FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2009095670> ?p ?o ?g. }

• W2009095670 endingPage "912" @default.
• W2009095670 startingPage "905" @default.
• W2009095670 abstract "Cyclodextrins are cyclic oligosaccharides with the shape of a hollow truncated cone. Their exterior is hydrophilic and their cavity is hydrophobic, which gives cyclodextrins the ability to accommodate hydrophobic molecules/moieties in the cavity. This special molecular arrangement accounts for the variety of beneficial effects cyclodextrins have on proteins, which is widely used in pharmacological applications. We have studied the interaction between beta-cyclodextrin and four non-carbohydrate-binding model proteins: ubiquitin, chymotrypsin inhibitor 2 (CI2), S6 and insulin SerB9Asp by NMR spectroscopy at varying structural detail. We demonstrate that the interaction of beta-cyclodextrin and our model proteins takes place at specific sites on the protein surface, and that solvent accessibility of those sites is a necessary but not compelling condition for the occurrence of an interaction. If this behaviour can be generalized, it might explain the wide range of different effects of cyclodextrins on different proteins: aggregation suppression (if residues responsible for aggregation are highly solvent accessible), protection against degradation (if point of attack of a protease is sterically 'masked' by cyclodextrin), alteration of function (if residues involved in function are 'masked' by cyclodextrin). The exact effect of cyclodextrins on a given protein will always be related to the particular structure of this protein." @default.
• W2009095670 created "2016-06-24" @default.
• W2009095670 creator A5046625995 @default.
• W2009095670 creator A5055008207 @default.
• W2009095670 creator A5076002285 @default.
• W2009095670 creator A5081812332 @default.
• W2009095670 date "2003-12-01" @default.
• W2009095670 modified "2023-10-17" @default.
• W2009095670 title "Structural background of cyclodextrin-protein interactions" @default.
• W2009095670 cites W604100514 @default.
• W2009095670 doi "https://doi.org/10.1093/protein/gzg137" @default.
• W2009095670 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/14983070" @default.
• W2009095670 hasPublicationYear "2003" @default.
• W2009095670 type Work @default.
• W2009095670 sameAs 2009095670 @default.
• W2009095670 citedByCount "147" @default.
• W2009095670 countsByYear W20090956702012 @default.
• W2009095670 countsByYear W20090956702013 @default.
• W2009095670 countsByYear W20090956702014 @default.
• W2009095670 countsByYear W20090956702015 @default.
• W2009095670 countsByYear W20090956702016 @default.
• W2009095670 countsByYear W20090956702017 @default.
• W2009095670 countsByYear W20090956702018 @default.
• W2009095670 countsByYear W20090956702019 @default.
• W2009095670 countsByYear W20090956702020 @default.
• W2009095670 countsByYear W20090956702021 @default.
• W2009095670 countsByYear W20090956702022 @default.
• W2009095670 countsByYear W20090956702023 @default.
• W2009095670 crossrefType "journal-article" @default.
• W2009095670 hasAuthorship W2009095670A5046625995 @default.
• W2009095670 hasAuthorship W2009095670A5055008207 @default.
• W2009095670 hasAuthorship W2009095670A5076002285 @default.
• W2009095670 hasAuthorship W2009095670A5081812332 @default.
• W2009095670 hasBestOaLocation W20090956701 @default.
• W2009095670 hasConcept C12554922 @default.
• W2009095670 hasConcept C178790620 @default.
• W2009095670 hasConcept C185592680 @default.
• W2009095670 hasConcept C201194858 @default.
• W2009095670 hasConcept C2779433975 @default.
• W2009095670 hasConcept C32909587 @default.
• W2009095670 hasConcept C47701112 @default.
• W2009095670 hasConcept C55493867 @default.
• W2009095670 hasConcept C71240020 @default.
• W2009095670 hasConcept C86803240 @default.
• W2009095670 hasConcept C90260826 @default.
• W2009095670 hasConceptScore W2009095670C12554922 @default.
• W2009095670 hasConceptScore W2009095670C178790620 @default.
• W2009095670 hasConceptScore W2009095670C185592680 @default.
• W2009095670 hasConceptScore W2009095670C201194858 @default.
• W2009095670 hasConceptScore W2009095670C2779433975 @default.
• W2009095670 hasConceptScore W2009095670C32909587 @default.
• W2009095670 hasConceptScore W2009095670C47701112 @default.
• W2009095670 hasConceptScore W2009095670C55493867 @default.
• W2009095670 hasConceptScore W2009095670C71240020 @default.
• W2009095670 hasConceptScore W2009095670C86803240 @default.
• W2009095670 hasConceptScore W2009095670C90260826 @default.
• W2009095670 hasIssue "12" @default.
• W2009095670 hasLocation W20090956701 @default.
• W2009095670 hasLocation W20090956702 @default.
• W2009095670 hasOpenAccess W2009095670 @default.
• W2009095670 hasPrimaryLocation W20090956701 @default.
• W2009095670 hasRelatedWork W1558163028 @default.
• W2009095670 hasRelatedWork W1965238818 @default.
• W2009095670 hasRelatedWork W2009741933 @default.
• W2009095670 hasRelatedWork W2071122984 @default.
• W2009095670 hasRelatedWork W2090391251 @default.
• W2009095670 hasRelatedWork W2093532064 @default.
• W2009095670 hasRelatedWork W2615330267 @default.
• W2009095670 hasRelatedWork W3015752896 @default.
• W2009095670 hasRelatedWork W4294723901 @default.
• W2009095670 hasRelatedWork W4310690213 @default.
• W2009095670 hasVolume "16" @default.
• W2009095670 isParatext "false" @default.
• W2009095670 isRetracted "false" @default.
• W2009095670 magId "2009095670" @default.
• W2009095670 workType "article" @default.