FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2061429027> ?p ?o ?g. }

• W2061429027 endingPage "S15" @default.
• W2061429027 startingPage "S10" @default.
• W2061429027 abstract "Protein sequencing and molecular cloning of human endothelial angiotensin I-converting enzyme (ACE; kininase II), have led to a description of the structure of the enzyme and to several questions concerning the intracellular maturation of ACE and the mechanisms of enzyme action. With the help of recombinant ACE expression in mammalian cells and site-directed mutagenesis, a model for the maturation of ACE in endothelial cells has been proposed. This model comprises transmembrane anchoring of the membrane-bound ACE near its carboxyterminal extremity, and post-translational cleavage of the anchor in the secreted form. The endothelial ACE displays a high degree of internal homology between two large peptidic domains that each bears a consensus sequence for zinc binding and therefore a putative active site. The testicular ACE, however, encoded from the same gene by a shorter mRNA, contains only the carboxyterminal half of endothelial ACE and therefore a single active site. Expression of ACE mutants with only one intact homologous domain, however, indicates that in endothelial ACE both domains are enzymatically active. Further characterization of these two active sites of endothelial ACE is in progress. In humans, population studies have indicated that the large interindividual variability in plasma ACE levels is partly genetically determined and under the influence of a major gene effect. This was later confirmed and extended by the observation of an insertion-deletion polymorphism of the ACE gene that is associated with the level of ACE in plasma. The clinical implications of these observations are discussed." @default.
• W2061429027 created "2016-06-24" @default.
• W2061429027 creator A5023912786 @default.
• W2061429027 creator A5033263108 @default.
• W2061429027 creator A5046945534 @default.
• W2061429027 creator A5056794570 @default.
• W2061429027 creator A5086893621 @default.
• W2061429027 date "1992-01-01" @default.
• W2061429027 modified "2023-10-12" @default.
• W2061429027 title "The Angiotensin I–Converting Enzyme (Kininase II): Molecular Organization and Regulation of Its Expression in Humans" @default.
• W2061429027 doi "https://doi.org/10.1097/00005344-199200209-00004" @default.
• W2061429027 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/1282623" @default.
• W2061429027 hasPublicationYear "1992" @default.
• W2061429027 type Work @default.
• W2061429027 sameAs 2061429027 @default.
• W2061429027 citedByCount "28" @default.
• W2061429027 countsByYear W20614290272013 @default.
• W2061429027 countsByYear W20614290272018 @default.
• W2061429027 countsByYear W20614290272021 @default.
• W2061429027 countsByYear W20614290272022 @default.
• W2061429027 crossrefType "journal-article" @default.
• W2061429027 hasAuthorship W2061429027A5023912786 @default.
• W2061429027 hasAuthorship W2061429027A5033263108 @default.
• W2061429027 hasAuthorship W2061429027A5046945534 @default.
• W2061429027 hasAuthorship W2061429027A5056794570 @default.
• W2061429027 hasAuthorship W2061429027A5086893621 @default.
• W2061429027 hasBestOaLocation W20614290271 @default.
• W2061429027 hasConcept C104317684 @default.
• W2061429027 hasConcept C134018914 @default.
• W2061429027 hasConcept C143065580 @default.
• W2061429027 hasConcept C153911025 @default.
• W2061429027 hasConcept C170493617 @default.
• W2061429027 hasConcept C181199279 @default.
• W2061429027 hasConcept C185592680 @default.
• W2061429027 hasConcept C27016395 @default.
• W2061429027 hasConcept C2779611605 @default.
• W2061429027 hasConcept C2908929049 @default.
• W2061429027 hasConcept C40767141 @default.
• W2061429027 hasConcept C55493867 @default.
• W2061429027 hasConcept C84393581 @default.
• W2061429027 hasConcept C86803240 @default.
• W2061429027 hasConceptScore W2061429027C104317684 @default.
• W2061429027 hasConceptScore W2061429027C134018914 @default.
• W2061429027 hasConceptScore W2061429027C143065580 @default.
• W2061429027 hasConceptScore W2061429027C153911025 @default.
• W2061429027 hasConceptScore W2061429027C170493617 @default.
• W2061429027 hasConceptScore W2061429027C181199279 @default.
• W2061429027 hasConceptScore W2061429027C185592680 @default.
• W2061429027 hasConceptScore W2061429027C27016395 @default.
• W2061429027 hasConceptScore W2061429027C2779611605 @default.
• W2061429027 hasConceptScore W2061429027C2908929049 @default.
• W2061429027 hasConceptScore W2061429027C40767141 @default.
• W2061429027 hasConceptScore W2061429027C55493867 @default.
• W2061429027 hasConceptScore W2061429027C84393581 @default.
• W2061429027 hasConceptScore W2061429027C86803240 @default.
• W2061429027 hasIssue "Supplement 9" @default.
• W2061429027 hasLocation W20614290271 @default.
• W2061429027 hasLocation W20614290272 @default.
• W2061429027 hasLocation W20614290273 @default.
• W2061429027 hasOpenAccess W2061429027 @default.
• W2061429027 hasPrimaryLocation W20614290271 @default.
• W2061429027 hasRelatedWork W1865915409 @default.
• W2061429027 hasRelatedWork W1983513268 @default.
• W2061429027 hasRelatedWork W1986920602 @default.
• W2061429027 hasRelatedWork W2006771406 @default.
• W2061429027 hasRelatedWork W2016628627 @default.
• W2061429027 hasRelatedWork W2064042198 @default.
• W2061429027 hasRelatedWork W2167664552 @default.
• W2061429027 hasRelatedWork W2365370541 @default.
• W2061429027 hasRelatedWork W2372340362 @default.
• W2061429027 hasRelatedWork W214510971 @default.
• W2061429027 hasVolume "20" @default.
• W2061429027 isParatext "false" @default.
• W2061429027 isRetracted "false" @default.
• W2061429027 magId "2061429027" @default.
• W2061429027 workType "article" @default.