Pybox ligand

Asymmetric epoxidation of olefins with ruthenium catalysts based either on chiral porphyrins or on pyridine-2,6-bisoxazoline (pybox) ligands has been reported (Scheme 6.21). Berkessel et al. reported that catalysts 27 and 28 were efficient catalysts for the enantioselective epoxidation of aryl-substituted olefins (Table 6.10) [139]. Enantioselectivities of up to 83% were obtained in the epoxidation of 1,2-dihydronaphthalene with catalyst 28 and 2,6-DCPNO. Simple olefins such as oct-l-ene reacted poorly and gave epoxides with low enantioselectivity. The use of pybox ligands in ruthenium-catalyzed asymmetric epoxidations was first reported by Nishiyama et al., who used catalyst 30 in combination with iodosyl benzene, bisacetoxyiodo benzene [PhI(OAc)2], or TBHP for the oxidation of trons-stilbene [140], In their best result, with PhI(OAc)2 as oxidant, they obtained trons-stilbene oxide in 80% yield and with 63% ee. More recently, Beller and coworkers have reexamined this catalytic system, finding that asymmetric epoxidations could be perfonned with ruthenium catalysts 29 and 30 and 30% aqueous hydrogen peroxide (Table 6.11) [141]. Development of the pybox ligand provided ruthenium complex 31, which turned out to be the most efficient catalyst for asymmetric... 

Desimoni et al. [101] further investigated the influence of the variation of the lanthanide and of the PyBOx ligand (bearing a Pr- or Ph-substituent with the same configuration) on the enantioselectivity of the Diels-Alder test... 

Evans and Wu have prepared complexes derived from PyBOx ligands and samarium or gadolinium triflates that were efficient for the Diels-Alder reaction between various quinones and dienes [102] (see Scheme 38 for an example). 

Related catalytic enantioselective processes [115] Two catalytic procedures for asymmetric addition of cyanides to meso epoxides have been reported [116]. One is the result of work carried out in these laboratories, shown in Eq. 6.24, promoted by Ti-peptide chiral complexes, while the other, developed by Jacobsen and Schaus, is a Yb-catalyzed enantioselective reaction that is effected in the presence of pybox ligands (Eq. 6.25) [117]. Although the Shibasaki method (Eq. 6.21) is not as enantioselective as these latter methods, it has the advantage that it accomplishes both the epoxidation and subsequent desymmetrization in a single vessel. 

Reactions Catalyzed by Iridium Complexes of Pybox Ligands... 

Cyclopropanation is an important synthetic method, and enantioselective catalytic reactions of olefins and diazoacetates provide access to valuable products with biological activity. In general, these reactions are conducted in anhydrous solvents and in several cases water was found to diminish the rate or selectivity (or both) of a given process. Therefore it came as a surprise, that the Cyclopropanation of styrene with (+)- or (-)-menthyl diazoacetates, catalyzed by a water-soluble Ru-complex with a chiral bis(hydroxymethyldihydrooxazolyl)pyridine (hm-pybox) ligand proceeded not only faster but with much Wgher enantioselectivity (up to 97 % e.e.) than the analogous reactions in neat THF or toluene(8-28 % e.e.) (Scheme 6.34) [72]. The fine yields and enantioselectivities may be the results of an accidental favourable match of the steric and electronic properties of hm-pybox and those of the menthyl-dizaoacetates, since the hydroxyethyl or isopropyl derivatives of the ligand proved to be inferior to the hydroxymethyl compound. Nevertheless, this is the first catalytic aqueous cyclopropanation which may open the way to other similar reactions in aqueous media. 

CuOTf/PyBox System The first direct asymmetric addition of alkynes to imines, generated from aldehydes and amines in situ, was reported by using copper salts in the presence of chiral PyBox ligand (Scheme 5.2). The products were obtained in good yields and excellent enantioselectivities in most cases. When toluene was used as solvent, up to 93% yield and 99% ee were obtained. Up to 99.5% ee was obtained when the reaction was carried out in 1,2-dichloroethane. The reaction can also be performed in water smoothly, and good enantioselectivities (78-91% ee) were obtained. 

The C2-symmetric 2,6-bis(2-oxazolin-2-yl)pyridine (pybox) ligand was originally applied with Rh for enantioselective hydrosilylation of ketones [79], but Nishiyama, Itoh, and co-workers have used the chiral pybox ligands with Ru(II) as an effective cyclopropanation catalyst 31 [80]. The advantages in the use of this catalyst are the high enantiocontrol in product formation (>95 % ee) and the exceptional diastereocontrol for production of the trans-cyclopropane isomer (>92 8) in reactions of diazoacetates with monosubstituted olefins. Electronic influences from 4-substituents of pyridine in 31 affect relative reactivity (p = +1.53) and enantioselectivity, but not diastereoselectivity [81]. The disadvantage in the use of these catalysts, at least for synthetic purposes, is their sluggish reactivity. In fact, the stability of the intermediate metal carbene has allowed their isolation in two cases [82]. 

Asymmetric Mukaiyama aldol reactions in aqueous media [EtOH-H20 (9 1)] were reported with FeCl2 and PYBOX ligands 27a [36] and 27b [37]. The latter provides product 28 with higher yield and diastereo- and enantioselectivity (Scheme 8.9). The ee values given are for the syn-diastereoisomer. Whereas ligand 27a is a derivative ofL-serine, compound 27b has four stereogenic centers, since it was prepared from... 

The iron-catalyzed process can also be performed with iron-PYBOX systems, as reported by Redlich and Hossain [29]. The PYBOX ligands are powerful tools in organic synthesis. However, for the iron-catalyzed synthesis of aziridines (Scheme 9.14), the results are not as convincing as for similar copper-PYBOX systems. Not only are the yields moderate (up to 54%), but also the enantiomeric excesses (up to 49%) are not in a synthetically useful range, which precludes their use in elaborate applications. 

Scandium(III) and lutetium(ni)133 and zinc134 complexes of C2-symmetric pyri-dine-bis(oxazoline) (PYBOX) ligands are highly effective enantioselective catalysts of Mukaiyama aldol reactions. 

New 4-substituted phenyl(bisoxazoline) ligands (PHEBOX ligands) have been com-plexed with rhodium and examined as enantioselective catalysts of the reductive aldol of acrylates and aldehydes.160 The results have been compared with the corresponding pyridine-centred (PYBOX) ligand complexes. 

Enantiopure amide derivatives (64) of -unsaturated a-hydroxy acids have been made by addition of a vinylsilane, R2R1C=(4ISiMe3, to /V-phcnylglyoxamide.181 The reaction is catalysed by scandium(III) triflate complexed to a C2-symmetric PYBOX ligand derived from (f )-norephedrine. 

Allylic oxidation of a variety of cyclic alkenes with copper complexes of different pybox ligands (8) and with various peresters shows high enantioselectivity (80-96% ee). Use of phenylhydrazine as an additive and acetone as solvent accelerates the reaction. It has been suggested that the phenylhydrazone is responsible for the observed acceleration. Using EPR spectra, it has been shown that the Cu(II) species is reduced to Cu(I) by phenylhydrazine and phenylhydrazone. It has been found that the presence of a gem-diphenyl group at C(5) and a secondary or tertiary alkyl substituent at the chiral centre at C(4) of the oxazoline rings is crucial for high enantioselectivity. 

A chiral pyridine-bisoxazoline ( PYBOX ) ligand has been combined with indium (III) triflate to produce an enantioselective catalyst for allylation of a wide variety of aldehydes in ionic liquids 183 ees of >90% were obtained, and extraction and reuse of the catalyst-ionic liquid combination saw this figure hold up to >80% on the fourth recycle. 

Chiral pybox ligands were synthesized as ligands for the asymmetric cyclopropanation of styrene.10 In-pybox ligand 3 was prepared by reaction of 1 with 2,6-pyridine dicarbonyl dichloride in the presence of potassium hydrogen carbonate in isopropyl acetate followed by cyclization of the fcA-hydroxyamide with BF3 OEt2 at 120°C.22... 

Fu s group showed more recently that ot-bromo ketones 6b can be coupled with arylzinc halides catalyzed by 5 mol% NiCl2 DME and 6.5 mol% of PyBOX ligand 5e with good asymmetric induction providing benzylic ketones in 71-93% yield and 72-96% ee (entry 12) [54]. The lower ee values were obtained with orf/io-substituted aryl bromo ketones, while orf/to-substituted arylzinc reagents as well as a-branched bromo ketones did not react. 

In 1994, asymmetric cydopropanation (ACP) with ruthenium catalysts was first reported by Nishiyama and coworkers [ 19,20] by adoption of their chiral bis(oxazolinyl)pyridine (Pybox) ligands. The reaction profiles of Ru Pybox catalysts reveal extremely high trans selectivity with high enantioselectivity (or di-astereoselectivity) of cyclopropane products at the relatively low reaction temperatures (around 20-50 °C) so far reported for ruthenium catalysts. After 1997,... 

We came up with the idea of the combination of Pybox and a ruthenium atom, like a bolt from the blue, after screening several metals. The new catalytic system was eventually reported in 1994 [19]. A combination of Pybox ligand with a ruthenium(II) cymene complex exhibits high stereochemical efficiency as an in situ catalyst (Scheme 2). The Ru Pybox-ip in situ catalyst (catalyst A)... 

Optically active alcohols, amines, and alkanes can be prepared by the metal catalyzed asymmetric hydrosilylation of ketones, imines, and olefins [77,94,95]. Several catalytic systems have been successfully demonstrated, such as the asymmetric silylation of aryl ketones with rhodium and Pybox ligands however, there are no industrial processes that use asymmetric hydrosilylation. The asymmetric hydrosilyation of olefins to alkylsilanes (and the corresponding alcohol) can be accomplished with palladium catalysts that contain chiral monophosphines with high enantioselectivities (up to 96% ee) and reasonably good turnovers (S/C = 1000) [96]. Unfortunately, high enantioselectivities are only limited to the asymmetric hydrosilylation of styrene derivatives [97]. Hydrosilylation of simple terminal olefins with palladium catalysts that contain the monophosphine, MeO-MOP (67), can be obtained with enantioselectivities in the range of 94-97% ee and regioselectivities of the branched to normal of the products of 66/43 to 94/ 6 (Scheme 26) [98.99]. 

---