Structural plasticity broadens the specificity of an engineered protease
- 1 May 1989
- journal article
- research article
- Published by Springer Science and Business Media LLC in Nature
- Vol. 339 (6221), 191-195
- https://doi.org/10.1038/339191a0
Abstract
The substrate specificity of α-lytic protease has been changed dramatically, with a concomitant increase in activity, by replacing an active-site Met with Ala. The substrate specificity of both this mutant and another similar mutant are extraordinarily broad. X-ray crystallographic analysis shows that structural plasticity, a combination of alternate side-chain conformations and binding-site flexibility, allows both large and small substrates to be well accommodated.Keywords
This publication has 24 references indexed in Scilit:
- A Specific, Highly Active Malate Dehydrogenase by Redesign of a Lactate Dehydrogenase FrameworkScience, 1988
- Role of arginine-292 in the substrate specificity of aspartate aminotransferase as examined by site-directed mutagenesisBiochemistry, 1988
- Recruitment of substrate-specificity properties from one enzyme into a related one by protein engineering.Proceedings of the National Academy of Sciences of the United States of America, 1987
- Probing Steric and Hydrophobic Effects on Enzyme-Substrate Interactions by Protein EngineeringScience, 1986
- Refined structure of α-lytic protease at 1.7 Å resolution analysis of hydrogen bonding and solvent structureJournal of Molecular Biology, 1985
- Redesigning Trypsin: Alteration of Substrate SpecificityScience, 1985
- Catalytic mechanism of serine proteases: reexamination of the pH dependence of the histidyl 1J13C2-H coupling constant in the catalytic triad of alpha-lytic protease.Proceedings of the National Academy of Sciences of the United States of America, 1981
- Molecular structure of the α-lytic protease from Myxobacter 495 at 2·8 Å resolutionJournal of Molecular Biology, 1979
- Mechanism of action of serine proteases: tetrahedral intermediate and concerted proton transferBiochemistry, 1976
- High resolution nuclear magnetic resonance studies of the active site of chymotrypsin: II. Polarization of histidine 57 by substrate analogues and competitive inhibitorsJournal of Molecular Biology, 1974