Literature DB >> 30926606

Mechanism and regulation of ferrous heme-nitric oxide (NO) oxidation in NO synthases.

Jesús Tejero1, Andrew P Hunt2, Jérôme Santolini1, Nicolai Lehnert2, Dennis J Stuehr3.   

Abstract

Nitric oxide (NO) synthases (NOSs) catalyze the formation of NO from l-arginine. We have shown previously that the NOS enzyme catalytic cycle involves a large number of reactions but can be characterized by a global model with three main rate-limiting steps. These are the rate of heme reduction by the flavin domain (kr ), of dissociation of NO from the ferric heme-NO complex (kd ), and of oxidation of the ferrous heme-NO complex (k ox). The reaction of oxygen with the ferrous heme-NO species is part of a futile cycle that does not directly contribute to NO synthesis but allows a population of inactive enzyme molecules to return to the catalytic cycle, and thus, enables a steady-state NO synthesis rate. Previously, we have reported that this reaction does involve the reaction of oxygen with the NO-bound ferrous heme complex, but the mechanistic details of the reaction, that could proceed via either an inner-sphere or an outer-sphere mechanism, remained unclear. Here, we present additional experiments with neuronal NOS (nNOS) and inducible NOS (iNOS) variants (nNOS W409F and iNOS K82A and V346I) and computational methods to study how changes in heme access and electronics affect the reaction. Our results support an inner-sphere mechanism and indicate that the particular heme-thiolate environment of the NOS enzymes can stabilize an N-bound FeIII-N(O)OO- intermediate species and thereby catalyze this reaction, which otherwise is not observed or favorable in proteins like globins that contain a histidine-coordinated heme.
© 2019 Tejero et al.

Entities:  

Keywords:  computational biology; dioxygenation; enzyme kinetics; enzyme mechanism; heme; heme protein; heme-thiolate; nitric oxide; nitric-oxide synthase; reaction mechanism; redox reaction; thermodynamics

Mesh:

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Year:  2019        PMID: 30926606      PMCID: PMC6514623          DOI: 10.1074/jbc.RA119.007810

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  55 in total

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2.  Molecular basis for hyperactivity in tryptophan 409 mutants of neuronal NO synthase.

Authors:  S Adak; Q Wang; D J Stuehr
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Authors:  Mohammad Mahfuzul Haque; Jesús Tejero; Mekki Bayachou; Zhi-Qiang Wang; Mohammed Fadlalla; Dennis J Stuehr
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Review 10.  What does "NO-Synthase" stand for ?

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Journal:  Front Biosci (Landmark Ed)       Date:  2019-01-01
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