Catalysts amino-alcohol zinc

A combination of the Lewis acid zinc triflate and the bases NEt, or pyridine acted as an achiral catalyst for this reaction. Instead, using a chiral base which incorporates a bipy ligand to bind zinc gave 26% ee of the product (Scheme 5-42a). Alternatively, diethylzinc was an active precatalyst, but attempts to use chiral amino alcohols as ligands in this system gave low ees (Scheme 5-42b) [31]. 

A related enantiomerically pure zinc amide initiator, (340), has also been described.966 This complex catalyzes the alternating copolymerization of CHO and C02 to yield isotactic material (RR SS = 86 14). Similar enantiomeric excesses have been achieved using a mixture of Et2Zn and the chiral amino alcohol (341).967 Molecular weight distributions are much broader than using catalyst (340), but this protocol is still a convenient way to prepare optically pure diols (Scheme 23). 

A direct catalytic conversion of esters, lactones, and carboxylic acids to oxazolines was efficiently achieved by treatment with amino alcohols in the presence of the tetranuclear zinc cluster Zn4(0C0CF3)60 as catalyst, essential for condensation and cyclodehydration reactions. For example, the use of (5)-valinol allowed the easy synthesis of oxazolines 125 and 126 in satisfactory yields <06CC2711>. A one-pot direct preparation of various 2-substituted oxazolines (as well as benzoxazoles and oxadiazoles) was also performed from carboxylic acids and amino alcohols (or aminophenols or benzhydrazide) using Deoxo-Fluor reagent <06TL6497>. 

However, there are numerous reported instances of stereocontrol by a site-control mechanism involving chiral metal catalysts. That is, Nozaki and coworkers first illustrated the asymmetric alternating copolymerization of cyclohexene oxide and CO2 employing a chiral zinc catalyst derived from an amino alcohol (Fig. 2a) [13-16]. This was soon followed by studies of Coates and coworkers utilizing an imine-oxazoline zinc catalyst (Fig. 2b) [17]. Both investigations provided isotactic poly(cyclohexene carbonate) (Fig. 3) with enantiomeric excess of approximately 70%. 

The cyclocondensation of l,3-amino alcohols with carboxylic acid derivatives is a method often applied for the synthesis of 5,6-dihydro-4/7-l,3-oxazines <1996CHEC-II(6)301 >. Ebsorb-4, a weakly acidic zeolite-type adsorbent with 4 A pore size, proved an efficient catalyst of the cyclization of benzoic acid and 3-aminopropanol <2002TL3985>. In the presence of zinc chloride as a catalyst, the expulsion of ammonia drove the reactions of 3-aminopropanol with nitriles to completion, affording 2-substituted 5,6-dihydro-47f-l,3-oxazines in good yields... 

Transition State Models. The stoichiometry of aldehyde, dialkylzinc, and the DAIB auxiliary strongly affects reactivity (Scheme 9) (3). Ethylation of benzaldehyde does not occur in toluene at 0°C without added amino alcohol however, addition of 100 mol % of DAIB to diethylzinc does not cause the reaction either. Only the presence of a small amount (a few percent) of the amino alcohol accelerates the organometallic reaction efficiently to give the alkylation product in high yield. Dialkyl-zincs, upon reaction with DAIB, eliminate alkanes to generate alkylzinc alkoxides, which are unable to alkylate aldehydes. Instead, the alkylzinc alkoxides act as excellent catalysts or, more correctly, catalyst dimers (as shown below) for reaction between dialkylzincs and aldehydes. The unique dependence of the reactivity on the stoichiometry indicates that two zinc atoms per aldehyde are responsible for the alkyl transfer reaction. 

Compared with asymmetric ethylation, reports on asymmetric phenylation are limited. We disclosed the enantioselective phenylation using diphenylzinc prepared in situ from phenyl Grignard reagent and zinc chloride. This method needs a stoichiometric amount of chiral amino alcohol DBNE 18 but good ee of 82% was achieved [32], A catalytic phenylation was examined using planar chiral compound 1 based on ferrocene, and chiral diaryl carbinols of moderate ee were provided from diphenylzinc and 4-chlorobenzaldehyde (Scheme 10) [33]. A catalytic and highly enantioselective phenylation was realized by binaphthyl-based chiral catalyst 23. In this reaction, the addition of 2 equivalents of diethyl-zinc against catalyst increases the yield and ee [34]. Recently, chiral amino alcohol DPMPM 9 was also reported to be an efficient catalyst for asymmetric phenylation [35]. 

In the course of the continuing study [9a,b] on the enantioselective addition of dialkylzincs to aldehydes by using chiral amino alcohols such as diphenyl(l-methyl-2-pyrrolidinyl)methanol (45) (DPMPM) [48] A. A -dibutylnorephedrine 46 (DBNE) [49], and 2-pyrrolidinyl-l-phenyl-1-propanol (47) [50] as chiral catalysts, Soai et al. reacted pyridine-3-carbaldehyde (48) with dialkylzincs using (lS,2/ )-DBNE 46, which gave the corresponding chiral pyridyl alkanols 49 with 74-86% ee (Scheme 9.24) [51]. The reaction with aldehyde 48 proceeded more rapidly (1 h) than that with benzaldehyde (16 h), which indicates that the product (zinc alkoxide of pyridyl alkanol) also catalyzes the reaction to produce itself. This observation led them to search for an asymmetric autocatalysis by using chiral pyridyl alkanol. 

High anti-diastereoselectivity is observed for several aromatic imines for ortho-substituted aromatic imines the two newly formed stereocenters are created with almost absolute stereocontrol. Aliphatic imines can also be used as substrates and the reaction is readily performed on the gram scale with as little as 0.25 mol% catalyst loading. Furthermore, the Mannich adducts are readily transformed to protected a-hydroxy-/8-amino acids in high yield. The absolute stereochemistry of the Mannich adducts revealed that Et2Zn-linked complex 3 affords Mannich and aldol adducts with the same absolute configuration (2 R). However, the diastereoselectiv-ity of the amino alcohol derivatives is anti, which is opposite to the syn-l,2-diol aldol products. Hence, the electrophiles approach the re face of the zinc enolate in the Mannich reactions and the si face in the aldol reactions. The anti selectivity is... 

A further example used the supported amino alcohols 45,46 and 47 (Scheme 4.76), where the reagents were pumped up from the bottom of the polymer using a pair of long needles connected to peristaltic pumps. The product was collected from the top using another pump and quenched in a solution of dilute hydrochloric acid. For the first run with catalyst 46, the yields and ee were excellent (94% yield in 97% ee), but when 46 was recovered and reused, the yield dropped to 75% and the ee to 50%. This was ascribed to degradation of both the chiral and backbone sites of the polymer by diethyl zinc, again demonstrating that not only do the solid supports need to be mechanically sound but both the backbone support and active site must be also chemically resistant to the reaction conditions [171]. 

Chiral amino alcohols catalyze the enantioselective reaction of diethyl zinc with benzaldehyde to give 1-phenyl propanol. A mixture of the two enantiomers of the amino alcohol, not in equal proportion, is used as the catalyst, and the relative amounts varied. More than 90% e.e. is obtained with a ratio of 1.2, but zero e.e. is obtained when it is 1.0 (exactly racemic). Explain. 

The same differential behavior can be observed with amine nucleophiles. For example, calcium triflate promotes the aminolysis of propene oxide 84 with benzylamine to give 1-(A -benzyl)amino-2-propanol 85, the result of attack at the less substituted site <03T2435>, and which is also seen in the solventless reaction of epoxides with heterocyclic amines under the catalysis of ytterbium(III) triflate <03SC2989>. Conversely, zinc chloride directs the attack of aniline on styrene oxide 34 at the more substituted carbon center <03TL6026>. A ruthenium catalyst in the presence of tin chloride also results in an SNl-type substitution behavior with aniline derivatives (e.g., 88), but further provides for subsequent cyclization of the intermediate amino alcohol, thus representing an interesting synthesis of 2-substituted indoles (e.g., 89) <03TL2975>. 

Several new ligands containing the oxazoline nucleus were synthesized in enantiopure form. Compounds of general structure 165 were obtained from L-serine or L-threonine and found application as catalysts for the zinc addition to aldehydes <03TA3292> or were derived from P-amino alcohols and used in diethylzinc addition to A -(diphenylphosphinoyl) imines <03JOC4322>. Also, compound 166 was derived from a commercially available amino acid and afforded good selectivity in allylic alkylation <03TL6469>. 

We have tried here to incorporate the ferrocene moiety into amino alcohol catalysts and have synthesized the following four kinds of compounds (a) chiral ferrocenyl zincs bearing an aminoethanol auxiliary [12] (b) iV-(l-ferrocenylalkyl)-iV-alkylnorephedrines [13] (c) chiral polymers bearing iV-ferrocenylmethylephe-drine [14] and (d) chiral 1,2-disubstituted ferrocenyl amino alcohols (Fig. 3-2) [15-17]. 

Catalytic reactions have the advantage over the methods discussed so far in that the chiral catalyst need not be added in stoichiometric amounts, but only in very small quantities, which is important if not only the metal (very often a precious one) but also the chiral ligand are expensive. Among the ferrocenes, phosphines are by far the most important catalysts for stereoselective reactions, and are covered in Chapter 2 of this book. We will therefore focus here mainly on the catalytic applications of chiral ferrocenes not containing phosphine groups. Only recently, some progress has been made with such compounds, mainly with sulfides and selenides, and with amino alcohols in the side chain (for this topic, see Chapter 3 on the addition of dialkyl zinc to aldehydes). 

Recently, Soai et al. reported the synthesis of series of chiral dendrimer amino alcohol ligands based on PAMAM, hydrocarbon and carbosilane dendritic backbones (Figure 4.31) [99-102]. These chiral dendrimers were used as catalysts for the enantioselective addition of dialkylzincs to aldehydes and N-diphenylphosphi-nylimines (Scheme 4.25). The molecular structures of the dendrimer supports were shown to have a significant influence on the catalytic properties. The negative dendrimer effect for the PAMAM-bound catalysts was considered due to the fact that the nitrogen and oxygen atoms on the dendrimer skeleton could coordinate to zinc. 

Though not so general as the reactions we have just seen, the catalysed addition of dialkyl zincs to certain aldehydes sets a new standard for catalysis that needs some explaining. Dialkyl zincs add to the pyrimidine aldehyde 216 under catalysis from amino alcohols, amino acids such as leucine 219, hydroxy acids, and simple secondary alcohols or amines such as 218 to give enantiomerically enriched alcohols 217. Plain sailing so far, except for the extraordinary range of catalysts. 

The mechanisms that have been proposed for the amino alcohol-catalyzed reaction all involve two zinc atoms, one amino alcohol and three alkyl groups on the active catalyst [65,71-74]. A composite mechanism is illustrated in Scheme 4.5 for a generic P-amino alcohol. NMR evidence [71] indicates dynamic exchange of the alkyl groups on zinc as shown in the brackets (a bridged species has also been proposed [71]). In experiments done with a polymer-bound amino alcohol catalyst, Frechet has noted that the alkoxide product is not bound to the catalyst and that the alkyl transfer must have therefore occured from diethylzinc in solution. 

The simple amino alcohols discussed have been used as catalysts for enantioselective addition of zinc alkyls to carbonyl compounds (Section D. 1.3.1.4.). In most cases, the reactive amino function is used for the formation of derivatives (including hcterocycles. such as dihydrooxa-zoles. which are formed with acids) which are useful as sources of chiral carbanions (see Sections C., D.l.1.1.2., D.l.3.1.4., D.l.6.1.2.1.. D.1.6.1.3., D.1.6.1.5., D.2.1. and D.2.3.I.). 

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