Asymmetric Hydrophosphonylation of Aldehydes and Imines

Enantioselective addition of P-H bonds in diaUcyl phosphites to aldehydes and imines has been studied in detail. These reactions typically use early metal or Ian- 

When 3 equiv. of TiCh was used, a 93 7 ratio of diastereomers was formed, but with 1.2 equiv. of TiCh, no selectivity was observed and the yield was reduced [20]. 

Subsequent nucleophilic attack on the aldehyde then forms the P-C bond. Protonolysis with i-PrOH gives the product and regenerates the bis(isopropoxide) form of the catalyst alternatively, reaction with 25 would reform the next intermediate [21], 

Since these early reports, several groups have continued to improve these catalytic reactions. The most successful catalysts to date are rare earth/alkaU metal/BINOL complexes like LLB, while titanium, aluminum, and zinc catalysts have also been described. 

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In comparison to related P(III) chemistry, metal-catalyzed additions of P-H bonds in P(V) compounds to unsaturated substrates have been studied in more detail, and several synthetically useful processes have been developed. In particular, the use of heterobimetallic BINOL-based catalysts allows asymmetric hydrophosphonylation of aldehydes and imines in high yield and enantiomeric excess. 

In conclusion, chiral heterobimetallic lanthanoid compexes LnMB, which were recently developed by Shibasaki et al., are highly efficient catalysts in stereoselective synthesis. This new and innovative type of chiral catalyst contains a Lewis acid as well as a Bronsted base moiety and shows a similar mechanistic effect as observed in enzyme chemistry. A broad variety of asymmetric transformations were carried out using this catalysts, including asymmetric C-C bond formations like the nitroaldol reaction, direct aldol reaction, Michael addition and Diels-Alder reaction, as well as C-0 bond formations (epoxidation of enones). Thereupon, asymmetric C-P bond formation can also be realized as has been successfully shown in case of the asymmetric hydrophosphonylation of aldehydes and imines. It is noteworthy that all above-mentioned reactions proceed with high stereoselectivity, resulting in the formation of the desired optically active products in high to excellent optical purity. 

A logical extension of these themes is for one catalyst to activate both the P-nucleophile and the unsaturated electrophile. This approach has been especially popular in asymmetric hydrophosphonylation of aldehydes and imines, which has been reviewed recently [59]. 

The second part of the chapter deals with several kinds of asymmetric reactions catalyzed by unique heterobimetallic complexes. These reagents are lanthanoid-alkali metal hybrids which form BINOL derivative complexes (LnMB, where Ln = lanthanoid, M = alkali metal, and B = BINOL derivative). These complexes efficiently promote asymmetric aldol-type reactions as well as asymmetric hydrophosphonylations of aldehydes (catalyzed by LnLB, where L = lithium), asymmetric Michael reactions (catalyzed by LnSB, where S = sodium), and asymmetric hydrophosphonylations of imines (catalyzed by LnPB, where P = potassium) to give the corresponding desired products in up to 98% ee. Spectroscopic analysis and computer simulations of these asymmetric reactions have revealed the synergistic cooperation of the two different metals in the complexes. These complexes are believed to function as both Brpnsted bases and as Lewis acids may prove to be applicable to a variety of new asymmetric catalytic reactions.1,2... 

Some of the metal-based catalysts used in the asymmetric hydrophosphonylation of aldehydes (see Section 6.4) can also be applied to the phosphonylation of imines. For instance, Shibasaki s heterobimetallic BINOL complexes work well for the catalytic asymmetric hydrophosphonylation of imines. In this case lanthanum-potassium-BINOL complexes (6.138) have been found to provide the highest enantioselectivities for the hydrophosphonylation of acyclic imines (6.139). The hydrophosphonylation of cyclic imines using heterobimetallic lanthanoid complexes has been reported. Ytterbium and samarium complexes in combination with cyclic phosphites have shown the best results in the cases investigated so far. For example, 3-thiazoline (6.140) is converted into the phosphonate (6.141) with 99% ee using ytterbium complex (6.142) and dimethyl phosphite (6.108). The aluminium(salalen) complex (6.110) developed by Katsuki and coworkers also functions as an effective catalyst for the hydrophosphonylation of both aromatic and aliphatic aldimines providing the resulting a-aminophosphonate with 81-91% ee. ... 

The base-catalysed hydrophosphonylation of aldehydes or imines (Pudovik reaction) [58] as a convenient method was widely used for the synthesis of 1-hydrox-yalkylphosphonates. Since the pioneering work of Shibuya [50] and Spilling [51] was reported, much attention has been devoted to developing enantioselective catalysts for the synthesis of chiral 1 -hydroxy alkylphosphonates. Chiral aluminium complexes were shown to be more effective chiral catalysts [59-62]. Based on the success of using A1 (salen) and A1 (salcyen) as asymmetric catalysts, Al-Schiff base complexes [63, 64] have been developed to catalyze the asymmetric addition reaction of dial-kylphosphonates and aldehydes. Tridentate Schiff base metal complexes, such as vanadium, chromium, and iron [65], have been successfully applied in many asymmetric synthetic reactions. We noticed that Al(III) complexes could catalyse the asymmetric Pudovik reaction and these ligands could be easily synthesized [66-70]. 

Heterobimetallic catalysis mediated by LnMB complexes (Structures 2 and 22) represents the first highly efficient asymmetric catalytic approach to both a-hydro and c-amino phosphonates [112], The highly enantioselective hydrophosphonylation of aldehydes [170] and acyclic and cyclic imines [171] has been achieved. The proposed catalytic cycle for the hydrophosphonylation of acyclic imines is shown representatively in Scheme 10. Potassium dimethyl phosphite is initially generated by the deprotonation of dimethyl phosphite with LnPB and immediately coordinates to the rare earth metal center via the oxygen. This adduct then produces with the incoming imine an optically active potassium salt of the a-amino phosphonate, which leads via proton-exchange reaction to an a-amino phosphonate and LnPB. 

Akiyama et al. disclosed an asymmetric hydrophosphonylation in 2005 (Scheme 32) [55], Addition of diisopropyl phosphite (85a) to A-arylated aldimines 86 in the presence of BINOL phosphate (R)-M (10 mol%, R = 3,5-(CF3)j-C Hj) afforded a-amino phosphonates 87 in good yields (72-97%). The enantioselectivities were satisfactory (81-90% ee) in the case of imines derived from a,(3-unsaturated aldehydes and moderate (52-77% ee) for aromatic substrates. 

This kind of heterobimetallic complexes are excellent catalysts for a wide range of reactions, including epoxidation of enones, hydrophosphonylation of imines and aldehydes, and a range of asymmetric C-C bond formation reactions, involving Michael addition reaction, Diels-Alder reaction, aldol and nitroaldol reaction, etc. The alkaU metal has a profoimd effect on the catalytic property of these compounds. 

In 2007, Ooi and coworkers introduced chiral tetraaminophosphonium salts as a new class of Bronsted acids [166]. Similar to the guanidine/guanidinium case, these tetraaminophosphonium salts act as Bronsted bases in their neutral/ deprotonated (triaminoiminophosphorane) form, while they can also be used as mono-functional Bronsted acids in their protonated, phosphonium form. Phos-phonium salt 67, when neutralized in situ with KO Bu, was shown to be a highly effective catalyst in the enantioselective Henry reaction of nitroalkanes with various aromatic and aliphatic aldehydes (Scheme 10.65). The same strategy was further applied to the catalytic asymmetric Henry reaction of ynals [167] and hydrophosphonylation of ynones (Scheme 10.66) [168]. Brfunctional catalysis using this scaffold were also obtained using the carboxylate salts of tetraaminophosphoniums in the direct Mannich reaction of sulfonyl imines with azlactones (Scheme 10.67) [169]. 

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