From 2-aminothiazoles

Quaternary salts (33) obtained from aminothiazole derivatives liberate 2-imino-4-thiazolines in basic medium (Scheme 24). This reaction is general and independent of the nature of R in 33 (160-167). The same result was found when 2-propynylbromide (168) or 3-chloropropionic acid (169) were the quaternizing reagents. This method is particularly... 

Acylation of the amine with the methoxime from aminothiazole-glyoxylate has a similar effect on broadening the antibacterial spectmm in the 3-methyl series. In this case, the amine group on the starting thiazole (21-3) is first protected by conversion to (28-2) by alkylation with thriphenylmethyl chloride. Condensation of the acid by the mixed anhydride method with 7-ADC A (26-6) leads to the corresponding amide. The trityl group is then removed to afford the antibiotic cefetamet (28-3) [34]. 

Schiff bases, 256-259, 268, 270 to amines. 40 from aminothiazoles, 98 with 2-amino thiazoles, 30, 40 complexes of, 99 cyclization to, 42 IR spectra of, 41 in reduction by AlLiH,. 14 in reduction by NaBH4, 14 LTV spectra of, 41 see also Thiazolylamidines Schistosomacidal, 141 Schistosomiasis japonica, 145 Schotten-Bauman reaction. 51. 123 Sedative, 145. 148,438 Selective herbicide, 135 Self association, effect of, on UV spectra of A-4-thiazoline-2-thione. 381 A-4-thiazoline-2-one, relation with protomery, 377... 

These genera] trends direct the organization of Chapters VI and VII syntheses from the already formed thiazole ring, physicochemical studies, ambident reactivity ring carbon reactivity, main derivatives, and aminothiazole applications. 

Halothiazoles are usually obtained from 2-aminothiazoles through the Sandmeyer reaction. Nevertheless, ammonolysis has sometimes proved useful for the preparation of 2-aminothiazole derivatives. Detweiler et al. (18) obtained 2-(u-pyridinylamino)thiazole (1) from 2-bromothiazole (Scheme 1). The reaction is easier if a nitro group occupies the 5-position of the thiazole ring (19-21). Ethylene diamine derivatives undergo this reaction with 2-haiothiazoles (22-24). 

Aminothiazole and derivatives have been reported in reactivity studies starting from 2-p-nitrophenylsulfenylaminothiazole (4) (32), 2-tritylaminothiazole (5) (33), 2-nitrothiazole (34,35), and 5-methyI-2-phenylimino-4-thiazolidinone (36) (Scheme 4). 

The Curtius rearrangement in acetic anhydride of the azide (8) prepared from 4-carboxythiazole yields 4-acetamidothiazole (Scheme 8) (47). The same reaction starting with ethyl-2-methyl-4-thiazolyl carboxy-late, failed to give the 4-aminothiazole (48). Heterocyclizations are more convenient synthetic methods (Chapter II. Table 40). 

The main features are the molecular ions as the base peak and the M-t-1 ions arising from another species. For 2-aminothiazole the m/e 73 ion (M-HCN) is shifted to m/e 75 in the spectrum of the dideuteroamino derivative and, therefore, largely arises via rupture of 2-3 and 4-5 bonds (Scheme 18). This fragmentation process could involve the kind of intermediates postulated in photochemical rearrangements (see Chapter III, Section IX.3.B). The other fragments fit well the general pattern of fragmentation proposed by Clarke (136). 

Dyatlova (193) reports the preparation of product 49, resulting from the dialkylation of 2-aminothiazole with a-chloroacetic acid under mild conditions (Scheme 36). 

Benzoyl chloride and derivatives acylate 2-amino-4-aryithiazoles in dioxane in yields of 80 to 90% (249, 250). The location of the acyl group on the exocyclic N has been demonstrated by the fact that the benzoyla-tion product is identical to the benzamidothiazole synthesized from benzamide and 2-bromothiazole (251). 3-Indolyl acetic acid chloride (89) acylates 2-aminothiazole in pyridine (Scheme 62) (81). 

As an application of this nucleophilic reactivity, 2-aminothiazole was used to partially convert into amide the polymer obtained from acrylic acid, benzene, and acetic anhydride (271). An aqueous medium is reported to favor the reaction between acetic anhydride and 2-aminothiazole (272). 

The weakly basic 2-aminothiazoles are most readily diazotized in concentrated solutions of oxygen containing acids such as sulfuric acid, 40 to 50% (322-326) fiuoroboric phosphoric acids (589) phosphoric acid (327, 328) and mixtures of phosphoric and nitric acid (74. 322, 323. 329-331). From strong acid solutions, solid diazonium salts can be isolated (34, 332. 333). 

Sulfenamidothiazoles are obtained from the reaction between 2-aminothiazoles and arylsulfenyl chlorides (see p. 113). 

No systematic study of the free radical reactivity of aminothiazole derivatives has yet been reported. Their behavior, however, may be extrapolated from the detailed work performed on other thiazoles (see Chapter III. Section IX. 1). 

Carbocations derived from the alcohol are probably the reactive species, but data concerning by-products expected with carbocationic intermediates are lacking. Rearrangement of 2-alkylaminothiazoles to 2-amino-5-alkylthiazoles may also explain the observed products 2-aminothiazole with benzyl chloride yields first 2-benz Iaminothiazole (206). which then rearranges to 2-amino-5-benzvlthiazole (207) (Scheme 130) (163. 165. 198). 

Acidic hydrolysis of 2,5-dipheny]-4-aminothiazole similarly gives product 233, resulting from nucleophilic attack on C-4 (Scheme 142) (465). 

Treating 5.5 g of 2-amino-4,5-dimethylthiazole HCl with 0.66 g of solid sodium hydroxide 15 min at 220°C yields 53% of 4.4. 5.5 -tetramethyT 2,2 -dithiazolylamine, whose structure w as proved by identification with the produa obtained from the reaction between dithiobiuret and 3-bromo-2-butanone (467). This result is comparable to the reaction between 2-aminopyridine and its hydrochloride to yield bis(pyridyl-2)amine (468). Gronowitz applied this reaction to 2-aminothiazole, refluxing it with its hydrochloride 4 hr in benzene and obtained the dimeric 2-aminothiazole (236). He proposed a mechanism (Scheme 143) that involves the addition of a proton to the 5-position of the ring to give 234. The carbocation formed then reacts on the 5-position of a second... 

Aminothiazole in its neutral form seems to be able to react in 3 different positions according to the electrophilic center considered (Scheme 146). The question of C-5 reactivity for this neutral form remains open, however, because the observed product might also be formed from the protonated form of 2-aminothiazoles. A surprising... 

These compounds are easily prepared from the appropriate 2-aminothiazole and acyl chloride (see Section III.2.D) or by general heterocydization methods. Acyl chlorides may be replaced by the corresponding anhydrides (471). Acids themselves may be used as acylating agents provided that the imidazole-triphenyl phosphine mixture is used as a catalyst (472). The Curtius degradation of 247 yields 2-acetamido-4-phenylthiazole (248) (Scheme 149) (473). 

Co(II), Ni(n), Cu(n), and Zn(II) complexes of Schiff bases derived from 4-aryl-2-aminothiazoles and salicylaldehyde have been prepared, and structure 276 (Scheme 170) was established by magnetic susceptibility measurements and by infrared, electronic, and mass spectra (512). 

Alkv lation of the appropriate 2-aminothiazole in neutral medium (46, 173, 263 i followed by liberation of the free base from the quaternary salt is also used. The quaternary salt (365) is the starting material for the... 

A wide variety of applications has been proposed for aminothiazole derivatives from fungicides (Table VI-6) to a component of hair-waving lotions containing cosmetic resins for dyeing hair (733). The main applications cover the fields of agriculture, pharmacy, and photography or related activities. This section is only representative, not exhaustive, and can be completed with the indications given in Tables of Section VII. 

Decomposition of diazonium salts obtained from 2-aminothiazole (4) (29, 34. 35) could be an interesting reaction to introduce O in A-4-thiazoline-2-one. Acidic hydrolvsis of ethers (36. 37). oxidative hydrolysis... 

Substitmed A-2-thiazoline-4-ones are much more stable (59. 386. 387. 413, 414). 2.5-Diphenyl-A-2-thiazoline-4-one (173) is obtained in 95% yield from 2.5-diphenyl-4-aminothiazole (172) by heating under reflux with 40% sulfuric acid (Scheme 89) (415). 

Probably first obtained by Hantzsch and Arapides (105) by condensation of a,/3-dichlorether with barium thiocyanate, and identified by its pyridine-like odor, thiazole was first prepared in 1889 by G. Popp (104) with a yield of 10% by the reduction in boiling ethanol of thiazol-2-yldiazonium sulfate resulting from the diazotization of 2-aminothiazole. prepared the year before by Traumann (103). The unique cyclization reaction affording directly the thiazole molecule was described in 1914 by Gabriel and Bachstez (106). They applied the method of cyclization, developed by Gabriel (107, 108), to the diethylacetal of 2-formylamino-ethanal and obtained thiazole with a yield of 62% - Thiazole was also formed in the course of a study on the ease of decarboxylation of the three possible monocarboxylic acids derived from it (109). On the other... 

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