Phenyl extraction

Place the distillate in a separating-funnel and extract the benzonitrile twice, using about 30 ml. of ether for each extraction. Return the united ethereal extracts to the funnel and shake with 10% sodium hydroxide solution to eliminate traces of phenol formed by decomposition of the benzenediazonium chloride. Then run off the lower aqueous layer, and shake the ethereal solution with about an equal volume of dilute sulphuric acid to remove traces of foul-smelling phenyl isocyanide (CaHjNC) which are always present. Finally separate the sulphuric acid as completely as possible, and shake the ether with water to ensure absence of acid. Run off the water and dry the benzonitrile solution over granular calcium chloride for about 20 minutes. 

Note on the laboratory preparation of monoethylaniline. Although the laboratory preparation of monomethyl- or monoethyl-aniline is hardly worth whUe, the following experimental details may be useful to those who wish to prepare pure monoethylaniline directly from amline. In a flask, fitted with a double surface reflux condenser, place 50 g. (49 ml.) of aniline and 65 g. of ethyl bromide, and boU gently for 2 hours or until the mixture has almost entirely sohdified. Dissolve it in water and boil off the small quantity of unreacted ethyl bromide. Render the mixture alkaUne with concentrated sodium hydroxide solution, extract the precipitated bases with three 50 ml. portions of ether, and distil off the ether. The residual oil contains anihne, mono- and di-ethylaniline. Dissolve it in excess of dilute hydrochloric acid (say, 100 ml. of concentrated acid and 400 ml. of water), cool in ice, and add with stirring a solution of 37 g. of sodium nitrite in 100 ml. of water do not allow the temperature to rise above 10°. Tnis leads to the formation of a solution of phenyl diazonium chloride, of N-nitrosoethylaniline and of p-nitrosodiethylaniline. The nitrosoethylaniline separates as a dark coloured oil. Extract the oil with ether, distil off the ether, and reduce the nitrosoamine with tin and hydrochloric acid (see above). The yield of ethylaniline is 20 g. 

Liberate the free base by adding to the phenylhydrazine hydrochloride 125 ml. of 25 per cent, sodium hydroxide solution. Extract the phenyl-hydrazine with two 40 ml. portions of benzene, dry the extracts with 25 g. of sodium hydroxide pellets or with anhydrous potassium carbonate thorough drying is essential if foaming in the subsequent distillation is to be avoided. Most of the benzene may now be distilled under atmospheric pressure, and the residual phenylhydrazine under reduced pressure. For this purpose, fit a small dropping funnel to the main neck of a 100 ml. Claisen flask (which contains a few fragments of porous porcelain) and assemble the rest of the apparatus as in Fig. II, 20, 1, but do not connect the Perkin triangle to the pump. Run in about 40 ml. of the benzene, solution into the flask, heat the latter in an air bath (Fig. II, 5, 3) so that... 

To hydrolyse an ester of a phenol (e.g., phenyl acetate), proceed as above but cool the alkaline reaction mixture and treat it with carbon dioxide until saturated (sohd carbon dioxide may also be used). Whether a solid phenol separates or not, remove it by extraction with ether. Acidify the aqueous bicarbonate solution with dilute sulphuric acid and isolate the acid as detailed for the ester of an alcohol. An alternative method, which is not so time-consuming, may be employed. Cool the alkaline reaction mixture in ice water, and add dilute sulphuric acid with stirring until the solution is acidic to Congo red paper and the acid, if aromatic or otherwise insoluble in the medium, commences to separate as a faint but permanent precipitate. Now add 5 per cent, sodium carbonate solution with vigorous stirring until the solution is alkaline to litmus paper and the precipitate redissolves completely. Remove the phenol by extraction with ether. Acidify the residual aqueous solution and investigate the organic acid as above. 

Step 2. Extraction of the basic components. Extract the ethereal solution (Ej) with 15 ml. portions of 5 per cent, hydrochloric acid until all the basic components have been removed two or three portions of acid are usually sufficient. Preserve the residual ethereal solution (E2) for the separation of the neutral components. Wa.sh the combined acid extracts with 15-20 ml. of ether discard the ether extract as in Step 1. Make the acid extract alkaline with 10-20 per cent, sodium hydroxide solution if any basic component separates, extract it with ether, evaporate the ether, and characterise the residue. If a water-soluble base is also present, it may be recognised by its characteristic ammoniacal odour it may be isolated from the solution remaining after the separation of the insoluble base by ether extraction by distilling the aqueous solution as long as the distillate is alkahne to htmus. Identify the base with the aid of phenyl iso-thiocyanate (compare Section 111,123) or by other means. 

A sodium stannite solution was prepared by addition of aqueous sodium hydroxide (2.5 mol, lOOg) to aqueous stannous chloride (0.25 mol, 56g). The initially formed precipitate redissolved to form a clear solution. This solution was gradually added to a solution of 16.3g (0.1 mol) phenyl-2-nitropropene in THF at room temperature. A slightly exothermic reaction ensued, and the reaction mixture was stirred for 30 min, a saturated sodium chloride solution was added, and the solution was extracted with ether and the pooled extracts were evaporated under vacuum to give essentially pure P2P oxime in 80% yield. 

To a solution of 0.05 mol of 4-phenyl-1,2-butadiene (see Chapter V, Exp. 19) was added in 10 min at -25 to -35°C a solution of 0.10 mol of ethyllithium in 80 ml of diethyl ether (see Chapter II, Exp. 1). After the addition the cooling bath was removed and the reaction mixture was warmed to 30 C in about 15 min and held at this temperature for an additional 15 min. The brown solution was then cautiously poured into 200 ml of ice-water. After separation of the layers four extractions with diethyl ether were carried out. The combined ethereal solutions... 

Phenyl-3-oxopropanoic acid (25 mmol) and EtjN (87.5 mmol) were dissolved in THF (150 ml) and cooled to —40°C. Ethyl chloroformate (27.5 mmol) was added dropwise to this solution and then the reaction mixture was stirred for 30 min at —20°C. Di-n-hexylamine (27.5 mmol) was added to the suspension and it was stirred at room temperature for an additional hour. The reaction mixture was diluted with water (100 ml) and extracted with ether (400 ml). The extract was washed with aq. 5% HCl (100 ml) and brine (2 X 100 ml) and dried over NajSO. The crude amide was obtained by removal of the solvent in vacuo and phenylhydrazine (25 mmol) was added. The mixture was heated to 100°C for 30 min. The residue was held in vacuo to remove the water formed and then powdered ZnCl2 (125 mmol) was added. The mixture was heated at 170"C with manual stirring for 5 min. The cooled residue was dissolved in acetone (100 ml) and diluted with ether (500 ml). Water (100 ml) was added. The organic layer was separated and washed successively with 5% aq. HCl (100 ml) and brine (2 x 100 ml) and dried over NajSO. The solvent was removed in vacuo, and the residue was recrystallized from EtOAc-hexane. The yield was 79%. 

There are thousands of breweries worldwide. However, the number of companies using fermentation to produce therapeutic substances and/or fine chemicals number well over 150, and those that grow microorganisms for food and feed number nearly 100. Lists of representative fermentation products produced commercially and the corresponding companies are available (1). Numerous other companies practice fermentation in some small capacity because it is often the only route to synthesize biochemical intermediates, enzymes, and many fine chemicals used in minor quantities. The large volume of L-phenylalanine is mainly used in the manufacture of the artificial dipeptide sweetener known as aspartame [22389-47-0]. Prior to the early 1980s there was httle demand for L-phenyl alanine, most of which was obtained by extraction from human hair and other nonmicrobiological sources. 

Antioxidants resistant to extraction by lubricants and gasoline are preferred for the stabili2ation of elastomers used in automotive appfications such as gaskets and tubing. Aromatic amine antioxidants, such as A/-phenyl-Ar-(p-toluenesulfonyl)-A-phenylenediamine [100-93-6] (37), with low solubifity in hydrocarbons, are extracted slowly from elastomers and are used for these appfications. 

Catalyst Cation. The logarithms of extraction constants for symmetrical tetra- -alkylammonium salts (log rise by ca 0.54 per added C atom. Although absolute numerical values for extraction coefficients are vastly different in various solvents and for various anions, this relation holds as a first approximation for most solvent—water combinations tested and for many anions. It is important to note, however, that the lipophilicity of phenyl and benzyl groups carrying ammonium salts is much lower than the number of C atoms might suggest. Benzyl is extracted between / -propyl and -butyl. The extraction constants of tetra- -butylammonium salts are about 140 times larger than the constants for tetra- -propylammonium salts of the same anion in the same solvent—water system. 

Methyl>1,5-dlphsnyl-1,2,4-triazole (3), A mixture of phenyl hydrazine hydrochlonde 1 (14 5 g, 0.11 moQ, N-acetytbenzamide 2 (16.5 g, 0.1 moQ and NaOAc (10 g, 0.12 mol) in AcOH (30 mL) was refluxed for 10 h. The product was made elkaline wNaOH solution and extracted with Et20 Evaporation gave a pale yellow oil which slowly sofidiTied, mp 80-61 0. Recrystallization from 90% EtOH and petroleum ether afforded IS 4 g of 3 (76%). 

Phenyl-4(4H)-ona-5,7-dlhydroxy-1-benzopyran (3) A mixture oi phioroglucino 1 (2 77 g 22 mnx)l) and ethyl benzoylacetate 2 (7 65 g 40 mmol) was heated lo 240 250°C l< I 5 h The cooled mixture was extracted with 5% NaOH and Ihe aqueous solution was extracted with EtaO Acidification afforded a brown product which after sublimation at 250 300°C/0 01 mm and recrystallizalion from EtOH gave 2 2 g of 3 (33 5%) mp 278°C... 

Solutions in contact with polyvinyl chloride can become contaminated with trace amounts of lead, titanium, tin, zinc, iron, magnesium or cadmium from additives used in the manufacture and moulding of PVC. V-Phenyl-2-naphthylamine is a contaminant of solvents and biological materials that have been in contact with black rubber or neoprene (in which it is used as an antioxidant). Although it was only an artefact of the separation procedure it has been isolated as an apparent component of vitamin K preparations, extracts of plant lipids, algae, livers, butter, eye tissue and kidney tissue [Brown Chem Br 3 524 1967]. 

Ethers that are solids (e.g. phenyl ethers) can be steam distilled from an alkaline solution which will hold back any phenolic impurity. After the distillate is made alkaline with sodium carbonate, the insoluble ether is collected either by extraction (e.g. with chloroform, diethyl ether or toluene) or by filtration. It is then crystallised from alcohols, alcohol/petroleum ether, petroleum ether, toluene or mixtures of these solvents, sublimed in a vacuum and recrystallised if necessary. 

Hexafluoro-2-phenyl-2-propanol may be recovered from mother liquors, recovered solvent, and the KBr salt cake by extracting the mixture with aqueous base. Neutralization of the aqueous phase gives the alcohol (13-23 g.) which is purified by distillation. 

A-Fluoro-2,4,6-tnmethylpyndmium inflate (1 mmol) is added m several portions at room temperature to a tetrahydrofuran solution of sodium diethyl phenyl-malonate, obtained from 1 mmol of diethyl phenyl malonate and sodium hydnde at 0 C in tetrahydrofuran The reaction imxture is poured mto dilute hydrochlonc acid and extracted with ether The ether extract is washed with sodium bicarbonate and water and dned over magnesium sulfate The oily residue obtamed after removal of tihe ether is chromatographed on sihca gel (dichloromethane-hexane, 1 1) to give diethyl fluorophenylmalonate in 83% yield... 

Dexamethasone bovine tissue liq-liq extraction phenyl silica CN UV 29... 

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