Hydride transfer amines

Noyori and coworkers reported well-defined ruthenium(II) catalyst systems of the type RuH( 76-arene)(NH2CHPhCHPhNTs) for the asymmetric transfer hydrogenation of ketones and imines [94]. These also act via an outer-sphere hydride transfer mechanism shown in Scheme 3.12. The hydride transfer from ruthenium and proton transfer from the amino group to the C=0 bond of a ketone or C=N bond of an imine produces the alcohol or amine product, respectively. The amido complex that is produced is unreactive to H2 (except at high pressures), but readily reacts with iPrOH or formate to regenerate the hydride catalyst. 

Extension (70) of this investigation to the reduction of A-phenylazomethines with 36d-LAH gave optically active secondary amines (eq. [IS]). The products had the S configuration, as predicted by reference to Scheme 9, with hydride transfer of the less shielded H2 occurring preferentially when the phenyl points away from the shielding 3-O-benzyl group of the sugar derivative. 

To support the proposed hydride transfer as shown for the substrate geranylacetone 68 in Fig. 30 proline was linked to the primary face of P-CD yielding the tertiary amine 101 which was complexed with ruthenium and employed to ATH under standard conditions. No product was formed at all which is in good agreement with observations by other groups (31,49,50). The presence of a hydrogen... 

Trifluoroalanine has also been prepared by reducing trifluoropyruvate imines (ethyl trifluoropyruvate is available commercially it is prepared either from per-fluoropropene oxide or by trifluoromethylation of ethyl or f-butyl oxalate). These imines are obtained by dehydration of the corresponding aminals or by Staudinger reaction. They can also be obtained by palladium-catalyzed carbonylation of trifluoroacetamidoyl iodide, an easily accessible compound (cf. Chapter 3) (Figure 5.4). Reduction of the imines affords protected trifluoroalanines. When the imine is derived from a-phenyl ethyl amine, an intramolecular hydride transfer affords the regioisomer imine, which can further be hydrolyzed into trifluoroalanine. ... 

This process has not been studied in detail. It has been shown that diphenylnitren-ium ion reacts with various hydrocarbons and metal hydrides to give diphenyl amine. An analysis of the rate constants for these processes showed that the reaction was most likely a hydride transfer, rather than a hydrogen atom transfer (Fig. 13.56). Novak and Kazerani found a similar process in their study of the decay reaction of heteroarylnitrenium ions. 

Dr. Halpern Conceivably to stabilize the intermediate. I wrote the reaction out that way (-i.e., omitting coordination of the amine to the copper) to call attention to the specific point of hydride transfer. Conceivably, such transfer could occur intramolecularly. 

The chemistry of flavins is complex, a fact that is reflected in the uncertainity that has accompanied efforts to understand mechanisms. For flavoproteins at least four mechanistic possibilities must be considered.1533 233 (a) A reasonable hydride-transfer mechanism can be written for flavoprotein dehydrogenases (Eq. 15-23). The hydride ion is donated at N-5 and a proton is accepted at N-l. The oxidation of alcohols, amines, ketones, and reduced pyridine nucleotides can all be visualized in this way. Support for such a mechanism came from study of the nonenzymatic oxidation of NADH by flavins, a reaction that occurs at moderate speed in water at room temperature. A variety of flavins and dihydropyridine derivatives have been studied, and the electronic effects observed for the reaction are compatible with the hydride ion mecha-nism.234 236... 

Since the reaction was first order in aldehyde, the rate determining step was taken to be hydride transfer to the coordinated aldehyde. For simplicity, this reaction sequence has been used in the following discussion on amines. It is not known if the active species is monomeric nor is there IR evidence for any of the above intermediates. Heil and Marko explained the first-order dependence on CO (and H->) to be linked to formation of a catalytically active HRh(CO)3 complex from the CO- and H-deficient clusters discussed below. 

Almost 40 years ago150, the enthalpy of hydride transfer to a collection of N-substituted aldimines R1CH=NR2 was reported and compared with the reaction enthalpy of the same (complex metal) hydride with the corresponding amine R CH2NHR2 reactions 65 and 66, respectively. 

The reduction of nitriles by the nucleophilic attack of hydride transfer reagents has also been widely investigated and is a process with considerable synthetic potential. The reduction yields amine complexes, and rates are typically about ten thousand times faster than for reduction of the free ligand (Fig. 4-19). Once again, the principal effect appears to be associated with the build-up of positive charge on the ligand. 

Using LiAlH4 is a widespread method to generate piperidine rings from lactams. Mechanistically the tetrahedral intermediate 46 is formed first, and this then collapses to the iminium ion 47. The iminium ion is of course more electrophilic than the carbonyl group. Thus after a hydride transfer to the iminium ion and repetition of the reaction sequence again, the tertiary amine 49 is formed. As a matter of principle parallel to this reduction sequence the ketone in ring B is reduced to form 50. 

The scope and mechanism of ionic hydrogenation of iminium cations have been investigated for a CpRuH catalyst bearing a chelating diphosphine.64 The mechanism involves three steps hydride transfer (from the catalyst) to form an amine, coordination of H2 to the resulting ruthenium cation, followed by proton transfer from the dicoordinated H2 to the amine. The cationic intermediate [e.g. CpRu(dppm)( 72-H2)+] can be used to hydrogenate enamines provided that the latter are more basic than the product amine. The relative reactivity of C=C and C=N bonds in a, ft -unsaturated iminium cations has also been investigated. 

The conversion of nitrocoumarins into the amino compounds has been achieved by hydrogen transfer (95JCR(S)372) and an intramolecular hydride transfer features in the formation of Mannich bases of 4-aminocoumarins from 4-alkylaminocoumarin-3-carbaldehyde (95S633). Amine derivatives of coumarin-3-carboxaldehyde undergo a thermal 1,3-cycloaddilion involving an oxime nitrone isomerisation on reaction with Al-methyl-hydtoxylamine yielding hetero-fused coumarins (95JCS(P1)1857). 

Marcus treatment does not exclude a radical pathway in lithium dialkyl-amide reduction of benzophenone. It does, however, seem to be excluded (Newcomb and Burchill 1984a,b) by observations on the reductions of benzophenone by N-lithio-N-butyl-5-methyl-l-hex-4-enamine in THF containing HMPA. Benzophenone is reduced to diphenylmethanol in good yield, and the amine yields a mixture of the acyclic imines no cyclic amines, expected from radical cyclization of a putative aminyl radical, were detected. An alternative scheme (17) shown for the lithium diethylamide reduction, accounts for rapid formation of diphenylmethoxide, and for formation of benzophenone ketyl under these conditions. Its key features are retention of the fast hydride transfer, presumably via the six-centre cyclic array, for the formation of diphenylmethoxide (Kowaski et al., 1978) and the slow deprotonation of lithium benzhydrolate to a dianion which disproportion-ates rapidly with benzophenone yielding the ketyl. The mechanism demands that rates for ketyl formation are twice that for deprotonation of the lithium diphenylmethoxide, and, within experimental uncertainty, this is the case. 

The nicotinamide ring of nicotinamide adenine dinucleotide can exist in both oxidized (NAD+) and reduced (NADH) forms, where the reduced form can be viewed as a double vinylogous amine, i.e. a double enamine. The hydrogen transfer from the C4 atom is widely believed to proceed by a hydride transfer mechanism, reminiscent of the mechanism of carbonyl reduction by metal hydrides. 

Based on the above activation mechanism we wondered whether it would be possible to develop a biomimetic, organocatalytic reductive amination or transfer hydrogenation of ketimines. We reasoned that the activation of the imine by catalytic protonation through the Brpnsted acid should enable the hydrogen transfer from a suitable NADH mimic to yield the corresponding amine (Fig. 2). Hence, initial experiments focused on the examination of various Brpnsted acids in combination with different hydride sources (Rueping et al. 2005a). 

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