1hb0: Difference between revisions
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[[Category: serine proteinase]] | [[Category: serine proteinase]] | ||
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Revision as of 17:28, 5 November 2007
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SNAPSHOTS OF SERINE PROTEASE CATALYSIS: (D) ACYL-ENZYME INTERMEDIATE BETWEEN PORCINE PANCREATIC ELASTASE AND HUMAN BETA-CASOMORPHIN-7 JUMPED TO PH 10 FOR 2 MINUTES
OverviewOverview
Studies on the catalytic mechanism and inhibition of serine proteases are, widely used as paradigms for teaching enzyme catalysis. Ground-breaking, work on the structures of chymotrypsin and subtilisin led to the idea of a, conserved catalytic triad formed by the active site Ser, His and Asp, residues. An oxyanion hole, consisting of the peptide amide of the active, site serine and a neighbouring glycine, was identified, and hydrogen, bonding in the oxyanion hole was suggested to stabilize the two proposed, tetrahedral intermediates on the catalytic pathway. Here we show electron, density changes consistent with the formation of a tetrahedral, intermediate during the hydrolysis of an acyl-enzyme complex formed, between a natural heptapeptide and elastase. No electron density for an, enzyme-product complex was observed. The structures also suggest a, mechanism for the synchronization of hydrolysis and peptide release, triggered by the conversion of the sp2 hybridized carbonyl carbon to an, sp3 carbon in the tetrahedral intermediate. This affects the location of, the peptide in the active site cleft, triggering the collapse of a, hydrogen bonding network between the peptide and the beta-sheet of the, active site.
About this StructureAbout this Structure
1HB0 is a Single protein structure of sequence from Sus scrofa with CA and SO4 as ligands. Active as Transferred entry: 3.4.21.36, with EC number 3.4.21.11 Structure known Active Site: CAT. Full crystallographic information is available from OCA.
ReferenceReference
X-ray snapshots of serine protease catalysis reveal a tetrahedral intermediate., Wilmouth RC, Edman K, Neutze R, Wright PA, Clifton IJ, Schneider TR, Schofield CJ, Hajdu J, Nat Struct Biol. 2001 Aug;8(8):689-94. PMID:11473259
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