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Discrimination between oxygen and carbon monoxide and inhibition of autooxidation by myoglobin. Site-directed mutagenesis of the distal histidine
Sperm whale myoglobin mutants were constructed using site-directed mutagenesis to replace the highly conserved distal histidine residue (His(E7)-64). His-64 was substituted with Gly, Val, Phe, Cys, Met, Lys, Arg, Asp, Thr, and Tyr, and all 10 mutant proteins expressed to approximately 10% of the tot...
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Published in: | The Journal of biological chemistry 1989-02, Vol.264 (6), p.3057-3060 |
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Main Authors: | , , , , , |
Format: | Article |
Language: | English |
Subjects: | |
Online Access: | Get full text |
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Summary: | Sperm whale myoglobin mutants were constructed using site-directed mutagenesis to replace the highly conserved distal histidine
residue (His(E7)-64). His-64 was substituted with Gly, Val, Phe, Cys, Met, Lys, Arg, Asp, Thr, and Tyr, and all 10 mutant
proteins expressed to approximately 10% of the total soluble cell protein in Escherichia coli as heme containing myoglobin.
With the exception of His-64---Tyr, which did not form a stable oxygen (O2) complex, all mutant proteins could be reduced
and bound O2 and carbon monoxide (CO) reversibly. However, removal of the distal histidine increased the rate of autooxidation
40-350-fold. The His-64---Gly, Val, Phe, Met, and Arg mutants all showed markedly increased O2 dissociation rate constants
which were approximately 50-1500-fold higher than those for wild-type myoglobin and increased O2 association rate constants
which were approximately 5-15-fold higher than those for the native protein. All mutants studied (except His-64---Tyr) showed
approximately 10-fold increased CO association rates and relatively unchanged CO dissociation rates. These altered O2 and
CO association and dissociation rate constants resulted in 3-14-fold increased CO affinities, 10-200-fold decreased O2 affinities,
and 50-380-fold greater M (KCO/KO2) values for the mutants compared to the wild-type protein. Thus, the distal histidine of
myoglobin discriminates between CO and O2 binding by both sterically hindering bound CO and stabilizing bound O2 through hydrogen
bonding. The increased autooxidation rates observed for the mutants appear to be due to a decrease in oxygen affinity and
an increase in solvent anion accessibility to the distal pocket. |
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ISSN: | 0021-9258 1083-351X |