Amines by reductive amination with

Formyl-pinane can be isolated from the aldehyde mixture as pure compound in moderate yield by distillation with a column of 20 trays [70a]. In turn, the aldehyde was converted into the primary amine by reductive amination with ammonia. The chiral amine has been utilized, for example, for the optical resolution of racemic pantolactone. Alternatively, aldol condensation of the formed aldehydes with ketones and subsequent hydrogenation give alcohols that might have a broad scope of potential applications in perfumes, soaps, and shampoos [73]. 

Yields dropped notably, when this procedure was applied to synthesize branched polyamines. This comes from the slow reduction rate of the tertiary amide that leads mainly to only partially reduced side products, even after 5 days at 65 °C. The problem was satisfactorily solved for ahphatic substituents by alkylating the secondary amine by reductive amination with aldehydes using NaBHAcs as an additional hydride source. 

The dimethoxybenzyl group was used for backbone protection of the pseudopeptides of the form Xaai/r(CH2N)Gly (Xaa = amino acid). It is introduced by reductive alkylation with the aldehyde and NaCNBH3. Acidolysis with TFMSA in TFA/thioanisole is used to remove it from the amine, but the efficiency is dependent upon the peptide sequence. ... 

Amino acids were protected by reductive alkylation with salicylaldehyde (NaBH4, KOH, aq. EtOH). The amine is released by treatment with CF3SO3H (TFA, EDT, PhSMe, 2 h, >75% yield). ... 

Protection of primary aryl amines as the triazene is accomplished by diazotiza-tion of the amine followed by reaction with pyrrolidine in aq. KOH. This group is stable to metalation of the aromatic ring by metal halogen exchange. The amine is recovered by reductive cleavage with Ni-Al alloy (aq. KOH, rt, 37-68% yield). ... 

The synthesis of a triptan with a chiral side chain begins by reduction of the carboxylic acid in chiral 4-nitrophenylalanine (15-1). The two-step procedure involves conversion of the acid to its ester by the acid chloride by successive reaction with thionyl chloride and then methanol. Treatment of the ester with sodium borohy-dride then afford the alanilol (15-2). Reaction of this last intermediate with phosgene closes the ring to afford the oxazolidone (15-3) the nitro group is then reduced to the aniline (15-4). The newly obtained amine is then converted to the hydrazine (15-5). Reaction of this product with the acetal from 3-chloropropionaldehyde followed by treatment of the hydrazone with acid affords the indole (15-6). The terminal halogen on the side chain is then replaced by an amine by successive displacement by means of sodium azide followed by catalytic reduction of the azide. The newly formed amine is then methylated by reductive alkylation with formaldehyde in the presence of sodium cyanoborohydride to afford zolmitriptan (15-7) [15]. 

Aliphatic primary and secondary amines can be linked to insoluble supports as ben-zylamines by reductive alkylation with support-bound benzaldehydes or by N-alkyla-tion with support-bound benzyl halides or sulfonates (Figure 3.25 see also Section 10.1). Benzhydrylamines and tritylamines are usually prepared by N-alkylation with the corresponding halides. 

Cyclohexene is converted to tnmv-1-(4-mcthylphcnylsulfonylamino)-2-(phenylseleno)cyclohexane (59) by treatment with diphenyl diselenide and chloramine-T, followed by reductive workup with sodium borohydride66. The intermediate product A formed from diselenide and chlor-amine-T is believed to play the role of an electrophile attacking the alkene. 

SCHEME 18. Trans-sialylation using MUNeu5Ac derivatives prepared by periodate oxidation followed by reductive animation with various primary amines. 

AC2O. It is cleaved by methanolysis with NaOMe/MeOH to open the ring followed by reductive desulfurization with Bu SnH/AIBN. This leaves the amine protected as an acetamide. ... 

The amine is recovered by reductive cleavage with Ni-Al alloy (aq. KOH, rt, 37-68% yield). ... 

Kirschning and coworkers have recently reported the synthesis of a resin-bound diketone for the sequestration of amines and hydrazines [14]. The resin-bound diketone was synthesized via oxidation of a chloromethyl resin, followed by reductive coupling with 2,4-pentadione, to provide the requisite scavenger resin. This resin was found to be more efficient than supported-aldehydes for amine and hydrazine scavenging and, furthermore, found to be selective for the scavenging of primary amines over secondary amines (Scheme 8.10). 

Benzylamines and the chloro or bromo substituted anilines cannot be applied in the Buchwald Hartwig reaction and this is another limitation. These limitations can be overcome by triazene-linked anilines. On one hand, the amine could be benzylated by reductive alkylation with benzaldehydes, or on the other hand, be used for an inverse Buchwald-Hartwig reaction, e.g. with dichlorobenzenes for the assembly of chloroanilines. 

Azo-compounds can be obtained by reduction of nitro-compounds, or by oxidation of hydrazo-compounds. They are usually prepared, however, by reacting a phenol or amine with a diazonium salt. The coupling usually takes place in the position para to the hydroxyl or amino group, but if this position is occupied it goes to the ortho position, e.g. 

SchifT s bases A -Arylimides, Ar-N = CR2, prepared by reaction of aromatic amines with aliphatic or aromatic aldehydes and ketones. They are crystalline, weakly basic compounds which give hydrochlorides in non-aqueous solvents. With dilute aqueous acids the parent amine and carbonyl compounds are regenerated. Reduction with sodium and alcohol gives... 

Aldehydes and ketones may be converted into the corresponding primary amines by reduction of their oximes or hydrazones (p. 93). A method of more limited application, known as the Leuckart Reaction, consists of heating the carbonyl compound with ammonium formate, whereby the formyLamino derivative is formed, and can be readily hydrolysed by acids to the amine. Thus acetophenone gives the i-phenylethylformamide, which without isolation can be hydrolysed to i-phenylethylamine. 

Dissolve 0-5 g. of the substance in 10 ml. of 50 per cent, alcohol, add 0-5 g. of solid ammonium chloride and about 0 -5 g. of zinc powder. Heat the mixture to boiling, and allow the ensuing chemical reaction to proceed for 5 minutes. Filter from the excess of zinc powder, and teat the filtrate with Tollen s reagent Section 111,70, (i). An immediate black or grey precipitate or a silver mirror indicates the presence of a hydroxyl-amine formed by reduction of the nitro compound. Alternatively, the filtrate may be warmed with Fehling s solution, when cuprous oxide will be precipitated if a hydroxylamine is present. Make certain that the original compound does not aflfect the reagent used. 

Secondary and tertiary amines are not generally prepared in the laboratory. On the technical scale methylaniline is prepared by heating a mixture of aniline hydrochloride (55 parts) and methyl alcohol (16 parts) at 120° in an autoclave. For dimethylaniline, aniline and methyl alcohol are mixed in the proportion of 80 78, 8 parts of concentrated sulphuric acid are added and the mixture heated in an autoclave at 230-235° and a pressure of 25-30 atmospheres. Ethyl- and diethyl-anihne are prepared similarly. One method of isolating pure methyl- or ethyl-aniline from the commercial product consists in converting it into the Y-nitroso derivative with nitrous acid, followed by reduction of the nitroso compound with tin and hydrochloric acid ... 

The less hindered f/ans-olefins may be obtained by reduction with lithium or sodium metal in liquid ammonia or amine solvents (Birch reduction). This reagent, however, attacks most polar functional groups (except for carboxylic acids R.E.A. Dear, 1963 J. Fried, 1968), and their protection is necessary (see section 2.6). 

As another example of nitrene formation, the reaction of o-nitrostilbene (96) with CO in the presence of SnCU affords 2-phenylindole (97). The reaction is explained by nitrene formation by deoxygenation of the nitro group with CO, followed by the addition of the nitrene to alkene. Similarly, the 2//-indazole derivative 99 was prepared by reductive cyclization of the A-(2-nitrobenzyli-dene)amine 98[89]. 

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