion sites, requires the presence of alkali metal cations. Sodium antagonists do not protect 19-kDa membranes against further digestion, and occlusion is destroyed. Incubation of 19-kDa membranes at 37 degrees C, in the absence of occluded ions, leads rapidly to loss of ability to occlude rubidium ions. Rubidium, sodium, or other alkali metal cations protect fully, whereas sodium antagonists do not protect against this thermal inactivation. Like the alkali metal cations, sodium antagonists protect Na,K-ATPase and, somewhat less effectively, 19-kDa membranes against inactivation by the carboxyl reagent N,N'-dicyclohexylcarbodiimide. Cation occlusion from the cytoplasmic surface is suggested to occur in two steps. In an initial recognition, either transported cations or sodium antagonists interact with carboxyl groups. The second step is selective for transported cations and involves occlusion of cations (either potassium or sodium ions) and a conformational change to a compact structure, which is resistant to proteolysis and thermal inactivation. Sodium antagonists are sterically hindered from becoming occluded and block Na,K-ATPase activity. Implications for the structural basis of cation specificity of the Na/K pump are discussed." @default.
• W1609043222 created "2016-06-24" @default.
• W1609043222 creator A5009248419 @default.
• W1609043222 creator A5015542036 @default.
• W1609043222 creator A5069829590 @default.
• W1609043222 creator A5075326442 @default.
• W1609043222 creator A5082141342 @default.
• W1609043222 date "1993-08-01" @default.
• W1609043222 modified "2023-09-27" @default.
• W1609043222 title "Effects of competitive sodium-like antagonists on Na,K-ATPase suggest that cation occlusion from the cytoplasmic surface occurs in two steps" @default.
• W1609043222 doi "https://doi.org/10.1016/s0021-9258(19)85284-5" @default.
• W1609043222 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/8394324" @default.
• W1609043222 hasPublicationYear "1993" @default.
• W1609043222 type Work @default.
• W1609043222 sameAs 1609043222 @default.
• W1609043222 citedByCount "40" @default.
• W1609043222 countsByYear W16090432222014 @default.
• W1609043222 countsByYear W16090432222021 @default.
• W1609043222 countsByYear W16090432222023 @default.
• W1609043222 crossrefType "journal-article" @default.
• W1609043222 hasAuthorship W1609043222A5009248419 @default.
• W1609043222 hasAuthorship W1609043222A5015542036 @default.
• W1609043222 hasAuthorship W1609043222A5069829590 @default.
• W1609043222 hasAuthorship W1609043222A5075326442 @default.
• W1609043222 hasAuthorship W1609043222A5082141342 @default.
• W1609043222 hasBestOaLocation W16090432221 @default.
• W1609043222 hasConcept C12554922 @default.
• W1609043222 hasConcept C178790620 @default.
• W1609043222 hasConcept C181199279 @default.
• W1609043222 hasConcept C185592680 @default.
• W1609043222 hasConcept C190062978 @default.
• W1609043222 hasConcept C23265538 @default.
• W1609043222 hasConcept C517785266 @default.
• W1609043222 hasConcept C537181965 @default.
• W1609043222 hasConcept C55493867 @default.
• W1609043222 hasConcept C86803240 @default.
• W1609043222 hasConceptScore W1609043222C12554922 @default.
• W1609043222 hasConceptScore W1609043222C178790620 @default.
• W1609043222 hasConceptScore W1609043222C181199279 @default.
• W1609043222 hasConceptScore W1609043222C185592680 @default.
• W1609043222 hasConceptScore W1609043222C190062978 @default.
• W1609043222 hasConceptScore W1609043222C23265538 @default.
• W1609043222 hasConceptScore W1609043222C517785266 @default.
• W1609043222 hasConceptScore W1609043222C537181965 @default.
• W1609043222 hasConceptScore W1609043222C55493867 @default.
• W1609043222 hasConceptScore W1609043222C86803240 @default.
• W1609043222 hasIssue "23" @default.
• W1609043222 hasLocation W16090432221 @default.
• W1609043222 hasOpenAccess W1609043222 @default.
• W1609043222 hasPrimaryLocation W16090432221 @default.
• W1609043222 hasRelatedWork W1974281891 @default.
• W1609043222 hasRelatedWork W1991837432 @default.
• W1609043222 hasRelatedWork W2001720881 @default.
• W1609043222 hasRelatedWork W2005610124 @default.
• W1609043222 hasRelatedWork W2026283032 @default.
• W1609043222 hasRelatedWork W2040359168 @default.
• W1609043222 hasRelatedWork W2071979626 @default.
• W1609043222 hasRelatedWork W2080227248 @default.
• W1609043222 hasRelatedWork W2468347786 @default.
• W1609043222 hasRelatedWork W2744854703 @default.
• W1609043222 hasVolume "268" @default.
• W1609043222 isParatext "false" @default.
• W1609043222 isRetracted "false" @default.
• W1609043222 magId "1609043222" @default.
• W1609043222 workType "article" @default.