SOLVENT-DERIVED PROTONS IN CATALYSIS BY BREWERS-YEAST PYRUVATE DECARBOXYLASE

Catalysis of proton transfer to thiamin diphosphate (TDP) and 2-(1-hydroxyethyl)thiamin diphosphate (HETDP) by pyruvate decarboxylase isozymes (PDC; EC 4.1.1.1) from Saccharomyces carlsbergensis was investigated by determining the solvent discrimination tritium isotope effect, (k(H)/ k(T))(disc), on the reaction of pyruvate to form acetaldehyde in the presence of the nonsubstrate allosteric effector pyruvamide. The fractionation factors for TDP C(2)-L (phi(C(2)) = 0.98 +/- 0.06) and HETDP C(alpha)-L (phi(C(alpha)), = 1.01 +/- 0.07) (L = H or D) do not contribute significantly to observed enzymic isotopic discrimination. The value of (k(H)/k(T))(disc) = 1.0 for reprotonation of TDP C(2)-L under single-turnover conditions ([E] > [S]) is consistent with C(2)-hydron transfer via a catalytic group (phi = 1) equilibrated with solvent. [1-L]Acetaldehyde formation under transient steady-state ([E] < [S]) conditions shows solvent discrimination tritium isotope effects that increase over the range (k(H)/k(T))(disc) = 0.39 (single turnover) to 0.86 (ten turnovers). The 2-fold increase in the value of (k(H)/k(T))(disc) for the [l-L]acetaldehyde product under steady-state compared to single-turnover conditions is attributed to a fractionation factor of phi(1) = 0.88 +/- 0.06 for the residue(s) involved in C(alpha)-hydron transfer to form HETDP. This provides evidence that catalysis of acetaldehyde formation by PDC involves specific protonation of both HETDP C(a)-L and TDP C(2)-L (phi(2) = 1.0 +/- 0.1) and requires at least two catalytic groups. Values of phi less than or equal to 1 for protonation of TDP C(2)-L and HETDP C(alpha)-L provide no evidence that the exocyclic 4'-amino or -imino group (phi greater than or equal to 1.2) provides significant intramolecular catalysis in the enzyme-bound coenzyme.