Alkyl 3,3,3-trifluoropyruvate

C-alkylation of secondary and tertiary aromatic amines by hexafluoroacetone or methyl trifluoropyruvate is performed under mild conditions [172] (equation 147) The reaction of phenylhydrazme with hexafluoroacetone leads selectively to the product of the C-hydroxyalkylation at the ortho position of the aromatic ring The change from the para orientation characteristic for anilines is apparently a consequence of a cyclic transition state arising from the initial N hydroxy alky lation at the primary amino group [173] (equation 148)... 

A surpnsing feature of the reactions of hexafluoroacetone, trifluoropyruvates, and their acyl imines is the C-hydroxyalkylation or C-amidoalkylaOon of activated aromatic hydrocarbons or heterocycles even in the presence of unprotected ammo or hydroxyl functions directly attached to the aromatic core Normally, aromatic amines first react reversibly to give N-alkylated products that rearrange thermally to yield C-alkylated products. With aromatic heterocycles, the reaction usually takes place at the site of the maximum n electron density [55] (equaUon 5). 

Polyfluorinated a-diketones react with 1,2-diainino compounds, such as ortlio-phenylenediamine, to give 2,3-substituted quinoxalmes [103] Furthermore, the carboxyl function of trifluoropyruvates offers an additional electrophilic center. Cyclic products are obtained with binucleophiles [13, 104] With aliphatic or aromatic 1,2-diamines, six-memhered heterocycles are formed Anilines and phenols undergo C-alkylation with trifluoropyruvates in the ortho position followed by ring closure to form y-lactams and y-lactones [11, 13, 52, 53, 54] (equation 23). 

Uneyama has described some interesting reactions of the N-aryl imines of ethyl trifluoropyruvate. Tandem alkylation/defluorination occurred (Eq. 97) upon exposure to diethylzinc, via attack at nitrogen and SN2 displacement of fluoride anion [279]. Interestingly, an alkylzinc halide reagent attacked regioselec-tively at carbon, perhaps the more expected outcome. 

Prakash, Olah, and co-workers256 have prepared Mosher s acid analogs by the hydroxyalkylation of substituted benzenes with ethyl trifluoropyruvate [Eq. (5.95)]. Deactivated aromatics (fluorobenzene, chlorobenzene) required the use of excess triflic acid indicative of superelectrophilic activation.3 5 In contrast to these observations, Shudo and co-workers257 reported the formation gem-diphenyl-substituted ketones in the alkylation of benzene with 1,2-dicarbonyl compounds [Eq. (5.96)]. In weak acidic medium (6% trifluoroacetic acid-94% triflic acid), practically no reaction takes place. With increasing acidity the reaction accelerates and complete conversion is achieved in pure triflic acid, indicating the involvement of diprotonated intermediates. 

Methyl trifluoropyruvate alkylates a series of substituted indoles catalysed by the chiral non-racemic 2,2/-bipyridylcopper(II) triflate complex (32) to form methyl 3,3,3- trifluoro-2-hydroxy-2-indole-3-yl propanoates [e.g. (33)] in high enantiomeric excess and good yield.37... 

Sulfimines 175 are obtained in excellent yield by Staudinger condensation of sulfin-amide 174 with trifluoropyruvates. In contrast, and quite surprisingly, the Staudinger reaction of terf-butylsulfinamide 182 with the pyruvates under the same conditions does not work. Sulfimines 175 are alkylated with Grignard reagents in good yields but with poor to moderate diastereoselectivities (see Scheme 9.39) [67]. 

Base-catalyzed deprotonation-alkylation of trifluoroalanine is not easy because a-trifluoromethylated carbanions readily undergo defluorination in general [90]. Therefore, a-alkylated trifluoroalanines have been prepared either by alkylation of imines obtained from trifluoropyruvates [54, 57]or by Strecker cyanation [56] to trifluoroketimines fol-... 

Very recently, the enantioselective Friedel-Crafts alkylation of the simple phenols 157 with trifluoropyruvate was also accomplished by using the bifunctional quinidine... 

Keywords Friedel-Crafts alkylation, methyl trifluoropyruvate... 

The presence of a strongly electron-attracting group, such as trifluoromethyl can both enhance the reactivity of the carbonyl group and stabilize the carbinol. As a result, such compounds have been the most successful in giving the carbinol product. One of the first successful enantioselective alkylation reactions was carried out using 3,3,3-trifluoropyruvate esters [122]. 

The enantioselective Lewis-acid-promoted 2 -t- 2-cycloaddition of trifluoropyruvate with various alkynes produced stable oxetene derivatives for use in the synthesis of pharmaceuticals and agrochemicals. l,4-diazabicyclo[2.2.2]octane (DABCO)-catalysed 2- -2-cycloaddition of allenoates and trifluoromethylketones produced 2-alkyleneoxetanes in good yields and with good diastereo-selectivities dr > 20 1). A cinchona alkaloid (20) catalysed the 2- -2-cycloaddition between tV-sulfonylimines and alkyl 2,3-butadienoates to form / -configured 2,4-disubstituted azetidines in high yields and with high enantioselectivities. ... 

Enantioselective Friedel-Crafts alkylation reactions were performed between substituted indoles and methyl trifluoropyruvate, using a chiral nonracemic ( -symmetric 2,2 -bipyridyl copper triflate complex as catalyst. The active copper(II) catalyst was... 

Convenient routes to methyl-2-oxalylimino- and 2-(phosphonoformimido)-3,3,3-trifluoropropanoates (165) have been elaborated, based on the reaction of methyl trifluoropyruvate (166) with ethyl oxamate or diethyl carbomoylphosphonate, respectively, followed by dehydration and then alkylation. ... 

N-Boc-protected ethyl trifluoropyruvate imine was effectively used in a F-C reaction with indole derivatives for synthesizing, in high selectivities, quaternary a-amino acids via catalysis with chiral phosphoric acid 26e [64]. A binaphthyl-based chiral sulfonimide [42c] and a chiral squaramide-based hydrogen bond donor [42a] were used as effective catalysts for promoting F-C reaction of indoles with imines. Recently, the F-C alkylation of arenes with glyoxylate imine was described via a chiral phosphoric add (Scheme 35.11) [34]. 

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