Kinetic isotope effects hydride transfer

Three mechanisms have been proposed for this reaction (Scheme 21). The reaction is first order in each of the reactants. In another study, Reutov and coworkers159 found a large primary hydrogen-deuterium kinetic isotope effect of 3.8 for the reaction of tri-(para-methylphenyl)methyl carbocation with tetrabutyltin. This isotope effect clearly demonstrates that the hydride ion is transferred in the slow step of the reaction. This means that the first step must be rate-determining if the reaction proceeds by either of the stepwise mechanisms in Scheme 21. The primary hydrogen-deuterium kinetic isotope effect is, of course, consistent with the concerted mechanism shown in Scheme 21. 

The primary hydrogen-deuterium kinetic isotope effect is obtained from the percent cw-2-butene obtained from the deuterated and undeuterated stannanes. This is possible because a hydride and a deuteride are transferred to the carbocation when the undeuterated and deuterated stannane, respectively, forms c -2-butene. The secondary deuterium kinetic isotope effect for the hydride transfer reaction is obtained from the relative amounts of fraws-2-butene in each reaction. This is because a hydride is transferred from a deuterated and undeuterated stannane when trans-2-butene is formed. 

The exo and the endo ring closures (the kc reactions) are in competition with the aryl radical-tributyltin hydride transfer (the ks or ku reaction). These workers162 used this competition to determine the primary hydrogen-deuterium kinetic isotope effect in the hydride transfer reaction between the aryl radical and tributyltin hydride and deuteride. 

This method gave a primary hydrogen-deuterium kinetic isotope effect of 1.3 for the reaction between the aryl radical and tributyltin hydride. This isotope effect is smaller than the isotope effect of 1.9 which San Filippo and coworkers reported for the reaction between the less reactive alkyl radicals and tributyltin hydride163 (vide infra). The smaller isotope effect of 1.3 in the aryl radical reaction is reasonable, because an earlier transition state with less hydrogen transfer, and therefore a smaller isotope effect164, should be observed for the reaction with the more reactive aryl radicals. 

San Filippo and coworkers163 have determined the temperature dependence of the primary hydrogen-deuterium kinetic isotope effects for the hydrogen transfer reactions between several organic radicals and tributyltin hydride (deuteride) see equation 116. 

The pyridine-catalysed lead tetraacetate oxidation of benzyl alcohols shows a first-order dependence in Pb(OAc)4, pyridine and benzyl alcohol concentration. An even larger primary hydrogen kinetic isotope effect of 5.26 and a Hammett p value of —1.7 led Baneijee and Shanker187 to propose that benzaldehyde is formed by the two concurrent pathways shown in Schemes 40 and 41. Scheme 40 describes the hydride transfer mechanism consistent with the negative p value. In the slow step of the reaction, labilization of the Pb—O bond resulting from the coordination of pyridine occurs as the Ca—H bond is broken. The loss of Pb(OAc)2 completes the reaction with transfer of +OAc to an anion. 

Experiments have implied that quantum mechanical effects can be involved in the proton and hydride transfer of several biological processes. Specifically, large kinetic isotope effects (KIE) observed for... 

An interesting catalytic ruthenium system, Ru(7/5-C5Ar4OH)(CO)2H based on substituted cyclopentadienyl ligands was discovered by Shvo and coworkers [95— 98]. This operates in a similar fashion to the Noyori system of Scheme 3.12, but transfers hydride from the ruthenium and proton from the hydroxyl group on the ring in an outer-sphere hydrogenation mechanism. The source of hydrogen can be H2 or formic acid. Casey and coworkers have recently shown, on the basis of kinetic isotope effects, that the transfer of H+ and TT equivalents to the ketone for the Shvo system and the Noyori system (Scheme 3.12) is a concerted process [99, 100]. 

Andres, J., Moliner, V. and Safont, V. S. Theoretical kinetic isotope effects for the hydride-transfer step in Lactate Dehydrogenase, J. Chem. Soc. Faraday Trans., 90 (1994),... 

The practical usefulness of Equations 11.46 through 11.53 has been demonstrated for the malic enzyme catalyzed conversion of L-malate to pyruvate (Equation 11.72). Table 11.1 lists experimentally determined isotope effects for this reaction. Comparison of carbon kinetic isotope effects for protio and deutero-malate substituted at position 2 (the carbon that undergoes sp3 to sp2 transition) rules out the possibility that the hydride transfer and the decarboxylation events are concerted. This conclusion follows from Equation 11.48 which, for a concerted reaction, predicts that 13(V/K) should be smaller than 13(V/K)D, which is opposite to the order observed experimentally. 

In the following year, Cleland and his coworkers reported further and more emphatic examples of the phenomenon of exaltation of the a-secondary isotope effects in enzymic hydride-transfer reactions. The cases shown in Table 1 for their studies of yeast alcohol dehydrogenase and horse-liver alcohol dehydrogenase would have been expected on traditional grounds to show kinetic isotope effects between 1.00 and 1.13 but in fact values of 1.38 and 1.50 were found. Even more impressively, the oxidation of formate by NAD was expected to exhibit an isotope effect between 1.00 and 1/1.13 = 0.89 - an inverse isotope effect because NAD" was being converted to NADH. The observed value was 1.22, normal rather than inverse. Again the model of coupled motion, with a citation to Kurz and Frieden, was invoked to interpret the findings. 

It is difficult to correlate the kyi/k values with the operation of a hydride, proton or H atom transfer. The temperature dependence of the kinetic isotope effect, which is now easier to measure accurately, is more diagnostic of mechanism but has been applied mainly to organic systems. ... 

In the aldol-Tishchenko reaction, a lithium enolate reacts with 2 mol of aldehyde, ultimately giving, via an intramolecular hydride transfer, a hydroxy ester (51) with up to three chiral centres (R, derived from rYhIO). The kinetics of the reaction of the lithium enolate of p-(phenylsulfonyl)isobutyrophenone with benzaldehyde have been measured in THF. ° A kinetic isotope effect of fee/ o = 2.0 was found, using benzaldehyde-fil. The results and proposed mechanism, with hydride transfer rate limiting, are supported by ab initio MO calculations. 

The pyridinium chlorochromate (PCC) oxidations of pentaamine cobalt(III)-bound and unbound mandelic and lactic acids have been studied and found to proceed at similar rates.Free-energy relationships in the oxidation of aromatic anils by PCC have been studied. Solvent effects in the oxidation of methionine by PCC and pyridinium bromochromate (PBC) have been investigated the reaction leads to the formation of the corresponding sulfoxide and mechanisms have been proposed. The major product of the acid-catalysed oxidation of a range of diols by PBC is the hydroxyaldehyde. The reaction is first order with respect to the diol and exhibits a substantial primary kinetic isotope effect. Proposed acid-dependent and acid-independent mechanisms involve the rapid formation of a chromate ester in a pre-equilibrium step, followed by rate-determining hydride ion transfer via a cyclic intermediate. PBC oxidation of thio acids has been studied. ... 

Human type II inosine monophosphate dehydrogenase catalyses NAD-dependent conversion of inosine monophosphate (IMP) into xanthosine monophosphate (XMP) measurements of the primary kinetic isotope effect using [ H]IMP suggest that both substrates (IMP and NAD) can dissociate from the enzyme-substrate complex therefore, the kinetic mechanism is not ordered. NMR studies indicate hydride transfer to the B or pro-S face of the nicotinamide ring of NAD, while kinetic studies suggest... 

Isotope effects have also been applied extensively to studies of NAD+/NADP+-linked dehydrogenases. We typically treat these enzymes as systems whose catalytic rates are limited by product release. Nonetheless, Palm clearly demonstrated a primary tritium kinetic isotope effect on lactate dehydrogenase catalysis, a finding that indicated that the hydride transfer step is rate-contributing. Plapp s laboratory later demonstrated that liver alcohol dehydrogenase has an intrinsic /ch//cd isotope effect of 5.2 with ethanol and an intrinsic /ch//cd isotope effect of 3-6-4.3 with benzyl alcohol. Moreover, Klin-man reported the following intrinsic isotope effects in the reduction of p-substituted benzaldehydes by yeast alcohol dehydrogenase kn/ko for p-Br-benzaldehyde = 3.5 kulki) for p-Cl-benzaldehyde = 3.3 kulk for p-H-benzaldehyde = 3.0 kulk for p-CHs-benzaldehyde = 5.4 and kn/ko for p-CHsO-benzaldehyde = 3.4. 

The tropylium cation (274) first observed 1891 and rediscovered in 1957 is perfectly stable and isolable. Cyclopropenyl cations have been observed in solution a long time ago, but 273 remained elusive until very recently. Benzocyclo-propene (1) reacts with triphenylfluoroborate via hydride transfer some 5 times less rapidly than cycloheptatriene. The reaction of deuterated 1 exhibits a kinetic isotope effect of 7.0. However, only a low yield of benzaldehyde (277), the expected hydrolysis product of 273, could be isolated from the reaction mixture. ... 

Participation of the hydride-formyl equilibrium in (16) is also plausible in light of an apparent inverse kinetic deuterium isotope effect for the catalytic process. Use of deuterium gas instead of hydrogen (cf. Expts. 6 and 4 in Table II) causes an increased rate, with kH/k = 0.73 (37). The existence of an isotope effect implies that hydrogen atom transfer occurs before or during the rate-determining step, and an inverse kinetic isotope effect may be possible in the case of a highly endothermic, product-like transition state (73). On the other hand, Bell has concluded that inverse kinetic isotope... 

One of the important mechanistic uses of isotopic substitution is that it can selectively affect different steps in a stepwise mechanism and so help resolve mechanisms and pathways. For example, in reactions where there is hydride transfer coupled to C—C bond formation, the measurement of both 13C/12C and D/H kinetic isotope effects can distinguish whether the steps are concerted or stepwise. Consider, for example, the oxidative decarboxylation of malate catalyzed by the malic enzyme, which could occur either via an intermediate mechanism (2.81) or in a concerted mechanism (2.82).59... 

The enzyme-product complexes of the yeast enzyme dissociate rapidly so that the chemical steps are rate-determining.31 This permits the measurement of kinetic isotope effects on the chemical steps of this reaction from the steady state kinetics. It is found that the oxidation of deuterated alcohols RCD2OH and the reduction of benzaldehydes by deuterated NADH (i.e., NADD) are significantly slower than the reactions with the normal isotope (kn/kD = 3 to 5).21,31 This shows that hydride (or deuteride) transfer occurs in the rate-determining step of the reaction. The rate constants of the hydride transfer steps for the horse liver enzyme have been measured from pre-steady state kinetics and found to give the same isotope effects.32,33 Kinetic and kinetic isotope effect data are reviewed in reference 34 and the effects of quantum mechanical tunneling in reference 35. 

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