Possible mechanisms contributing to oxidative inactivation of activated protein C: molecular dynamics study
Activated protein C (APC) is a serine protease, an effector enzyme of the natural anticoagulant pathway. APC is approved for treatment of severe sepsis characterized by the increased concentrations of H(2)O(2) and hypochlorite. We found that treatment of APC with these oxidants markedly inhibits the...
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| Published in | Thrombosis and haemostasis Vol. 100; no. 1; p. 18 |
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| Main Authors | , |
| Format | Journal Article |
| Language | English |
| Published |
Germany
01.07.2008
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| Subjects | |
| Online Access | Get more information |
| ISSN | 0340-6245 |
| DOI | 10.1160/TH07-12-0750 |
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| Abstract | Activated protein C (APC) is a serine protease, an effector enzyme of the natural anticoagulant pathway. APC is approved for treatment of severe sepsis characterized by the increased concentrations of H(2)O(2) and hypochlorite. We found that treatment of APC with these oxidants markedly inhibits the cleavage of the APC-specific chromogenic substrate, suggesting that oxidants can induce changes in the structure of the active site of APC. Resistance of oxidant-treated APC to chemical digestion with cyanogen bromide (CNBr) implies that methionine oxidation can at least in part be responsible for inhibition of APC. Since methionine residues, the main targets of oxidants in APC, are not included in the active site, we hypothesize that oxidation induces allosteric changes in the architecture of the catalytic triad of APC. Using molecular dynamics (MD) simulations we found that methionine oxidation alters the distance between cSer195Ogamma and cHis57Nepsilon2 atoms placing them in positions unfavorable for the catalysis. At the same time, neither distances between Calpha atoms of the catalytic triad cAsp102-cHis57-cSer195, nor the overall structure of APC changed significantly after oxidation of the methionine residues. Disruption of the H-bond between Ndelta1 of cHis57 and carboxyl group of cAsp102, which can take place during the hypochlorite-induced modification of cHis57, dramatically changed the architecture of the catalytic triad in oxidized APC. This mechanism could contribute to APC inactivation by hypochlorite concurrently with methionine oxidation. These are novel findings, which describe potentially pathophysiologically relevant changes in the functional stability of APC exposed to the oxidative stress. |
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| AbstractList | Activated protein C (APC) is a serine protease, an effector enzyme of the natural anticoagulant pathway. APC is approved for treatment of severe sepsis characterized by the increased concentrations of H(2)O(2) and hypochlorite. We found that treatment of APC with these oxidants markedly inhibits the cleavage of the APC-specific chromogenic substrate, suggesting that oxidants can induce changes in the structure of the active site of APC. Resistance of oxidant-treated APC to chemical digestion with cyanogen bromide (CNBr) implies that methionine oxidation can at least in part be responsible for inhibition of APC. Since methionine residues, the main targets of oxidants in APC, are not included in the active site, we hypothesize that oxidation induces allosteric changes in the architecture of the catalytic triad of APC. Using molecular dynamics (MD) simulations we found that methionine oxidation alters the distance between cSer195Ogamma and cHis57Nepsilon2 atoms placing them in positions unfavorable for the catalysis. At the same time, neither distances between Calpha atoms of the catalytic triad cAsp102-cHis57-cSer195, nor the overall structure of APC changed significantly after oxidation of the methionine residues. Disruption of the H-bond between Ndelta1 of cHis57 and carboxyl group of cAsp102, which can take place during the hypochlorite-induced modification of cHis57, dramatically changed the architecture of the catalytic triad in oxidized APC. This mechanism could contribute to APC inactivation by hypochlorite concurrently with methionine oxidation. These are novel findings, which describe potentially pathophysiologically relevant changes in the functional stability of APC exposed to the oxidative stress. |
| Author | Nalian, Armen Iakhiaev, Alexei V |
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| BackLink | https://www.ncbi.nlm.nih.gov/pubmed/18612533$$D View this record in MEDLINE/PubMed |
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| Snippet | Activated protein C (APC) is a serine protease, an effector enzyme of the natural anticoagulant pathway. APC is approved for treatment of severe sepsis... |
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| SubjectTerms | Allosteric Regulation Aspartic Acid - chemistry Binding Sites Computer Simulation Cyanogen Bromide - chemistry Enzyme Activation Enzyme Stability Histidine - chemistry Humans Hydrogen Bonding Hydrogen Peroxide - chemistry Hydrogen Peroxide - metabolism Hypochlorous Acid - chemistry Hypochlorous Acid - metabolism Methionine - chemistry Models, Molecular Oxidants - chemistry Oxidants - metabolism Oxidation-Reduction Protein Binding Protein C - chemistry Protein C - metabolism Protein Conformation Recombinant Proteins - chemistry Recombinant Proteins - metabolism |
| Title | Possible mechanisms contributing to oxidative inactivation of activated protein C: molecular dynamics study |
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