Substituted anilines, preparation

A convenient method for preparing pure AW-dialkyl anilines and substituted anilines directly from the corresponding amines consists in heating the latter with trialkyl orthophosphates ... 

FrielA,nderSynthesis. The methods cited thus far all suffer from the mixtures which usually result with meta-substituted anilines. The use of an ortho-disubstituted benzene for the subsequent constmction of the quinoline avoids the problem. In the FrieWider synthesis (52) a starting material like 2-aminoben2aldehyde reacts with an CX-methyleneketone ia the presence of base. The difficulty of preparing the required anilines is a limitation ia this approach, but 2-nitrocarbonyl compounds and the subsequent reduction of the nitro group present a usehil modification (53). 

The Gassman indole synthesis provides a single regioisomer when ortho/para substituted anilines are employed, the yields of which are quite good generally. This provides some advantage in the preparation of 7-substituted indoles compared to other methods which normally give low yields, that is, the Fischer indole process. ... 

The key intermediate for the preparation of the 8-aminoquin-oline antimalarial agents is obtained by condensation of the substituted aniline, 90, with "dynamite-grade" glycerol in concentrated sulfuric acid. (The reaction may well follow some scheme such as that depicted below.) Ihe nitroquinoline obtained from... 

B) Preparation of 4-Amino-2-Chloro-5-(Methylsulfamyl)Benzenesulfonamide The 5-sub-stituted-2,4-dlsulfamyl anilines may be prepared by procedures described in the literature, for example, the general procedures in Monatsch. Chem. vol. 48, p 87 (1927), which involves the treatment of a m-substituted aniline with from 10 to 20 parts by weight of chlorosulfonic acid followed by the gradual addition of from about 90 to 170 parts by weight of sodium chloride. The resultant mixture is heated at approximately 150°C for about 2 hours after which the reaction mixture is poured into water and the resultant 5-substituted aniline-2,4-disulfonyl chloride is filtered and is then treated with concentrated ammonium hydroxide or suitable amine by standard procedures to obtain the corresponding disulfonamide. 

Chloroquinoxaline with appropriate substituted anilines gave 2-(substituted anihno)quinoxalines (preparative and kinetic aspects were measured in MeOH and EtOH at various precise temperatures). ... 

For the synthesis of quinolines and isoquinolines the classical approaches are the Skraup and the Bischler-Napieralski reactions. The reaction of substituted anilines with different carbonyl compounds in acid medium has been reported to be accelerated under microwave irradiation to give differently substituted quinolines and dihydro quinolines [137]. Although the yields are much better and the conditions are milder than under conventional heating, the acidity of the medium may prevent the preparation of acid-sensitive compounds. Thus, alternative approaches have been investigated. Substituted anilines and alkyl vinyl ketones reacted under microwave irradiation on the surface of sihca gel doped with InCU without solvent [137] to furnish good yields of quinohnes 213 (Scheme 77). 

The bidentate ligands were prepared by the Schiff-base condensation of two equivalents of the desired 2,6-dialkyl substituted anilines with acenaphthenequinone as in the scheme 1, The pre-catalysts, formed by addition of the ligand to (DME)NiBr2 are isolated and purified. The products were characterized by h, C NMR, GPC, DSC and Elemental Analysis. 

The synthesis of this aminoquinoline starts with one of the standard sequences for preparation of 4-hydroxyquinolines, i.e., with the formation of the Shiff base (5) from the appropriately substituted aniline and diethyl oxaloacetate. Thermal cycliza-tion gives the quinolone (6) this then spontaneously tautomerizes to the enol form (7). Saponification followed by decarboxylation gives the desired quinolol... 

The Skraup cyclization is another reaction principle that provides rapid access to the quinoline moiety. Theoclitou and Robinson have published the preparation of a 44-member library based on the 2,2,4-trisubstituted 1,2-dihydroquinoline scaffold by the Lewis acid-catalyzed cyclization of substituted anilines or aminoheterocyc-les with appropriate ketones (Scheme 6.237) [420], The best results were obtained using 10 mol% of scandium(III) triflate as a catalyst in acetonitrile as solvent at... 

The use of heterocyclic diazo components is particularly important in the preparation of blue disperse dyes. It is often difficult to prepare, diazotise and/or couple the highly electronegatively substituted diazo components of the benzene series needed to achieve blue hues, and feebly basic aminoheterocycles offer a convenient alternative. The small molecular size of these heterocyclic amines, compared with that of heavily substituted anilines, is another factor favouring their use. 

There are relatively few methods available for the preparation of condensed 1,2,3-triazines. By far the most commonly employed procedure is diazotization of a suitably ortho-substituted aniline (4) or amino-substituted heterocycle of the type 5, and examination of the different X substituents which have been used successfully in this synthesis reveals... 

There are a number of important reactions in this category and all of them involve at least one heteroatom functioning as a nucleophile and another as an electrophile. Diazo-tization of a variety of ortho-substituted anilines for instance, followed by intramolecular nucleophilic trapping of the corresponding diazonium salts by either nitrogen or carbon nucleophiles, is the basis of a series of very important syntheses of 1,2,3-benzotriazine and cinnoline derivatives, and this general approach has been widely exploited for the preparation of polycyclic systems. Representative examples are given in equations (51)—(54). 

The Lewis acid-catalyzed three-component reaction of dihydropyridines, aldehydes, and />-substituted anilines efficiently yields highly substituted tetrahydroquinolines in a stereoselective manner, through a mechanism believed to be imine formation followed by formal [4-1-2] cycloaddition (Scheme 41). The 1,4-dihydropyridine starting materials were also prepared in situ by the nucleophilic addition of cyanide to pyridinium salts, creating in effect a one-pot four-component reaction <20030L717>. 

Oxyindoles are prepared using a modified Gassman synthesis from the chlorosulfonium salt 167 on reaction with substituted anilines <1996TL4631> (Equation 92). 

One of the earlier second-generation quinolones indeed includes fluorine at the 6 position and a basic function at the 7 position, characteristic of the more potent drugs that also feature a broader spectmm of antibacterial activity. The starting material (39-3) for one of these agents is prepared by application of the same scheme as above to the substituted aniline (39-1). Nucleophilic aromatic displacement with A-methylpiperazine (39-4) proceeds at the 7 position due to activation by the carbonyl group para to the chlorine (39-5). Saponification of the displacement product leads to pefloxacin (39-6) [46]. 

The important methods involve ring closure of o-substituted anilines and phenols (type 108) and cyclization of o-unsubstituted aniline, etc., derivatives (type 109). Additionally, cycloadditions and transformations from other heterocycles are considered. Table 2 gives an overview of the important methods for preparation of derivatives of these types. 

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