FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4256343498> ?p ?o ?g. }

• W4256343498 endingPage "551" @default.
• W4256343498 startingPage "545" @default.
• W4256343498 abstract "Results from our molecular-modelling and site-directed-mutagenesis studies of prostaglandin I2 synthase (PGIS) have suggested that the large PGIS cytoplasmic domain is anchored to the endoplasmic reticulum (ER) membrane by the N-terminal segment in a way that orients the substrate access channel opening to face the membrane. To test this hypothesis we have explored the accessibility of the PGIS substrate channel opening to site-specific antibodies. The working three-dimensional PGIS model constructed by protein homology modelling was used to predict surface portions near the substrate access channel opening. Two peptides corresponding to the surface immediately near the opening [residues 66–75 (P66–75) and 95–116 (P95–116)], and two other peptides corresponding to the surface about 10–20Å (1Å = 0.1nm) away from the opening [residues 366–382 (P366–382) and 472–482 (P472–482)] were used to prepare site-specific antibodies. All four antipeptide antibodies specifically recognized the synthetic segments of human PGIS and recombinant PGIS, as shown by binding assays and Western-blot analysis. The site-specific antibodies were used to probe the accessibility of the substrate access channel opening in transiently transfected COS-1 cells expressing recombinant human PGIS, and in spontaneously transformed human endothelial cell line ECV cells expressing endogenous human PGIS. Immunofluorescence staining was performed for cells selectively permeabilized with streptolysin O and for cells whose membranes were permeabilized with detergent. Antibodies to peptides in the immediate vicinity of the substrate channel (P66–75 and P95–116) bound to their targets only after general permeabilization with Triton X-100. In contrast, the two antibodies to peptides further from the channel opening (P366–382 and P472–482) bound to their targets even in cells with intact ER membranes. These observations support our topology model in which the PGIS substrate access channel opening is positioned close to the ER membrane." @default.
• W4256343498 created "2022-05-12" @default.
• W4256343498 creator A5007140739 @default.
• W4256343498 creator A5020742387 @default.
• W4256343498 creator A5037384824 @default.
• W4256343498 creator A5050570624 @default.
• W4256343498 creator A5082400787 @default.
• W4256343498 date "2002-03-08" @default.
• W4256343498 modified "2023-09-30" @default.
• W4256343498 title "Substrate access channel topology in membrane-bound prostacyclin synthase" @default.
• W4256343498 doi "https://doi.org/10.1042/bj3620545" @default.
• W4256343498 hasPublicationYear "2002" @default.
• W4256343498 type Work @default.
• W4256343498 citedByCount "17" @default.
• W4256343498 countsByYear W42563434982013 @default.
• W4256343498 countsByYear W42563434982014 @default.
• W4256343498 countsByYear W42563434982017 @default.
• W4256343498 countsByYear W42563434982019 @default.
• W4256343498 countsByYear W42563434982021 @default.
• W4256343498 crossrefType "journal-article" @default.
• W4256343498 hasAuthorship W4256343498A5007140739 @default.
• W4256343498 hasAuthorship W4256343498A5020742387 @default.
• W4256343498 hasAuthorship W4256343498A5037384824 @default.
• W4256343498 hasAuthorship W4256343498A5050570624 @default.
• W4256343498 hasAuthorship W4256343498A5082400787 @default.
• W4256343498 hasConcept C104317684 @default.
• W4256343498 hasConcept C107824862 @default.
• W4256343498 hasConcept C12554922 @default.
• W4256343498 hasConcept C153911025 @default.
• W4256343498 hasConcept C158617107 @default.
• W4256343498 hasConcept C185592680 @default.
• W4256343498 hasConcept C190062978 @default.
• W4256343498 hasConcept C40767141 @default.
• W4256343498 hasConcept C41625074 @default.
• W4256343498 hasConcept C54009773 @default.
• W4256343498 hasConcept C55493867 @default.
• W4256343498 hasConcept C86803240 @default.
• W4256343498 hasConceptScore W4256343498C104317684 @default.
• W4256343498 hasConceptScore W4256343498C107824862 @default.
• W4256343498 hasConceptScore W4256343498C12554922 @default.
• W4256343498 hasConceptScore W4256343498C153911025 @default.
• W4256343498 hasConceptScore W4256343498C158617107 @default.
• W4256343498 hasConceptScore W4256343498C185592680 @default.
• W4256343498 hasConceptScore W4256343498C190062978 @default.
• W4256343498 hasConceptScore W4256343498C40767141 @default.
• W4256343498 hasConceptScore W4256343498C41625074 @default.
• W4256343498 hasConceptScore W4256343498C54009773 @default.
• W4256343498 hasConceptScore W4256343498C55493867 @default.
• W4256343498 hasConceptScore W4256343498C86803240 @default.
• W4256343498 hasIssue "3" @default.
• W4256343498 hasLocation W42563434981 @default.
• W4256343498 hasOpenAccess W4256343498 @default.
• W4256343498 hasPrimaryLocation W42563434981 @default.
• W4256343498 hasRelatedWork W2359239772 @default.
• W4256343498 hasRelatedWork W2363386379 @default.
• W4256343498 hasRelatedWork W2367323167 @default.
• W4256343498 hasRelatedWork W2371820180 @default.
• W4256343498 hasRelatedWork W2372736349 @default.
• W4256343498 hasRelatedWork W2373978809 @default.
• W4256343498 hasRelatedWork W2392841809 @default.
• W4256343498 hasRelatedWork W2394282857 @default.
• W4256343498 hasRelatedWork W2394425474 @default.
• W4256343498 hasRelatedWork W3028757768 @default.
• W4256343498 hasVolume "362" @default.
• W4256343498 isParatext "false" @default.
• W4256343498 isRetracted "false" @default.
• W4256343498 workType "article" @default.