Cooling Hydrolysis

The cyanohydrin is then treated with 98% sulphuric acid in a cooled hydrolysis kettle to yield methacrylamide sulphate (Figure 15.3)... 

The carboxylation of ketones is carried out essentially as in the preceding experiment, but at slightly higher temperatures (requiring an oil bath or mantle). Thus, acetophenone (6 g, 0.05 mole) in 100 ml of approx. 2 M MMC is stirred and heated at 110-120° for 1 hour. After cooling, hydrolysis in the acid-ice mixture, and isolation from ether, benzoylacetic acid, mp 99-100°, is obtained in 68% yield. Similarly, 1-indanone gives l-indanone-2-carboxylic acid, mp 100-101°, in 91 % yield. 

The performic acid is prepared in the usual manner by allowing a mixture of 1.0 ml of 30% (w/v) H2O2 and 9.0 ml of 88% (w/v) formic acid to stand at room temperature for 1 hr, after which it is cooled to 0°C. A known amount of protein, usually the amount used for routine hydrolysates, is dissolved in 1 to 2 ml of the reagent in a cooled hydrolysis tube. If the protein does not dissolve readily in the cold reagent, it can usually be dissolved first in 0.1 ml of 100% formic acid at room temperature. The mixture is kept at 0°C for 4 hr after which performic acid is destroyed by the addition of 0.15 ml of cold 48 % (w/v) HBr per ml of performic acid reagent used. The bromine which forms, as well as the formic acid solution, can best be removed from the hydrolysis tube by rotary evaporation under high vacuum (mechanical pump) at 40°C with NaOH pellets in the condenser trap the condenser should be cooled with dry ice in ethanol. Acid hydrolysis of the oxidized sample and analysis of the resulting hydrolysates are performed in the usual manner ( 2.1.2). 

A solution of ethyl 2-ethyl-3-methylcycloprop-2-ene-l-carboxylate (2.31 g, 15 mmol) in anhyd THF (40 mL) was added to a suspension of LiAlH (1.18 g, 31 mmol) in THF (100 mL), and the mixture was refluxed for 4 h. After cooling, hydrolysis and extraction with EtjO, distillation gave the title compound, which was purifled by preparative GC (SE 30 column). 

Lead ll) oxide, PbO, exists in two forms as orange-red litharge and yellow massicot. Made by oxidation of Pb followed by rapid cooling (to avoid formation of Pb304). Used in accumulators and also in ceramics, pigments and insecticides. A normal hydroxide is not known but hydrolysis of lead(II) oxyacid salts gives polymeric cationic species, e.g. [Pb OfOH) ] and plumbates are formed with excess base. 

Hydrolysis of Potassium Ethyl Sulphate. Dissolve about i g. of the crystals in about 4 ml. of cold distilled water, and divide the solution into two portions, a) To one portion, add barium chloride solution. If pure potassium ethyl sulphate were used, no precipitate should now form, as barium ethyl sulphate is soluble in water. Actually however, almost all samples of potassium ethyl sulphate contain traces of potassium hydrogen sulphate formed by slight hydrolysis of the ethyl compound during the evaporation of its solution, and barium chloride almost invariably gives a faint precipitate of barium sulphate. b) To the second portion, add 2-3 drops of concentrated hydrochloric acid, and boil the mixture gently for about one minute. Cool, add distilled water if necessary until the solution has its former volume, and then add barium chloride as before. A markedly heavier precipitate of barium sulphate separates. The hydrolysis of the potassium ethyl sulphate is hastened considerably by the presence of the free acid Caustic alkalis have a similar, but not quite so rapid an effect. 

Hydrolysis of Aspirin. Gently boil a mixture of i g. of aspirin and 15 ml. of 10% sodium hydroxide solution in a 50 ml. conical flask under reflux for 20 minutes. Then cool the solution thoroughly and add dilute sulphuric acid until the precipitation of the... 

Boil a mixture of 5 ml. (4 g.) of acetonitrile and 75 ml. of 10% aqueous sodium hydroxide solution in a 200 ml. flask under a refluxwater-condenser for 30 minutes, when hydrolysis will be complete. Detach the condenser and boil the solution in the open flask for a few minutes to drive off ull free ammonia. Then cool the solution, and add dilute sulphuric acid (i volume of concentrated acid 2 volumes of water)... 

A certain amount of hydrolysis of the original acetamide to acid and ammonia always occurs, and the final amine always contains traces of ammonia. This is separated by extracting the mixed anhydrous hydrochlorides with absolute ethanol, which dissolves the amine hydrochloride but not the ammonium chloride filtration of the hot ethanolic extract removes the ammonium chloride, whilst the amine hydrochloride crystallises readily from the filtrate on cooling. 

Hydrolyses to ethanol and acid on being heated for a few minutes. Cool, add a few ml. of water and then cone. HCl, and cool again. Crystals of benzoic acid separate out. Complete hydrolysis cannot be carried out effectively on a test-tube scale. ( ec p. 355). 

Place together in a 50 ml. conical flask about 1 g. of the substance and 10 ml. of 10% NaOH solution (or use apparatus in Fig. 38, p. 63)-Add a few pieces of unglazed porcelain, fit a reflux water- condenser, and boil gently for about 20 minutes. Nitriles require longer heating than amides, usually about 30 minutes. The completion of the hydrolysis of an insoluble nitrile ( .g., benzonitrile) is indicated by the disappearance of oily drops in the liquid. Cool the flask, add an excess of dil. H2SO4 and cool thoroughly. 

Hydrolysis by acids. Sucrose is readily hydrolysed by dilute acids. Dissolve 0 5 g. of sucrose in 5 ml. of water, add 2 ml. of dil. H2SO4 and heat in a boiling water-bath for 5 minutes. Cool and show that the solution has reducing properties, and will form glucosazone. Note that the excess of acid must be neutralised before carrying out the reduction tests. 

Hydrolysis by acids. Place 15 ml. of starch solution in a boiling-tube, add I ml. of cone. HCl, mix well and place in a boiling water-bath for 20 minutes. Cool and add 2 drops of iodine solution to i ml. of the solution no blue coloration is produced. On the remainder, perform tests for glucose in particular show that glucosazone can be formed. Neutralise the excess of acid before carrying out these tests. (Note that a more concentrated acid is required to hydrolyse starch than to hydrolyse the disaccharides, such as sucrose.)... 

Mix 3 g. of starch well with loml. of water in a test-tube and pour the mixture into 90 ml. of boiling water contained in a 300 ml. conical flask, stirring at the same time. Cool to about 70 and then place in a water-bath maintained at 65-70 , but not higher. Now add 2-3 ml. of the malt extract prepared as above, mix well and allow the hydrolysis to proceed. Take a series of test -tubes and in each put 10 ml. of water and 2 drops of a 1 % iodine solution. At intervals of about 4 minutes (depending upon the activity of the enzyme solution), remove 1 ml. of the reaction mixture, cool and add it to one of the test-tubes and note the colour obtained. At the beginning of the experiment the colour will be blue due to the starch alone. As the reaction proceeds, the colour gradually becomes violet, reddish, yellowish and finally colourless. 

For those nitriles which yield water-insoluble amides e.g., the higher alkyl cyanides), hydrolysis to the amide often leads to a satisfactory derivative. The hydration is eflfected by warming a solution of the nitrile in concentrated sulphuric acid for a few minutes, cooling and pouring... 

Hydrolysis of benzanilide. Place 5 g. of benzanilide and 50 ml. of 70 per cent, sulphuric acid in a small flask fitted with a reflux condenser, and boU gently for 30 minutes. Some of the benzoio acid will vapourise in the steam and solidify in the condenser. Pour 60 ml. of hot water down the condenser this will dislodge and partially dissolve the benzoic acid. Cool the flask in ice water filter off the benzoic acid (anifine sulphate does not separate at this dilution), wash well with water, drain, dry upon filter paper, and identify by m.p. (121°) and other tests. Render the filtrate alkaline by cautiously adding 10 per cent, sodium hydroxide solution, cool and isolate the aniline by ether extraction. Recover the ether and test the residue for anifine (Section IV,100). 

Hydrolysis of p-tolunitrile to p-toluic acid. Boil a mixture of 5 g. of p-tolunitrile, 80 ml. of 10 per cent, aqueous sodium hydroxide solution and 15 ml. of alcohol under a reflux condenser. (The alcohol is added to prevent the nitrile, which volatUises in the steam, from crystalhsing in the condenser it also increases the speed of hydrolysis. The alcohol may be omitted in the hydrolysis of nitriles which are hquid at the ordinary temperature, e.g., benzo-nitrUe.) The solution becomes clear after heating for about 1 hour, but continue the boiling for a total period of 1 - 5 hours to ensure complete hydrolysis. Detach the condenser and boil the solution for a few minutes in the open flask to remove dissolved ammonia and incidentally some of the alcohol CAUTION /). Cool, and add concentrated hydrochloric acid until precipitation of the p-toluic acid is complete. When cold, filter off the p-toluic acid with suction and wash with a little cold water. Recrystallise from a mixture of equal volumes of water and alcohol (methylated spirit) or from benzene. The yield of p-toluic acid, m.p. 178°, is 5-5 g. 

Hydrolysis of benzonitrile to benzoic acid. BoU 5 -1 g. (5 ml.) of benzo-nitrUe and 80 ml. of 10 per cent, sodium hydroxide solution in a 250 ml. round-bottomed flask fitted with a reflux water condenser until the condensed liquid contains no oUy drops (about 45 minutes). Remove the condenser, and boU the solution in an open flask for a few minutes to remove free ammonia. Cool the liquid, and add concentrated hydrochloric acid, cautiously with shaking, until precipitation of benzoic acid is complete. Cool, filter the benzoic acid with suction, and wash with cold water dry upon filter paper in the air. The benzoic acid (5-8 g.) thus obtained should be pure (m.p. 121°). Recrystal-lise a small quantity from hot water and redetermine the m.p. 

Hydrolysis of benzyl cyanide to phenylacetamide. In a 1500 ml. three-necked flask, provided with a thermometer, reflux condenser and efficient mechanical stirrer, place 100 g. (98 ml.) of benzyl]cyanide and 400 ml. of concentrated hydrochloric acid. Immerse the flask in a water bath at 40°. and stir the mixture vigorously the benzyl cyanide passes into solution within 20-40 minutes and the temperature of the reaction mixture rises to about 50°, Continue the stirring for an additional 20-30 minutes after the mixture is homogeneous. Replace the warm water in the bath by tap water at 15°, replace the thermometer by a dropping funnel charged with 400 ml. of cold distilled water, and add the latter with stirring crystals commence to separate after about 50-75 ml. have been introduced. When all the water has been run in, cool the mixture externally with ice water for 30 minutes (1), and collect the crude phenylacetamide by filtration at the pump. Remove traces of phenylacetic acid by stirring the wet sohd for about 30 minutes with two 50 ml. portions of cold water dry the crystals at 50-80°. The yield of phenylacetamide, m.p. 154-155°, is 95 g. RecrystaUisation from benzene or rectified spirit raises the m.p. to 156°. 

Hydrolysis of methyl m-nitrobenzoate to m-nitrobenzoic acid. Place 90 -5 g. of methyl m-nitrobenzoate and a solution of 40 g. of sodium hydroxide in 160 ml. of water in a 1-htre round-bottomed flask equipped with a reflux condenser. Heat the mixture to boiling during 5-10 minutes or until the ester has disappeared. Dilute the reaction mixture with an equal volume of water. When cold pour the diluted reaction product, with vigorous stirring, into 125 ml. of concentrated hydrochloric acid. Allow to cool to room temperature, filter the crude acid at the pump and wash it with a httle water. Upon drying at 100°, the crude m-nitrobenzoic acid, which has a pale brownish colour, weighs 80 g. and melts at 140°, Recrystalhsation from 1 per cent, hydrochloric acid afibrds the pure acid, m.p. 141°, as a pale cream sohd the loss of material is about 5 per cent. 

The hydrolysis by alkali is illustrated by the following experimental details for benzamido. Place 3 g. of benzamide and 50 ml. of 10 per cent, sodium hydroxide solution in a 150 ml. conical or round-bottomed flask equipped with a reflux condenser. Boil the mixture gently for 30 minutes ammonia is freely evolved. Detach the condenser and continue the boiling in the open flask for 3-4 minutes to expel the residual ammonia. Cool the solution in ice, and add concentrated hydrochloric acid until the mixture is strongly acidic benzoic acid separates immediately. Leave the mixture in ice until cold, filter at the pump, wash with a little cold water and drain well. RecrystaUise the benzoic acid from hot water. Determine the m.p., and confirm its identity by a mixed m.p. test. 

Method 1. Equip a 1 litre three-necked flask (or bolt-head flask) with a separatory funnel, a mechanical stirrer (Fig. II, 7, 10), a thermometer (with bulb within 2 cm. of the bottom) and an exit tube leading to a gas absorption device (Fig. II, 8, 1, c). Place 700 g. (400 ml.) of chloro-sulphonic acid in the flask and add slowly, with stirring, 156 g. (176 ml.) of pure benzene (1) maintain the temperature between 20° and 25° by immersing the flask in cold water, if necessary. After the addition is complete (about 2 5 hours), stir the mixture for 1 hour, and then pour it on to 1500 g. of crushed ice. Add 200 ml. of carbon tetrachloride, stir, and separate the oil as soon as possible (otherwise appreciable hydrolysis occurs) extract the aqueous layer with 100 ml. of carbon tetrachloride. Wash the combined extracts with dilute sodium carbonate solution, distil off most of the solvent under atmospheric pressure (2), and distil the residue under reduced pressure. Collect the benzenesulphonyl chloride at 118-120°/15 mm. it solidifies to a colourless sohd, m.p. 13-14°, when cooled in ice. The yield is 270 g. A small amount (10-20 g.) of diphen3 lsulphone, b.p. 225°/10 mm., m.p. 128°, remains in the flask. 

Hydrolysis of a substituted amide. A. With 10 per cent, sulphuric acid. Reflux 1 g. of the compound (e.g., acetanilide) with 20 ml. of 10 per cent, sulphuric acid for 1-2 hours. Distil the reaction mixture and collect 10 ml. of distillate this will contain any volatile organic acids which may be present. Cool the residue, render it alkaline with 20 per cent, sodium hydroxide solution, cool, and extract with ether. Distil off the ether and examine the ether-soluble residue for an amine. 

Hydrolysis of a nitrile to an amide. Warm a solution of 1 g. of the nitrile benzyl cyanide) in 4 ml. of concentrated sulphuric acid to 80-90°, and allow the solution to stand for 5 minutes. Cool and pour the solution cautiously into 40 ml. of cold water. Filter oflT the precipitate stir it with 20 ml. of cold 5 per cent, sodium hydroxide solution and filter again. RecrystaUise the amide from dilute alcohol, and determine its m.p. Examine the solubility behaviour and also the action of warm sodium hydroxide solution upon the amide. 

Hydrolysis of a sulphonamide. Mix 2 g. of the sulphonamide with 3-5 ml. of 80 per cent, sulphuric acid in a test-tube and place a thermometer in the mixture. Heat the test-tube, with frequent stirring by means of the thermometer, at 155-165° until the solid passes into solution (2-5 minutes). Allow the acid solution to cool and pour it into 25-30 ml. of water. Render the resulting solution alkaline with 20 per cent, sodium hydroxide solution in order to liberate the free amine. Two methods may be used for isolating the base. If the amine is volatile in steam, distil the alkaline solution and collect about 20 ml. of distillate extract the amine with ether, dry the ethereal solution with anhydrous potassium carbonate and distil off the solvent. If the amine is not appreciably steam-volatile, extract it from the alkaline solution with ether. The sulphonic acid (as sodium salt) in the residual solution may be identified as detailed under 13. 

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