Acetonedicarboxylic acid dimethyl ester

The mycotoxin patulin was synthesized via the oxidation of a disubstituted furan in the laboratory of M. Tada. The required 2,3-disubstituted furan was conveniently prepared via the Feist-Benary reaction of acetonedicarboxylic acid dimethyl ester and chloroacetaldehyde in the presence of pyridine. Subsequent functional group modification and oxidation of this furan finally gave the natural product. 

More recently, Tada and co-workers reported the total synthesis of patulin (348) in 1994 (Scheme 7.1) (507). Starting with the condensation of acetonedicarboxylic acid dimethyl ester (353) and chloroacetaldehyde to form an appropriately 2,3-disubstituted furan 354, this was further reduced and selectively oxidized at the aromatic carbinol to deliver 3-furaldehyde 355. Dean-Stark condensation of this species in the presence of methanol gave the methyloxy furanopyran 356. Oxidative ring-opening to a carboxylate intermediate and subsequent methylation with diazomethane provided ester 357, which was lactonized and finally demethylated to deliver the natural product 348 in 7% yield over a total of eight consecutive steps. 

The pool of C H acidic components is restricted to compounds that allow a double Mannich reaction. Most common are esters of acetonedicarbonic acid, especially dimethyl acetonedicarboxylate, which is the general substrate for the... 

The synthesis of pyridazine derivatives from hydrazones includes the thermal cyclization of 2-arylhydrazono-3-oxo-5-phenyl-4-pentenenitriles (readily obtained from ethyl cinnamate by condensation with acetonitrile followed by Japp-Klingemann type reactions) to l-aryl-3-cyano-6-phenyl-5,6-dihydro-4(l//)-pyridazinones (Scheme 85) <86JHC93>, and base-induced cyclization of a hydrazone of a 4-chloro-l-arylbutan-l-one to prepare a 2,3,4,5-tetrahydropyridazine (Scheme 85) <88JHC1543>. An earlier route to 6-carboxy-5-hydroxy-2-phenyl-3(2//)-pyridazinone via condensation of benzenediazonium chloride and dimethyl acetonedicarboxylate has been adapted to give a series of aryl derivatives either as esters (by thermal cyclization) or as acids (by cyclization with hydroxide). Both cyclizations proceed in high overall yield (Scheme 86) and decarboxylation of the acids also proceeds in high yield <89JHC169>. 

This reaction was first reported by Perkin in 1883. It is the nucleophilic alkylation between malonic ester and Q, o)-alkyl dihalide to form cyclic aliphatic 1,1-diester or acid and is known as the Perkin reaction or Perkin synthesis. Although it was once referred to as the Perkin condensation, this name should not be used for this type of reaction. Using this protocol, Perkin successfully prepared cyclopropane-, cyclobutane-, cyclopentane-, cyclohexane-, and cycloheptane-1,1-dicarboxylie acids. However, this reaction is often complicated by the side reaction that forms Q, o, a ,a -tetracarboxylic ester from the Sn2 reaction between malonic ester and o, a -alkyl dihalide, this side reaction can be depressed if alcoholic sodium malonic ester is added slowly to the o, a -alkyl dihalide with vigorous stirring. It is interesting that the K2CO3 promoted a reaction between dimethyl 1,3-acetonedicarboxylate and tran5 -l,4-dibromobutene yields vinyldihydrofuran. ... 

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See also in sourсe #XX -- [ ]

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