Isothiazoles preparation

Alkyl- and arylthiazoles rearrange undernltraviolel irradiation in different solvents to yield the corresponding isothiazoles or isomeric thiazoles. With alkylthiazoles the overall yields are very low, and it is not possible to use this method preparatively. For arylthiazoles it is possible 2-arylthiazoles. for instance, can be used to prepare 3-arylisothiazoles that are otherwise very difficult to obtain. 

In contrast to thiazoles, certain isothiazoles and benzisothiazoles have been directly oxidized to sulfoxides and sulfones. 4,5-Diphenyl-l,2,3-thiadiazole is converted by peracid into the trioxide (146). Although 1,2,5-thiadiazole 1,1-dioxides are known, they cannot be prepared in good yield by direct oxidation, which usually gives sulfate ion analogous to the results obtained with 1,2,4- and 1,3,4-thiadiazoles (68AHC 9)107). 

Lithioisothiazoles are readily prepared by the action of butyllithium, and the isothiazole ring is desulfurized by Raney nickel (see Section 4.02.1.8). Few cycloaddition reactions are known. 

In an attempt to prepare an isothiazolobenzodiazepine, ethyl 5-o-aminoanilino-3-methyl-isothiazole-4-carboxylate was treated with sodium methoxide, but the only reaction was transesterification to the methyl ester 76UC(B)394). Only the 5-ester group of dimethyl 3-methylisothiazole-4,5-dicarboxylate reacts with iV,iV -diphenylguanidine, as with the corresponding isoxazole compound, but the product could not be cyclized, even under drastic conditions. This is in marked constrast to the isoxazole compound which cyclized at room temperature (80JCS(P1)1667). 

A few isothiazoles, 2,1-benzisothiazoles and monocyclic sultams have been prepared by methods involving formation of the 4,5-bond. Thus, condensation of a-cyanooximes (179) with ethyl mercaptoacetate or related compounds gives a compound (180) which cyclizes... 

Cephalosporin 5-oxides and penicillin 5-oxides (221) can be converted into isothiazol-3-ones (222) by the action of bases. These reactions proceed via an intermediate azetidinonesulfenic acid (223 Scheme 37) (77SST(4)339). Attempts to prepare /3-lactam compounds from isothiazoles have, as yet, been unsuccessful (81X2181). 

Isothiazole itself is best prepared by the reaction between propynal, ammonia and sodium thiosulfate (see Section 4.17.9.3). A wide range of substituted mononuclear isothiazoles can be obtained by oxidative cyclization of y-iminothiols and related compounds (see Section 4.17.9.1.1). Substituents at the 3-position need to be in place before cyclization, but 4-substituents are readily introduced by electrophilic reagents (see Section 4.17.6.3), and 5-substituents via lithiation (see Section 4.17.6.4). 

There are many references in the patent literature to azo dyes prepared from 4- and 5-aminoisothiazoles, 3-, 5- and 7-amino-1,2-benzisothiazoles, and their quaternized derivatives. These are particularly useful in the dyeing of synthetic fibres. Isothiazole compounds have also been suggested for other industrial purposes, such as corrosion inhibitors, fireproofing agents, additives in rubber vulcanization, photographic chemicals and fluorescent whiteners in detergents. 

Isothiazole is the sulfur analogue of isoxazole. No member of the group is known. A necessary condition for the development of this field is the preparation of the unknown thiohydroxylamine. This reasonable assessment of the position in 1947 was not in fact true. 

The chemistry of mononuclear isothiazoles has been developed since 1956 without the aid of thiohydroxylamine, the preparation of this very unstable substance having only recently been reported. Bicyclic and polycyclic systems involving the isothiazole (1,2-thiazole) structure have long been known and were fully reviewed in 1952, but little new work has been reported since then and the present review... 

Adams and Slack s second isothiazole synthesis involved the preparation of j3-iminothiobutyramide (9) from the nitrile 8 and cycliza-... 

On the laboratory scale, isothiazole is most conveniently prepared by the acetylenic route.On the other hand, the olefinic route has... 

Formyl- and 4-bromo-3-formyl-isothiazole have been prepared in good yield from the dibromomethyl compounds obtained by side-chain halogenation of the appropriate 3-methylisothiazole with N-bromosuccinimide. 3-Acetyl- and 3-acetyl-4-bromo-isothiazole have been prepared from the 3-cyanoisothiazoles and methyl magnesium iodide. ... 

Isothiazole forms the carbenes upon treatment of its lithium salt with [CfiF5Au(THT)] and methyl triflate while the C-coordinated complex formed before methylation was not isolated. When [Ph3PAuCl] is used as the precursor, both C-coordinated complex and then carbene can be prepared (95JCS(D)2067). 

Isothiazoles can be prepared from thionyl chloride and a-aminoketones, a-iminoketones, a-iminonitriles, or acrylonitriles the reactions concerned have been discussed.62... 

Naphtho[l,2-c]isothiazole (52) and its [2,1-c] isomer (53) can be prepared from the corresponding methylnaphthaleneamines by a reaction similar to that described above the linear isomer (54) is not obtainable in this way.65... 

Individual aspects of nitrile oxide cycloaddition reactions were the subjects of some reviews (161 — 164). These aspects are as follows preparation of 5-hetero-substituted 4-methylene-4,5-dihydroisoxazoles by nitrile oxide cycloadditions to properly chosen dipolarophiles and reactivity of these isoxazolines (161), 1,3-dipolar cycloaddition reactions of isothiazol-3(2//)-one 1,1-dioxides, 3-alkoxy- and 3-(dialkylamino)isothiazole 1,1-dioxides with nitrile oxides (162), preparation of 4,5-dihydroisoxazoles via cycloaddition reactions of nitrile oxides with alkenes and subsequent conversion to a, 3-unsaturated ketones (163), and [2 + 3] cycloaddition reactions of nitroalkenes with aromatic nitrile oxides (164). 

Aromatic pyrrolo[ 1,2-A isothiazoles are not known and only a sulfone analog of tetrahydro and one perhydro derivative have been prepared. 

A series of five-membered heterocycles with two and three heteroatoms were synthesized. 4-Hydroxyisothiazoles 57 were prepared from a-amino ketones with sulfur monochloride (1968BCJ959). Polar solvents, especially N,Af-dimethylfor-mamide, were preferable (Scheme 28). In a similar reaction of 1-amino-l-phenyl-2-propanone with sulfur monochloride 5-chlorinated isothiazole 58 was obtained in high yield. 

The standard means for preparing oxicams 285, initially developed by Lombardino, is through the base-promoted rearrangement reaction of isothiazole dioxides 286, which in turn are prepared from saccharin derivatives such as 287 (Scheme 40) <1981AHC(28)73>. The oxicam core can be further derivatized by N-alkylation of oxicam 285 and amidation of the C-3 ester functionality of 288 to form the common drug scaffold 289. 

A series of bicyclic isothiazole-S-oxides 8 were prepared by reaction of fused 1,2-dithole-S-oxides 7 with a range of primary amines via an S/N exchange reaction <99JHC161>. 

Rees and co-workers in their study of the reactions of trithiazyl trichloride in the preparations of heterocyclic compounds have noted that the isothiazolo[5,4-, isothiazole compound 140 was produced in low yield on reaction with conjugated dienes, along with the other heterocyclic systems 142-145 in much higher yields (Equation 28). Since it is known that trithiazyl trichloride is in thermal equilibrium with its monomer NSCl (Equation 29), the authors propose the so-called criss-cross cycloaddition reaction (Equation 30) which has been reported for azabu-tadienes, but this represents the first example of such a criss-cross cycloaddition to an all-carbon diene <1998CC1207>. 

Much has been said about the application of this heterocyclic system in supramolecular chemistry and in materials chemistry, particularly in the preparation of organic conductors and superconductors. It should not be forgotten however that heterocyclic compounds in general are extremely important medicinal compounds. Although medicinal applications of this heterocyclic system have been rare in the years since CHEC-II(1996), some have been reported. Townsend and co-workers have described the preparation of imidazo[4,5-r/ isothiazole nucleosides 174-177 and have demonstrated their properties as antiproliferative and antiviral analogues of the antibiotic nebularine 172 and the highly cytotoxic 6-methylpurine nucleoside 173 <1997JME771>. 

Isothiazole synthesis Isothiazole can be prepared from thioamide in the following way. 

---