Gating NO Release from Nitric Oxide Synthase
Abstract
We have investigated the kinetics of NO escape from Geobacillus stearothermophilus nitric oxide synthase (gsNOS). Previous work indicated that NO release was gated at position 223 in mammalian enzymes; our kinetics experiments include mutants at that position along with measurements on the wild type enzyme. Employing stopped-flow UV–vis methods, reactions were triggered by mixing a reduced enzyme/N-hydroxy-l-arginine complex with an aerated buffer solution. NO release kinetics were obtained for wt NOS and three mutants (H134S, I223V, H134S/I223V). We have confirmed that wt gsNOS has the lowest NO release rate of known NOS enzymes, whether bacterial or mammalian. We also have found that steric clashes at positions 223 and 134 hinder NO escape, as judged by enhanced rates in the single mutants. The empirical rate of NO release from the gsNOS double mutant (H134/I223V) is nearly as rapid as that of the fastest mammalian enzymes, demonstrating that both positions 223 and 134 function as gates for escape of the product diatomic molecule.
Additional Information
© 2011 American Chemical Society. Received: July 29, 2011. Publication Date (Web): December 7, 2011. C.A.W. thanks Michael Winter for valuable discussions and Dr. Josh Woodward for a spectrum of ferric-NO NOS. Supported by an NSF graduate fellowship (C.A.W.), the NIH (DK019038 to H.B.G. and J.R.W.; GM068461 to J.R.W.; GM095037 postdoctoral fellowship to J.J.W.), and the Arnold and Mabel Beckman Foundation.Attached Files
Accepted Version - nihms343029.pdf
Supplemental Material - ja2069533_si_001.pdf
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Additional details
- PMCID
- PMC3257399
- Eprint ID
- 29957
- DOI
- 10.1021/ja2069533
- Resolver ID
- CaltechAUTHORS:20120403-112410644
- NSF Graduate Research Fellowship
- NIH
- DK019038
- NIH
- GM068461
- NIH
- GM095037
- Arnold and Mabel Beckman Foundation
- Created
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2012-04-03Created from EPrint's datestamp field
- Updated
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2021-11-09Created from EPrint's last_modified field