Equilibrium and ultrafast kinetic studies manipulating electron transfer: A short-lived flavin semiquinone is not sufficient for electron bifurcation.
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| Abstract | 
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              Flavin-based electron transfer bifurcation is emerging as a fundamental and powerful mechanism for conservation and deployment of electrochemical energy in enzymatic systems. In this process, a pair of electrons is acquired at intermediate reduction potential ( intermediate reducing power), and each electron is passed to a different acceptor, one with lower and the other with higher reducing power, leading to "bifurcation." It is believed that a strongly reducing semiquinone species is essential for this process, and it is expected that this species should be kinetically short-lived. We now demonstrate that the presence of a short-lived anionic flavin semiquinone (ASQ) is not sufficient to infer the existence of bifurcating activity, although such a species may be necessary for the process. We have used transient absorption spectroscopy to compare the rates and mechanisms of decay of ASQ generated photochemically in bifurcating NADH-dependent ferredoxin-NADP oxidoreductase and the non-bifurcating flavoproteins nitroreductase, NADH oxidase, and flavodoxin. We found that different mechanisms dominate ASQ decay in the different protein environments, producing lifetimes ranging over 2 orders of magnitude. Capacity for electron transfer among redox cofactors charge recombination with nearby donors can explain the range of ASQ lifetimes that we observe. Our results support a model wherein efficient electron propagation can explain the short lifetime of the ASQ of bifurcating NADH-dependent ferredoxin-NADP oxidoreductase I and can be an indication of capacity for electron bifurcation.  | 
        
| Year of Publication | 
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              2017 
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| Journal | 
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              The Journal of biological chemistry 
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| Volume | 
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              292 
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| Issue | 
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              34 
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| Number of Pages | 
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              14039-14049 
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| Date Published | 
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              2017 
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| ISSN Number | 
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              0021-9258 
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| URL | 
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              https://linkinghub.elsevier.com/retrieve/pii/S0021-9258(20)34222-8 
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| DOI | 
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              10.1074/jbc.M117.794214 
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| Short Title | 
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              J Biol Chem 
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