Acetamide, bromination

Sodium nitrite Aluminum oxide Acetamide Bromine Dimethylsulfone Sodium methylate... 

Derivativisation to methyl esters with diazomethane Study of conditions for nitration (using N,0-bis-trimethyl silyl-acetamide), bromination (using I -2,3,4,5,6 pentafluorobenzene) and silation of phenoxy alkanoic acids prior to GLC... 

Dissolve 36 g. of sodium hydroxide in 160 ml. of water contained in a 500 ml. conical flask, and chill the stirred solution to 0-5° in ice-water. Now add io-8 ml. (32-4 g.) of bromine slowly to the stirred solution exercise care in manipulating liquid bromine ) during this addition the temperature rises slightly, and it should again be reduced to 0-5°. Add a solution of 12 g. of acetamide in 20 ml. of water, in small portions, to the stirred hypobromite solution so that the temperature of the mixture does not exceed 20° the sodium acet-bromoamide is thus obtained in the alkaline solution. Now remove the flask from the ice-water, and set it aside at room temperature for 30 minutes. 

Place 25 g. of dry acetamide in a 350 ml. conical or flat-bottomed flask, and add 69 g. (23 ml.) of bromine (CAUTION ) a deep red liquid is produced. Cool the flask in ice water and add 10 per cent, sodium hydroxide solution (about 210 ml.) in small portions and with vigorous shaking until the solution acquires a pale yellow colour. At this stage the bromoacetamlde is present in the alkaline solution. If any solid should crystallise out, add a little water. 

Nitrosomethylurea is conveniently prepared by treating acetamide (2 0 mols) with bromine (1 1 mols), followed by 10-25 per cent aqueous caustic alkali (2 0 mols) when acetylmethylurea is produced ... 

Nitrosomethylurea. Acetamide method. To a solution of 59 g. of acetamide in 88 g. (28 ml.) of bromine (1) in a 4-litre beaker add dropwise, with hand stining, a solution of 40 g. of sodium hydroxide in 160 ml. of water. Heat the resulting yellow reaction mixture on a steam bath until eflfervescence sets in (2), after which continue the heating for 2-3 minutes. CrystaUisation of the product from the yellow or red coloured solution usually commences immediately. Cool in an ice bath for 1-2 hours, collect the product by suction filtration, wash with a little ice-cold water, and dry in the air. The yield of colourless acetylmethylurea, m.p. 178-180°, is 50 g. 

It may be neoeasary to heat gently on a steam bath to dissolve the acetamide, and care should be taken that only the minimum amount of bromine is lost during the heating. 

A mixture of acetamide (30 g. = 0-5 mole) and bromine (80 g. = 26 c.c.) in a half-litre flask is kept well cooled with water while enough of a solution of 50 g. of potassium hydroxide in 350 c.c. of water is added to change the initially red-brown colour into a pale yellow this requires most of the alkali. The solution is now run from a dropping funnel in an unbroken jet into a solution of 80 g. of potassium hydroxide in 150 c.c. of water, maintained at 70°-75° in a litre flask. The operation lasts for several minutes. Until the reaction mixture becomes colourless (one quarter to half an hour) the temperature is maintained at 70°-75°, and then the methylamine is distilled with steam. An adapter is fixed to the lower end of the condenser and dips 1 cm. below the surface of the liquid in the receiver (100 c.c. of approximately 5 N-hydrochloric acid2). As soon as the liquid which forms in the condenser is no longer alkaline the distillation is discontinued and the contents of the receiver are evaporated to dryness in a porcelain basin on the water bath. The last traces of water are removed by allowing the basin to stand over night in a vacuum desiccator. The dried material is boiled with absolute alcohol, which dissolves the methylamine hydrochloride but not the ammonium chloride with which it is mixed. The clear filtrate obtained when the ammonium chloride is removed by filtration is concentrated to a small volume and the methylamine hydrochloride is allowed to crystallise out in the cold. The salt is filtered with suction, washed with a little alcohol, and dried in a desiccator. Yield 15-20 g. 

Anodic oxidation of j9-methylbenzyl-sulfonic ester, -carboxylic ester, and -nitrile in Et3N-3HF/CH3CN affords fluorides and acetamides at tbe metbyl (Me) and substituted (CH2E) benzyl position Me/CH2E = 24/76 (E = C02Et), 9/91(CN), 69/31 (SOsEt). In tbe radical bromination of these compounds, substitution at CH3 is enhanced [20],... 

Methylamine occurs in herring brine 2 in crude methyl alcohol from wood distillation,3 and in the products obtained by the dry distillation of beet molasses residues.4 It has been prepared synthetically by the action of alkali on methyl cyanate or iso-cyanurate 5 by the action of ammonia on methyl iodide,6 methyl chloride,7 methyl nitrate,8 or dimethyl sulfate 9 by the action of methyl alcohol on ammonium chloride,10 on the addition compound between zinc chloride and ammonia,11 or on phos-pham 12 by the action of bromine and alkali on acetamide 13 by the action of sodamide on methyl iodide 14 by the reduction of chloropicrin,15 of hydrocyanic or of ferrocyanic acid,16 of hexamethylenetetramine,17 of nitromethane,18 or of methyl nitrite 19 by the action of formaldehyde on ammonium chloride.20... 

Nitration of 1-phenyladamantane occurs at the para position of the phenyl ring 1981. The resulting nitrobenzene brominates on the adamantane nucleus. If, however, the nitro group is converted to an acetamide function, bromine enters the aromatic ring (Scheme 16) I98 ... 

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