Nitro amides, reduction

Amide Cleavage Induced by Nitro Group Reduction... 

Very often reduction of an aromatic nitro compound is carried out in the presence of acetic anhydride, whereby the corresponding acetamido compound is formed. Amino amides are prepared by catalytic hydrogenation of nitro amides, e.g., 2-aminoacetanilide (90%). ... 

Aqueous reductions are useful for amine synthesis. Organic reducing agents (N H or formic acid) reduce amides or imines . Active metals in acid reduce nitro groups . Reduction of Ph3PNBr with I ... 

Amathamides A (108) and B (109) were synthesized by Osuna et al. from 3-hydroxybenzaldehyde 120 and it is depicted in Scheme 10 [58], In the synthetic sequence, aldehyde 120 was converted into required dibromomethoxybenzaldehyde 121 via bromination followed by methylation. Then aldehyde 121 was converted into amine 123 on nitroolefination followed by Michael addition and nitro group reduction (Scheme 10) [58], Amine 123 was coupled with A-methyl-L-proline to get amide 124. 

The imides, primaiy and secondary nitro compounds, oximes and sulphon amides of Solubility Group III are weakly acidic nitrogen compounds they cannot be titrated satisfactorily with a standard alkaU nor do they exhibit the reactions characteristic of phenols. The neutral nitrogen compounds of Solubility Group VII include tertiary nitro compounds amides (simple and substituted) derivatives of aldehydes and ketones (hydrazones, semlcarb-azones, ete.) nitriles nitroso, azo, hydrazo and other Intermediate reduction products of aromatic nitro compounds. All the above nitrogen compounds, and also the sulphonamides of Solubility Group VII, respond, with few exceptions, to the same classification reactions (reduction and hydrolysis) and hence will be considered together. 

Reduction of an azide a nitrile or a nitro compound furnishes a primary amine A method that provides access to primary secondary or tertiary amines is reduction of the carbonyl group of an amide by lithium aluminum hydride... 

The preparation of amines by the methods described m this section involves the prior synthesis and isolation of some reducible material that has a carbon-nitrogen bond an azide a nitrile a nitro substituted arene or an amide The following section describes a method that combines the two steps of carbon-nitrogen bond formation and reduction into a single operation Like the reduction of amides it offers the possibility of prepar mg primary secondary or tertiary amines by proper choice of starting materials... 

AletalHydrides. Metal hydrides can sometimes be used to prepare amines by reduction of various functional groups, but they are seldom the preferred method. Most metal hydrides do not reduce nitro compounds at all (64), although aUphatic nitro compounds can be reduced to amines with lithium aluminum hydride. When aromatic amines are reduced with this reagent, a2o compounds are produced. Nitriles, on the other hand, can be reduced to amines with lithium aluminum hydride or sodium borohydride under certain conditions. Other functional groups which can be reduced to amines using metal hydrides include amides, oximes, isocyanates, isothiocyanates, and a2ides (64). 

Most ring syntheses of this type are of modern origin. The cobalt or rhodium carbonyl catalyzed hydrocarboxylation of unsaturated alcohols, amines or amides provides access to tetrahydrofuranones, pyrrolidones or succinimides, although appreciable amounts of the corresponding six-membered heterocycle may also be formed (Scheme 55a) (73JOM(47)28l). Hydrocarboxylation of 4-pentyn-2-ol with nickel carbonyl yields 3-methylenetetrahy-drofuranone (Scheme 55b). Carbonylation of Schiff bases yields 2-arylphthalimidines (Scheme 55c). The hydroformylation of o-nitrostyrene, subsequent reduction of the nitro group and cyclization leads to the formation of skatole (Scheme 55d) (81CC82). 

A series of amides has been prepared as protective groups that are cleaved by intramolecular cyclization after activation, by reduction of a nitro group, or by activation by other chemical means. These groups have not found much use since the first edition of this volume and are therefore only listed for completeness. The concept is generalized in the following scheme ... 

The alkylation of enamines with nitroolefins, which gives intermediates for reductive cyclization (6S2), also provided an example of a stable cycliza-tion product derived from attack of the intermediate imonium function by the nitro anion (683). A previously claimed tetrasubstituted enamine, which was obtained from addition of a vinylsulfone to morpholinocyclohexene (314), was shown to be the corresponding cyclobutane (684). Perfluoro-olefins also gave alkylation products with enamines (685). Reactions of enamines with diazodicarboxylate (683,686) have been used diagnostically for 6-substituted cyclohexenamines. In a reaction of 2-penten-4-one with a substituted vinylogous amide, stereochemical direction was seen to depend on solvent polarity (687). 

Acylation of a sulfonamide on the amide nitrogen serves to remove the sometimes objectionable taste of these drugs. Reac-I ion of intermediate, 154, with acetic anhydride followed by reduction of the nitro group affords acetyl methoxyprazine (156). The last, which has much the same biologic action as Mie parent compound, is used for oral administration in syrups. 

A heterocyclic ring may be used in place of one of the benzene rings without loss of biologic activity. The first step in the synthesis of such an agent starts by Friedel-Crafts-like acylation rather than displacement. Thus, reaction of sulfenyl chloride, 222, with 2-aminothiazole (223) in the presence of acetic anhydride affords the sulfide, 224. The amine is then protected as the amide (225). Oxidation with hydrogen peroxide leads to the corresponding sulfone (226) hydrolysis followed by reduction of the nitro group then affords thiazosulfone (227). ... 

Replacement of chlorine on the pendant benzoyl group by azide is apparently consistent with antiinflammatory activity. Acylation of indomethacin intermediate with p-nitrobenzoyl chloride leads to the corresponding amide (7). Saponification ( ) followed by reduction of the nitro group gives the amine 9. The diazonium salt (10) obtained on treatment with nitrous acid is then reacted with sodium azide there is thus obtained zidomethacin (11). 

Reductions of nitronitriles situated to favor interaction are apt to involve both functions (S4,93). Hydrogenation of o-nitrobenzonitrile over either palladium or platinum gave o-aminobenzamide (78), with the amide oxygen transferred from the nitro group (66). On the other hand, l-amino-2-cyanonaphthalene gave the amino amide on reduction over Pt02, but the amino nitrile over palladium (82). 

Amide (1) was needed for a synthesis of an isoquinoline. Disconnecting the amide reveals the amine (2) which could be made by reduction of an unsaturated nitro compound. The a, -disconnection is simple. 

In our second approach, we considered reversal of these functional group transformations, wherein reduction of the nitro group followed by palladium-mediated intramolecular amidation would provide the desired tricylcic lactam (Scheme 6.6). One concern with this approach, however, was to identify reaction conditions that would selectively reduce the nitro functionality and not lead to... 

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