Thioureas acidity

Scheme 19.2 Carbonyl group shows greater dimerisation potency - urea/thiourea acidity.

Tin Tin, thiourea, acids, whisker inhibiting trace metals, chelation. 4.0-12.0... 

Barbituric acid and 2-thiobarbituric acid are readily prepared by the condensation of diethylmalonate with urea and thiourea respectively, in the presence of sodium ethoxide. The use of substituted derivatives of urea and thiourea and of diethyl malonate will clearly lead to a wide range of barbituric and thiobarbituric acids having substituents in the i, 3, or 5 positions. 

Dissolve 13 g. of sodium in 30 ml. of absolute ethanol in a 250 ml. flask carrying a reflux condenser, then add 10 g. (9 5 ml.) of redistilled ethyl malonate, and place the flask on a boiling water-bath. Without delay, add a solution of 5 3 g. of thiourea in a minimum of boiling absolute ethanol (about 100 ml.). The sodium salt of thiobarbituric acid rapidly begins to separate. Fit the water-condenser with a calcium chloride guard-tube (Fig. 61, p. 105), and boil the mixture on the water-bath for 1 hour. Cool the mixture, filter off the sodium salt at the pump and wash it with a small quantity of cold acetone. Dissolve the salt in warm water and liberate the acid by the addition of 30 ml. of concentrated hydrochloric acid diluted with 30 ml. of water. Cool the mixture, filter off the thiobarbituric acid, and recrystallise it from hot water. Colourless crystals, m.p. 245 with decomposition (immersed at 230°). Yield, 3 5 -4 0 g. 

Amides (except urea and thiourea), imides and nitriles, after the above alkaline hydrolysis, give derivatives similarly to those from the alkaline solution obtained from ammonium salts (p. 360). (A) If the original compound is aromatic, acidification of the cold solution deposits the crystalline acid. (B) The cold solution, when carefully neutralised (p. 332) and treated with benzylthiuronium chloride, deposits the thiuromum salt. 

Place a mixture of 0-5 g. of finely powdered thiourea, 0-5 g. of the alkyl halide and 5 ml. of alcohol in a test-tube or small flask equipped with a reflux condenser. Reflux the mixture for a j)eriod depending upon the nature of the halide primary alkyl bromides and iodides, 10-20 minutes (according to the molecular weight) secondary alkyl bromides or iodides, 2-3 hours alkyl chlorides, 3-5 hours polymethy lene dibromides or di-iodides, 20-50 minutes. Then add 0 5 g. of picric acid, boil until a clear solution is obtained, and cool. If no precipitate is obtained, add a few drops of water. RecrystaUise the resulting S-alkyl-iso-thiuronium picrate from alcohol. 

S-Benzyl-wo-thiuronium chloride (S-benzyl-iao-thiourea hydrochloride) reacts with the alkali metal salts of organic acids to produce crystalline S benzyl-MO-thiuronium salts ... 

To a solution of 0-5 g. of the salt in 5 ml. of water and 2-3 drops of O li hydrochloric acid (or to a solution of the acid treated as above), add a shght excess of a cold, 15 per cent, aqueous solution of benzyl-wo-thiourea hydrochloride (if the molecular weight of the compound is not known, use a solution of 1 g. of the reagent in 5 ml. of water), and cool in ice. Filter off the crystaUine derivative and recrystaUise it from 50 per cent, alcohol. 

Method 1. Dissolve 76 g. of thiourea in 200 ml. of warm water in a 750 ml. or 1 litre round-bottomed flask. Dilute the solution with 135 ml. of rectified spirit and add 126-5 g. of benzyl chloride. Heat the mixture under reflux on a water bath until the benzyl chloride dissolves (about 15 minutes) and for a further 30 minutes taking care that the mixture is well shaken from time to time. Cool the mixture in ice there is a tendency to supersaturation so that it is advisable to stir (or shake) the cold solution vigorously, when the substance crystallises suddenly. Filter off the sohd at the pump. Evaporate the filtrate to about half bulk in order to recover a further small quantity of product. Dry the compound upon filter paper in the air. The yield of hydrochloric acid filter off the sohd which separates on cooling. Concentrate the filtrate to recover a further small quantity. The yield of recrystalhsed salt, m.p. 175° is 185 g. some of the dimorphic form, m.p. 150°, may also separate. 

Method 2. Place a mixture of 126-5 g. of benzyl chloride, 76 g. of thiourea and loO ml. of rectified spirit in a 500 ml. round-bottomed flask fitted with a reflux condenser. Warm on a water bath. A sudden exothermic reaction soon occurs and aU the thiourea passes into solution. Reflux the resulting yellow solution for 30 minutes and then cool in ice. Filter off the white crystals and dry in the air upon filter paper. Concentrate the filtrate to half its original volume and thus obtain a further small crop of crystals. The yield of crude hydrochloric acid as in Method 1 the m.p. is raised to 150°, although on some occasions the form, m.p. 175°, separates. 

The sulfur atom of the thiocarbonyl group is a good nucleophile, and reaction between benzyl bromide and l-(2-thiazolyl)thiourea yields the isothiouronium salt (496). The sulfur atom may also be engaged in a chelate, as exemplified by the Cu chelate of 2-thioureido-4-methylthiazole (491). These chelates with metal ions were thoroughly studied in acidic, neutral, and alkaline media for 66 metal ions in order to define their analytical use. They are formed in the molar ratio of 1 2 for metal II compounds (498). 

The preparation and spectroscopic properties (infrared, ultraviolet, NMR) of iV-alkoxycarbonyl-N -(2-thiazolyl)thioureas (268) have been studied by the Nagano group (78, 264). These compounds react with bromine in acetic acid or chloroform to give 2--alkoxycarbonylimino-thiazolo[3,2-h]thiadiazolines (Scheme 162), whose structures were established by mass spectroscopy, infrared, NMR, and reactivity patterns (481). 

Beyond pharmaceutical screening activity developed on aminothiazoles derivatives, some studies at the molecular level were performed. Thus 2-aminothiazole was shown to inhibit thiamine biosynthesis (941). Nrridazole (419) affects iron metabohsm (850). The dehydrase for 5-aminolevulinic acid of mouse liver is inhibited by 2-amino-4-(iS-hydroxy-ethyl)thiazole (420) (942) (Scheme 239). l-Phenyl-3-(2-thiazolyl)thiourea (421) is a dopamine fS-hydroxylase inhibitor (943). Compound 422 inhibits the enzyme activity of 3, 5 -nucleotide phosphodiesterase (944). The oxalate salt of 423, an analog of levamisole 424 (945) (Scheme 240),... 

In 1873, almost simultaneously, Maly (24), Volhard (38), and Nencki (42) studied the action of thiourea on chloroacetic acid. As mentioned previously, they believed the product to be the thioanalog of hydantoin and called it thiohydantoin with formula 34. 

In 1879, Lange (47) prepared N,N -diphenylthiohydantoin (m.p. 178°C) by condensing chloroacetic acid with N,N -dipheny thiourea and attributed to it structure 43, noting however that it was difficult to derive from 1-43 the structure of the monophenyl derivative (m.p. 148 C)... 

In 1888, Foerster (91), reproducing the same reaction with dianisyl-thiourea, demonstrated that the compound he obtained (59) could lose a sulfur atom by reduction with tin and hydrochloric acid to form a product analogous to N-phenylpiperidine (60). 

In 1882, Nencki and Sieber (98), condensing dibromopyruvic acid with thiourea, obtained a compound they named sulfuvinuric acid (Sulfuvinursaure), which was later demonstrated (99) to be a derivative of 2-aminothiazole. The same year Will (100) observed that the sulfur atom of 56 is masked to Pb(N03)2 and to alkalis. 

The cyclization of -halocarbonyl compounds is carried out with a great variety of reactants including thioamides, thioureas, their mono- or disubstituted derivatives, and salts and esters of monothiocar-bamic acid, leading to variously substituted thiazoles. 

The a-halogenated acids or their esters (105) also react with thiourea to give 2-amino-4-hydroxythiazoles (106a) or their 2-amino-4-thiazolone (106b) (1, 247, 254, 530) or 2-imino-4-oxathia2olidine (106c) tautomers (Scheme 47). 

The synthesis of these disubstituied thioureas takes place in three steps. First the alkyl bromide is prepared by the action of hydrobromic acid on the corresponding alcohol (518). Then the dialkylcyanamide is obtained by treatment at 25°C with calcium cyanamide. The yields are of the order of 30 to 60%. Thioureas are obtained in a third step from the cyanamide by reaction at 40 C with HjS in the presence of pyridine. Yields ranged from 57 to 90% (518),... 

Other sulfur compounds such as thiourea, ammonium dithiocarbamate, or hydrogen sulfide also lead to 2-mercaptothiazoles. Thus thiourea has been used in the syntheses of 4,5-dimethyl (369) and 4-aryl-2-mercapto-thiazoles (Table 11-30) (519). The reactions were carried out by condensing the ia -thiocyanatoketones with thiourea in alcohol and water acidified with hydrochloric acid. By this procedure, 4-aryl-2-mercaptothiazoles were obtained in yields of 40 to 80% with bis-(4-aryl-2-thiazolyl) sulfides as by-products (519). These latter products (194) have also been observed as a result of the action of thiourea on 2-chloro-4-arylthiazole under the same experimental conditions. They can be separated from 2-mercaptothiazoles because of their different degrees of solubility in sodium hydroxide solution at 5%. In this medium bis-(4-phenyl-2-thiazolyl)sulfide is... 

Reactions were carried out by condensing a-thiocyanatokeiones with thiourea in alcohol and water acidified with hydrochloric acid. 

Br , citrate, CE, CN , E, NH3, SCN , S20 , thiourea, thioglycolic acid, diethyldithiocarba-mate, thiosemicarbazide, bis(2-hydroxyethyl)dithiocarbamate Acetate, acetylacetone, BE4, citrate, C20 , EDTA, E , formate, 8-hydroxyquinoline-5-sul-fonic acid, mannitol, 2,3-mercaptopropanol, OH , salicylate, sulfosalicylate, tartrate, triethanolamine, tiron... 

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