Bifurcating electron transferring flavoproteins (Bf-ETFs) tune chemically identical
flavins to two contrasting roles. To understand how, we used hybrid quantum mechanical
molecular mechanical calculations to characterize non-covalent interactions applied to
each flavin by the protein. Our computations replicated the differences between the
reactivities of the flavins: the electron transferring flavin (ETflavin) was calculated to
stabilize anionic semiquinone (ASQ) as needed to execute its single-electron transfers,
whereas the Bf flavin (Bfflavin) was found to disfavor the ASQ state more than does free
flavin and to be less susceptible to reduction. The stability of ETflavin ASQ was attributed
in part to H-bond donation to the flavin O2 from a nearby His side chain, via comparison
of models employing different tautomers of His. This H-bond between O2 and the ET
site was uniquely strong in the ASQ state, whereas reduction of ETflavin to the anionic
hydroquinone (AHQ) was associated with side chain reorientation, backbone
displacement and reorganization of its H-bond network including a Tyr from the other
domain and subunit of the ETF. The Bf site was less responsive overall, but formation of
the Bfflavin AHQ allowed a nearby Arg side chain to adopt an alternative rotamer that can
H-bond to the Bfflavin O4. This would stabilize the anionic Bfflavin and rationalize effects
of mutation at this position. Thus, our computations provide insights on states and
conformations that have not been possible to characterize experimentally, offering
explanations for observed residue conservation and raising possibilities that can now be
tested.
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