Glycine ester Schiff bases, asymmetric

Asymmetric Monoalkylation of Glycine Ester Schiff Bases... 

Another synthetic approach was used by Lamaty et al. in asymmetric alkylation of Schiff bases in ball mill (Scheme 2.69) [59]. In optimized reaction conditions, grinding of Schiff base of glycine ester 213 with organic halides in the presence of... 

A-(Diphenylmethylene)glycine t-butyl ester (t-butyl glycinate-benzophenone Schiff base) (171) is a reactive prochiral nucleophile and a-allyl-a-amino acids can be prepared by allylation and hydrolysis of the allylated product. Asymmetric allylation of 171 with cinnamyl acetate (41) afforded 172 regioselec-tively with high % ee when the reaction was carried out in presence of achiral phosphite P(OPh)3, and a ehiral phase-transfer catalyst of alkaloid [0-allyl-(9-anthracenylmethyOcinchonidinium iodide] [65,66]. 

Simple esters cannot be allylated with allyl acetates, but the Schiff base 109 derived from o -amino acid esters such as glycine or alanine is allylated with allyl acetate. In this way. the o-allyl-a-amino acid 110 can be prepared after hydrolysis[34]. The Q-allyl-o-aminophosphonate 112 is prepared by allylation of the Schiff base 111 of diethyl aminomethylphosphonates. [35,36]. Asymmetric synthesis in this reaction using the (+ )-A, jV-dicyclohex-ylsulfamoylisobornyl alcohol ester of glycine and DIOP as a chiral ligand achieved 99% ec[72]. 

More recently, catalytic asymmetric allylations of imines and imine derivatives in aqueous media have been studied. An /V-spiro C2-symmetrical chiral quaternary ammonium salt (5,5)-I-Br (,S, .S )-()-Np-NAS-Br] has been evaluated in the allylation of glycine tert-Bu ester benzophenone Schiff base [Ph2C=NCH2COOCMe3] for synthesis of both natural and unnatural a-amino acids (Eq. 11,45).76... 

Enantioselective Michael addition of glycine derivatives by means of chiral phase-transfer catalysis has been developed to synthesize various functionalized a-alkyl-a-amino acids. Corey utilized 4d as catalyst for asymmetric Michael addition of glycinate Schiff base 1 to a,(3-unsaturated carbonyl substrates with high enantioselectivity (Scheme 2.15) [35,36]. With methyl acrylate as an acceptor, the a-tert-butyl-y-methyl ester of (S)-glutamic acid can be produced, a functionalized glutamic acid... 

The requisite aldimine Schiff base 21 can be readily prepared by the simple imine formation between glycine tert-butyl ester and p-chlorobenzaldehyde in MeOH at room temperature, with the aid of MgS04. The asymmetric monoalkylation of 21 was... 

In all cases it was reported that the trifluoromethyl group enhances the interaction in the prochiral ion pair, resulting in higher ee. The exception appears to be the asymmetric synthesis of a-amino acids via alkylation of the benzophenone Schiff base of glycine alkyl esters with allyl bromide, which produced a 56% ee with the trifluoromethyl-substituted catalyst compared to 66% with the unsubstituted catalysts TY-benzylcinchoninium chloride (3) or TY-benzylcinchonidinium chloride (4) (eq 5). ... 

The glycinate Schiff base of benzophenone 17 was also shown to be a suitable Michael donor for the asymmetric 1,6-addition to the activated dienes 44 having ketones, esters, and sulfones as substituents. Using Corey s phase-transfer catalyst, 16, the corresponding allylated products 47 were obtained as a single E-isomer with high enantioselectivity (from 92 to 98% ee). The synthetic utility of this reaction... 

A phase-transfer-catalyzed direct Mannich reaction of glycinate Schiff base 5 with a-itnino ester 78 was achieved with high enantioselectivity by the use of N-spiro chiral quaternary ammonium bromide 9e as catalyst (Scheme 11.21) [62]. This method enabled the catalyhc asymmetric synthesis of differentiatly protected 3-aminoaspartate, a nitrogen analogue of dialkyl tartrate, the utility of which was demonstrated by the conversion of product (sy -79) into a precursor (80) of strep-tohdine lactam. 

Fluorine substituents on the aromatic ring in chiral quaternary ammonium salts also play an important role for the improvement of enantioselectivity in asymmetric alkylations of the Schiff base of glycine esters in an aqueous biphase system. Dolling first demonstrated asymmetric methylation of indanone (44) by cinchonidine ammonium salt (43) (Scheme 5.12) [18]. 

In 2004, the gronp of Maruoka reported the direct asymmetric Mannich reaction of glycinate Schiff base 104 with a-imino ester 10a catalyzed by A-spiro-C -symmetric chiral quaternary ammoninm bromide 103 to provide the protected 3-aminoaspartate 105 in 88% yield (81 18 dr, 91% ee) [60]. The latter was afterwards converted into a precnrsor of the streptothricin antibiotics core structure (Scheme 5.43). 

---