FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2080550653> ?p ?o ?g. }

• W2080550653 endingPage "218" @default.
• W2080550653 startingPage "217" @default.
• W2080550653 abstract "Thiolases belong to a superfamily of condensing enzymes that includes also β-ketoacyl acyl carrier protein synthases (KAS enzymes), involved in fatty acid synthesis. Here, we describe the high resolution structure of human cytosolic acetoacetyl-CoA thiolase (CT), both unliganded (at 2.3 Å resolution) and in complex with CoA (at 1.6 Å resolution). CT catalyses the condensation of two molecules of acetyl-CoA to acetoacetyl-CoA, which is the first reaction of the metabolic pathway leading to the synthesis of cholesterol. CT is a homotetramer of exact 222 symmetry. There is an excess of positively charged residues at the interdimer surface leading towards the CoA-binding pocket, possibly important for the efficient capture of substrates. The geometry of the catalytic site, including the three catalytic residues Cys92, His 353, Cys383, and the two oxyanion holes, is highly conserved between the human and bacterial Zoogloea ramigera thiolase. In human CT, the first oxyanion hole is formed by Wat38 (stabilised by Asn321) and NE2(His353), and the second by N(Cys92) and N(Gly385). The active site of this superfamily is constructed on top of four active site loops, near Cys92, Asn321, His353, and Cys383, respectively. These loops were used for the superpositioning of CT on the bacterial thiolase and on the Escherichia coli KAS I. This comparison indicates that the two thiolase oxyanion holes also exist in KAS I at topologically equivalent positions. Interestingly, the hydrogen bonding interactions at the first oxyanion hole are different in thiolase and KAS I. In KAS I, the hydrogen bonding partners are two histidine NE2 atoms, instead of a water and a NE2 side-chain atom in thiolase. The second oxyanion hole is in both structures shaped by corresponding main chain peptide NH-groups. The possible importance of bound water molecules at the catalytic site of thiolase for the reaction mechanism is discussed." @default.
• W2080550653 created "2016-06-24" @default.
• W2080550653 creator A5014069398 @default.
• W2080550653 creator A5014936646 @default.
• W2080550653 creator A5015898061 @default.
• W2080550653 creator A5025717497 @default.
• W2080550653 creator A5055064108 @default.
• W2080550653 creator A5057133785 @default.
• W2080550653 creator A5079948261 @default.
• W2080550653 creator A5087458476 @default.
• W2080550653 date "1996-08-01" @default.
• W2080550653 modified "2023-10-13" @default.
• W2080550653 title "Assignment of the Human Cytosolic Acetoacetyl-Coenzyme A Thiolase (ACAT2) Gene to Chromosome 6q25.3–q26" @default.
• W2080550653 doi "https://doi.org/10.1006/geno.1996.0452" @default.
• W2080550653 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/8812443" @default.
• W2080550653 hasPublicationYear "1996" @default.
• W2080550653 type Work @default.
• W2080550653 sameAs 2080550653 @default.
• W2080550653 citedByCount "9" @default.
• W2080550653 countsByYear W20805506532023 @default.
• W2080550653 crossrefType "journal-article" @default.
• W2080550653 hasAuthorship W2080550653A5014069398 @default.
• W2080550653 hasAuthorship W2080550653A5014936646 @default.
• W2080550653 hasAuthorship W2080550653A5015898061 @default.
• W2080550653 hasAuthorship W2080550653A5025717497 @default.
• W2080550653 hasAuthorship W2080550653A5055064108 @default.
• W2080550653 hasAuthorship W2080550653A5057133785 @default.
• W2080550653 hasAuthorship W2080550653A5079948261 @default.
• W2080550653 hasAuthorship W2080550653A5087458476 @default.
• W2080550653 hasConcept C161790260 @default.
• W2080550653 hasConcept C179506582 @default.
• W2080550653 hasConcept C181199279 @default.
• W2080550653 hasConcept C185592680 @default.
• W2080550653 hasConcept C2776317432 @default.
• W2080550653 hasConcept C2778934325 @default.
• W2080550653 hasConcept C2781031557 @default.
• W2080550653 hasConcept C41183919 @default.
• W2080550653 hasConcept C55493867 @default.
• W2080550653 hasConcept C71240020 @default.
• W2080550653 hasConcept C86803240 @default.
• W2080550653 hasConceptScore W2080550653C161790260 @default.
• W2080550653 hasConceptScore W2080550653C179506582 @default.
• W2080550653 hasConceptScore W2080550653C181199279 @default.
• W2080550653 hasConceptScore W2080550653C185592680 @default.
• W2080550653 hasConceptScore W2080550653C2776317432 @default.
• W2080550653 hasConceptScore W2080550653C2778934325 @default.
• W2080550653 hasConceptScore W2080550653C2781031557 @default.
• W2080550653 hasConceptScore W2080550653C41183919 @default.
• W2080550653 hasConceptScore W2080550653C55493867 @default.
• W2080550653 hasConceptScore W2080550653C71240020 @default.
• W2080550653 hasConceptScore W2080550653C86803240 @default.
• W2080550653 hasFunder F4320309785 @default.
• W2080550653 hasFunder F4320320912 @default.
• W2080550653 hasFunder F4320321945 @default.
• W2080550653 hasIssue "1" @default.
• W2080550653 hasLocation W20805506531 @default.
• W2080550653 hasLocation W20805506532 @default.
• W2080550653 hasOpenAccess W2080550653 @default.
• W2080550653 hasPrimaryLocation W20805506531 @default.
• W2080550653 hasRelatedWork W1963907668 @default.
• W2080550653 hasRelatedWork W2007976176 @default.
• W2080550653 hasRelatedWork W2013364636 @default.
• W2080550653 hasRelatedWork W2033283984 @default.
• W2080550653 hasRelatedWork W2051709886 @default.
• W2080550653 hasRelatedWork W2059997198 @default.
• W2080550653 hasRelatedWork W2073351880 @default.
• W2080550653 hasRelatedWork W2080550653 @default.
• W2080550653 hasRelatedWork W2323800439 @default.
• W2080550653 hasRelatedWork W2570206517 @default.
• W2080550653 hasVolume "36" @default.
• W2080550653 isParatext "false" @default.
• W2080550653 isRetracted "false" @default.
• W2080550653 magId "2080550653" @default.
• W2080550653 workType "article" @default.