Cofactor Dependence of Reduction Potentials for [4Fe-4S]2+/1+ in Lysine 2,3-Aminomutase

Abstract

Lysine 2,3-aminomutase (LAM) catalyzes the interconversion of l-lysine and l-β-lysine by a free radical mechanism. The 5‘-deoxyadenosyl radical derived from the reductive cleavage of S-adenosyl-l-methionine (SAM) initiates substrate-radical formation. The [4Fe-4S]¹⁺ cluster in LAM is the one-electron source in the reductive cleavage of SAM, which is directly ligated to the unique iron site in the cluster. We here report the midpoint reduction potentials of the [4Fe-4S]^2+/1+ couple in the presence of SAM, S-adenosyl-l-homocysteine (SAH), or 5‘-{N-[(3S)-3-aminocarboxypropyl]-N-methylamino}-5‘-deoxyadenosine (azaSAM) as measured by spectroelectrochemistry. The reduction potentials are −430 ± 2 mV in the presence of SAM, −460 ± 3 mV in the presence of SAH, and −497 ± 10 mV in the presence of azaSAM. In the absence of SAM or an analogue and the presence of dithiothreitol, dihydrolipoate, or cysteine as ligands to the unique iron, the midpoint potentials are −479 ± 5, −516 ± 5, and −484 ± 3 mV, respectively. LAM is a member of the radical SAM superfamily of enzymes, in which the CxxxCxxC motif donates three thiolate ligands to iron in the [4Fe-4S] cluster and SAM donates the α-amino and α-carboxylate groups of the methionyl moiety as ligands to the fourth iron. The results show the reduction potentials in the midrange for ferredoxin-like [4Fe-4S] clusters. They show that SAM elevates the reduction potential by 86 mV relative to that of dihydrolipoate as the cluster ligand. This difference accounts for the SAM-dependent reduction of the [4Fe-4S]²⁺ cluster by dithionite reported earlier. Analogues of SAM have a weakened capacity to raise the potential. We conclude that the midpoint reduction potential of the cluster ligated to SAM is 1.2 V less negative than the half-wave potential for the one-electron reductive cleavage of simple alkylsulfonium ions in aqueous solution. The energetic barrier in the reductive cleavage of SAM may be overcome through the use of binding energy.