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Asymmetric Transfer Hydrogenation Reactions

As another successful application of Noyori s TsDPEN ligand, Yan et al. reported the synthesis of antidepressant duloxetine, in 2008. Thus, the key step of this synthesis was the asymmetric transfer hydrogenation of 3-(dime-thylamino)-l-(thiophen-2-yl)propan-l-one performed in the presence of (5,5)-TsDPEN Ru(II) complex and a HCO2H TEA mixture as the hydrogen donor. The reaction afforded the corresponding chiral alcohol in both high yield and enantioselectivity, which was further converted in two steps into expected (5)-duloxetine, as shown in Scheme 9.17. [Pg.281]

Apart from the Meerwin-Ponndorf-Verley (MPV) reaction,16 18catalytic asymmetric transfer hydrogenation has remained quite primitive,111,112 with successful examples of reduction of activated olefins, using alcohols or formic acid as hydrogen source, being reported only recently.113,114... [Pg.92]

A number of excellent reviews have recently been published [1] consequently, this chapter will consider mainly the practical aspects of asymmetric transfer hydrogenation by reviewing each of the components of the reaction, namely catalyst, hydrogen donor, substrate, product and other elements such as solvent, reaction conditions and scale-up. [Pg.1215]

The mechanism of the Meerwein-Pondorf-Verley reaction is by coordination of a Lewis acid to isopropanol and the substrate ketone, followed by intermolecular hydride transfer, by beta elimination [41]. Initially, the mechanism of catalytic asymmetric transfer hydrogenation was thought to follow a similar course. Indeed, Backvall et al. have proposed this with the Shvo catalyst [42], though Casey et al. found evidence for a non-metal-activation of the carbonyl (i.e., concerted proton and hydride transfer [43]). This follows a similar mechanism to that proposed by Noyori [44] and Andersson [45], for the ruthenium arene-based catalysts. By the use of deuterium-labeling studies, Backvall has shown that different catalysts seem to be involved in different reaction mechanisms [46]. [Pg.1223]

The synthesis of amines by the in-situ reductive amination of ketones is termed the Leuckart-Wallach reaction. Recently, an asymmetric transfer hydrogenation version of this reaction has been realized [85]. Whilst many catalysts tested give significant amounts of the alcohol, a few produced almost quantitative levels of the chiral amine, in high enantiomeric excess. [Pg.1234]

Increasing effort has been applied to develope asymmetric transfer hydrogenations for reducing ketones to alcohols because the reaction is simple to perform and does not require the use of reactive metal hydrides or hydrogen. Ruthenium-catalyzed hydrogen transfer from 2-propanol to ketones is an efficient method for the preparation of secondary alcohols. [Pg.377]

The treatment of [Cp MCl2]2 (M = Rh and Ir) with (S,S)-TsDPEN gave chiral Cp Rh and Cp Ir complexes (12a and 12b Scheme 5.9). An asymmetric transfer hydrogenation of aromatic ketones using complex 12 was carried out in 2-propanol in the presence of aqueous KOH (1 equiv.) the results obtained are summarized in Table 5.4. In all of the reactions, the (S)-alcohols were obtained with more than 80% enantiomeric excess (ee) and in moderate to excellent yields. The rhodium catalyst 12a was shown to be considerably more active than the iridium catalyst... [Pg.114]

Figure 1.25 exemplifies the strucmres of certain efficient precatalysts for asymmetric transfer hydrogenation of ketones. Precatalysts C1-C3 use the NH effect described above. A turnover frequency, defined as moles of product per mol of catalyst per hour, of 30,000 h is achieved by using of C2 and an alkaline base in 2-propanol. A Rh complex C3 is an isolobal to the corresponding arene-Ru complex (see Figure 1.23). The Ru complexes C4 " and C5 without NH group in ligand catalyze the reaction by different mechanisms. A higher than 90% optical yield is achieved by using C5 in reduction of certain aliphatic ketones. Figure 1.25 exemplifies the strucmres of certain efficient precatalysts for asymmetric transfer hydrogenation of ketones. Precatalysts C1-C3 use the NH effect described above. A turnover frequency, defined as moles of product per mol of catalyst per hour, of 30,000 h is achieved by using of C2 and an alkaline base in 2-propanol. A Rh complex C3 is an isolobal to the corresponding arene-Ru complex (see Figure 1.23). The Ru complexes C4 " and C5 without NH group in ligand catalyze the reaction by different mechanisms. A higher than 90% optical yield is achieved by using C5 in reduction of certain aliphatic ketones.
Asymmetric transfer hydrogenation of imines catalyzed by chiral arene-Ru complexes achieves high enantioselectivity (Figure 1.34). Formic acid in aprotic dipolar solvent should be used as a hydride source. The reaction proceeds through the metal-ligand bifunctional mechanism as shown in the carbonyl reduction (Figure 1.24). [Pg.26]

Furo[3,4-7]pyridines can be prepared in a stereoselective synthesis involving a ruthenium-catalyzed asymmetric transfer hydrogenation reaction <2001TL1899>. The reaction proceeds with exceptionally high yield and ee (Equation 50). [Pg.312]

A wide range of metals and ligand combinations have been demonstrated to effect the ATH reaction and in this book we concentrate on the systems that have demonstrated high activities and ees that would be the requirement of an industrial application. The initial breakthrough in this area came in 1995 with the report from Ohkuma et alP on the use of chiral monotosylated diamine complexes for asymmetric transfer hydrogenation. [Pg.15]

Asymmetric transfer hydrogenation of benzaldehyde-l-d with (R,R)-28 and (CH3)3COK in 2-propanol gave (R)-benzyl-l-d alcohol quantitatively in 98% ee (Scheme 41) [114], Introduction of electron-donating and electron-accepting groups at the 4 position had little effect on the enantioselectivity. Catalytic deuteration of benzaldehydes was achieved by use of the same complex (R,R)-28 and a 1 1 mixture of formic acid-2-d and triethylamine to give the S deuter-io alcohols in up to 99% ee (Scheme 42) [114], The dt content in the product alcohol was >99%. Only a stoichiometric amount of deuterium source is required to complete the reaction. [Pg.37]

Hydrogenation of dienes with up to 20 1.0 diastereoselectivity and 99% ee is mediated by carbene complexes. The scope and limitations of these reactions were investigated.288 Asymmetric transfer hydrogenation to prochiral ketones, catalysed by a Ru(II) complex (10) or its dimer, with formic acid-triethylamine has been reported, (0 The protocol leads to high yields and enantioselectivity up to 96%. It has been suggested that 16-electron Ru(II) and the Ru-H intermediates are involved in this reaction.289... [Pg.119]

Asymmetric transfer hydrogenation.1 Bis(oxazolines) lacking a methylene bridge such as 3 are prepared by reaction of dimethyl oxalate with a-amino alcohols,... [Pg.40]

See other pages where Asymmetric Transfer Hydrogenation Reactions is mentioned: [Pg.271]    [Pg.279]    [Pg.116]    [Pg.151]    [Pg.1216]    [Pg.1230]    [Pg.1239]    [Pg.1240]    [Pg.1240]    [Pg.378]    [Pg.382]    [Pg.15]    [Pg.86]    [Pg.86]    [Pg.87]    [Pg.116]    [Pg.117]    [Pg.685]    [Pg.433]    [Pg.143]    [Pg.123]    [Pg.29]    [Pg.50]    [Pg.71]    [Pg.71]    [Pg.73]    [Pg.80]    [Pg.115]    [Pg.120]    [Pg.85]    [Pg.44]    [Pg.140]    [Pg.251]    [Pg.114]    [Pg.414]    [Pg.34]   
See also in sourсe #XX -- [ Pg.123 ]



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