Formylation ethyl formate

Hydrazinopyridazines are easily formylated with formic acid or ethyl formate and acety-lated with acetic anhydride. A-Pyridazinylthiosemicarbazides are obtained from thiocyanates or alkyl- and aryl-isothiocyanates. Hydrazinopyridazines condense with aliphatic and aromatic aldehydes and ketones to give hydrazones. 

On digestion of this solid mass with 1 1. of ice and water, the sodium salt of the enol dissolves in the water, and the unreacted ester is removed by extracting the aqueous layer with two 200-ml. portions of ether (Note 5). The foimyl derivative settles out as an oil upon acidification of the aqueous layer with dilute sulfuric acid. The oil is extracted with three 200-ml. portions of ether, and the ethereal extract is washed several times with water and dried over anhydrous sodium sulfate. The ether is distilled, and, to remove traces of ethyl formate, the oil is heated on a steam bath under a pressure of 20-30 mm. for 1 hour. The remaining yellow formyl derivative weighs 27-29 g. (Note 6). 

Selective formylation of the 3,20-diketone (1) with ethyl formate gives the 2-hydroxymethylene ketone (2). Subsequent methylation and acidic de-formylation affords the 2a-monomethyl product (4) in 50% yield. 

After the addition is complete, the whole Is cooled on an ice bath and there is added drop-wise a solution of 144 parts dl-N-formyl-N-[(ethoxycarbonyl)methyl] -1-phenylethylamine in 133 parts ethyl formate. After the addition is complete, the mixture is stirred overnight at room temperature. 

Block one side of the ketone by introducing a removable group. Alkylation takes place on the other side the blocking group is then removed. A common reaction for this purpose is formylation with ethyl formate (10-119) this generally blocks the less hindered side. The formyl group is easily removed by alkaline hydrolysis (12-41). 

Ethyl formate serves to introduce the formyl group ... 

The lower spectrum shows an ester group (triplet at 1.2 ppm, quartet at 4.2 ppm) and a singlet at 8.1 ppm, the latter indicating the presence of a formyl group. Peak 1 results from ethyl formate, formed by adventitious hydrolysis of the acetal 4. The middle and top spectra correspond to the two acetals (see equation) the assignment is very simple. 

Lactam 299 was prepared from tryptamine and cyano diester 298 by reductive alkylation in about 12% yield. Phosphorus oxychloride cyclization of 299, followed by catalytic reduction, resulted in the corresponding trans disubstituted indolo[2,3-a]quinolizine 300. After transesterification, formylation and methyla-tion were carried out in two subsequent steps with ethyl formate in the presence of triphenylmethylsodium and with an excess of diazomethane to supply ( )-dihydrocorynantheine (163). 

Deprotonation readily occurs at C-7, and the resulting anion can further react with various electrophiles. Thus, treatment with BuLi at — 78 °C followed by reaction with diiodoethane was used to prepare the 7-iodo derivatives depicted in Table 2, while the 7-chloro derivatives were prepared by lithiation with lithium diisopropylamide (LDA), followed by reaction with CCI4. The 7-formyl derivative of the parent pyrazolo[l,5- ]pyridine has been prepared in 82% yield by reaction of the BuLi-generated anion with ethyl formate <2001JME2691>. 

Ethyleneurea see Ethylene thiourea Ethyl formate, see 2-Ethoxyethanol, Ethyl ether s-Ethyl formic acid, see EPTC 5-Ethyl A-formyl-A-propylthiocarbamate, see EPTC 5-Ethyl hexahydro-2-0X0-1 //-azepine-1 -carbothioate, see Molinate... 

Carbon tetrachloride. Chloroform, 2-Chlorophenol, Cyclohexanol, Cyclopentene, 1,1-Dichloroethylene, irans-l, 2-Dichloroethylene, IV.yV-Dimethylaniline, lV,lV-Dimethylformamide, 2,4-Dimethylphenol, 2,4-Dinitrotoluene, 1,4-Dioxane, 1,2-Diphenylhydrazine, Ethyl formate. Formaldehyde, Glycine, Methanol, Methylene chloride. Methyl formate, 2-Methvlphenol. Monuron, 4-Nitrophenol, Oxalic acid, Parathion, Pentachlorophenol, Phenol, l idine. Styrene, Trichloroethylene, Vinyl chloride Formylacetic acid, see cis-l,3-Dichloropropylene, irans-1,3-Dichloropropylene IV-Formylcarbamate of 1-naphthol, see Carbaryl Formyl chloride, see Chloroethane, Chloroform, sym-Dichloromethyl ether, ds-1,3-Dichloropropylene, irans-ES-Dichloropropylene, Methyl chloride. Methylene chloride. Trichloroethylene, Vinyl chloride lV-Formyl-4-chloro-o-toluidine, see Chlornhenamidine. 

Interposition of a methylene group between the phenyl ring and the heterocycle leads to the benzyldiami nopyrimidines, a class of compounds notable for their antibacterial activity. Condensation of hydrocinnamate 54 with ethyl formate leads to the hydroxymethylene derivative 55. In this case, too, the heterocyclic ring is formed by reaction with guanidine. This sequence probably involves initial addition-elimination to the formyl carbon to form 56 cyclization in this case involves simple amide formation. Tautomerization then affords the hydroxy derivative 57. This is converted to tetroxoprim (58) by first replacing the hydro) l by chlorine and then- displacement of halogen with ammonia. 

Formylation of l,4-dimethylpiperazine-2,5-dione (ethyl formate, sodium methoxide) proceeds in nearly quantitative yield to give the hydroxymeth-ylene derivative (94) (80JOC2625). The silyl enol ether of this has been benzylated at C-6 to give (95) in 80-97% yield. 

A somewhat different route is used to prepare an analogue that bears additional oxygen. The sequence, in this case, starts by base-catalyzed formylation of the hydro-cinnamic acid derivative (40-1) with ethyl formate. Condensation of the product (40-2) with guanidine in this case leads to a pyrimidone (40-3), with the cyclization involving an ester-amide interchange between guanidine and the ester. Reaction of... 

We have previously seen (0-96) that dianions of carboxylic acids can be alkylated in the a position. These ions can also be acylated on treatment with a carboxylic ester1705 to give salts of p-keto acids. As in 0-96, the carboxylic acid can be of the form RCH2COOH or RR"CHCOOH. Since p-keto acids are so easily converted to ketones (2-40), this is also a method for the preparation of ketones R COCHiR and R COCHRR", where R can be primary, secondary, or tertiary alkyl, or aryl. If the ester is ethyl formate, an a-formyl carboxylate salt (R = H) is formed, which on acidification spontaneously de-carboxylates into an aldehyde.1706 This is a method, therefore, for achieving the conversion RCH2COOH — RCH2CHO, and as such is an alternative to the reduction methods discussed in 0-83. When the carboxylic acid is of the form RR CHCOOH. better yields are obtained by acylating with acyl halides rather than esters.1707... 

Substitution of hydrogen by fluorine also occurs, albeit with difficulty, in the formyl group of formates ethyl formate reacts with sulfur tetrafluoride in the presence of potassium fluoride to give a mixture of difluoromethyl ethyl ether (14) and ethyl trifluoromethyl ether (15).175... 

---