Benzylamine, methylation

Benzyl alcohol, 23, 14 Benzylamine, methylation of, 26, 91 Benzylamine, a methyl-, 23, 68 Benzyl carbamate, 23,14 Benzyl chlonde, 21, 99 Benzyl chloroformatf, 23,13 Benzyl chlorometiiyl xr toni, 26, 13... 

In general the method is more satisfactory with esters of aromatic acids than with esters of aliphatic acids. Esters of alcohols other than methyl and ethyl are best treated by first converting them into methyl esters thus Heat together under reflux i ml. of the higher ester, 5 ml. of methanol and 0-2 g. of sodium methoxide. [In place of the sodium methoxide, it suffices to add o i g. of metallic sodium to the methanol.] After refluxing, distil off the excess of methanol (b.p, 65 ). The residue is then heated under reflux with benzylamine as described above. 

The reaction (which is essentially the direct aminolysis of esters with benzylamine) proceeds readily when R is methyl or ethyl. Esters of higher alcohols should preferably be subjected to a preliminary methano-lysis by treatment with sodium methoxide in methanol ... 

The methylation of benzylamine (1) and of ammonia (2) are competitive processes by increasing the proportion of hexamine, the source of ammonia, the yield of benzaldehyde is increased and that of metliylbenzylamine is decreased. 

Benzylamine, o-chloro-N-(cyanomethyl)-N-methyl-isoindole synthesis from, 4, 323 Benzylisoquinoline alkaloids synthesis, 1, 446 Benzynes... 

Intramolecular chalcogen interactions may also stabilize reactive functional groups enabling the isolation of otherwise unstable species or their use as transient intermediates, especially in the case of selenium and tellurium. For example, tellurium(II) compounds of the type ArTeCl are unstable with respect to disproportionation in the absence of such interactions. The diazene derivative 15.23 is stabilized by a Te N interaction. Presumably, intramolecular coordination hinders the disproportionation process. Other derivatives of the type RTeX that are stabilized by a Te N interaction include 8-(dimethylamino)-l-(naphthyl)tellurium bromide, 2-(bromotelluro)-A-(p-tolyl)benzylamine, and 2-[(dimethylammo)methyl]phenyltellunum iodide. Intramolecular donation from a nitrogen donor can also be used to stabilize the Se-I functionality in related compounds." ... 

Modification of the Erlenmeyer reaction has been developed using imines of the carbonyl compounds, obtained with aniline," benzylamine or n-butylamine. Ivanova has also shown that an A-methylketimine is an effective reagent in the Erlenmeyer azlactone synthesis. Quantitative yield of 19 is generated by treatment of 3 equivalents of 2-phenyl-5(4ff)-oxazolone (2) (freshly prepared in benzene) with 1 equivalent of iV-methyl-diphenylmethanimine (18) in benzene. Products resulting from aminolysis (20), alkali-catalyzed hydrolysis (21), and alcoholysis (22) were also described. 

I, 4- and 3,4-Dihydroquinazolines are tautomeric but any attempts to prepare the former w ithout a 1-substituent have led to the latter. The greater stability to proto tropic change of 1,2-dihydronaphthalene over 1,4-dihydronaphthalene is also found in 3,4-dihydroquinazoline. Earlier claims to the preparation of l,4-dihydroquinazolines ° were erroneous and based on incomplete experimental data. The first 1,4-dihydroquinazoline was prepared as recently as 1961. 1-Methyl and l-benzyl-l,4-dihydroquinazolines were obtained from o-methylamino-and o-benzylamino-benzylamines (42) by formylation and ring closure. Attempts to remove the benzyl group gave 3,4-dihydroquinazoline. These 1,4-dihydro compounds are susceptible to oxidation, and attempts made to prepare 1,2-dimethyl-1,4-dihydroquinazoline from o-... 

Some substituents such as the acylamino group are readily decomposed by many nucleophiles to give a poorer leaving group (e.g., amino). Others, such as nitroamino and sulfonylamino, are less reactive when they are anionized by the nucleophile. 3-Nitroamino-pyridazine (117) and its 6-methyl derivative are readily aminated with benzylamine (130°, short time ). 4,6-Dimethyl- and 6-methyl-2-nitroaminopyrimidine undergo 2-substitution on warming a few minutes with hydroxylamine, hydrazine, primary or secondary alkylamines, or anilines. 

A -methyl-5//,7//-dibenzo[d,.g][l,5]telluroazocine 65, its thiooxide 67a (X=S, R= Me) (95JA6388). The same type of reaction with benzylamine and sodium selenide gives A-benzyl-5//,7//-dibenzo[d,g][l,5]telluroazocine selenoxide 67b (X = Se, R = CH2Ph). Reaction of the tellurium dibromide 66 with sodium sulfide carried out in the absence of the primary amines affords the eight-member Te,S-containing heterocycle 5//,7//-dibenzo[d,g][l,5]telluroazocine (92CL151). 

Recently, it was found that the addition of benzylamine to 2-(5//)-furano-3-ylmethanesulfonate 280 (X = O—SOaMe) in methanol afforded a 7 1 mixture of the trans- and cw-methyl-A-benzyl-2-hydroxymethylaziridine-2-carboxylates 281 and 282, respectively (00TL3061). Treatment of 281 with benzyl alcohol in the presence of BF3 OEta furnished, after hydrolysis, rac-cw-amino-a-hydroxy-/3-butyrolactone 284 (Scheme 74). 

Thus, condensation of isoniazide with acetone at the basic nitrogen gives the corresponding Shiff base (8). Catalytic reduction affords the antidepressant, iproniazid (9). Addition of the same basic nitrogen to methyl acrylate by Michael condensation leads to the 3-amino ester (10). This is converted to the amide, nialamide (11), on heating with benzylamine. 

A mixture of 23.8 grams (0.2 mol) of propargyl bromide, 24.2 grams (0.2 mol) of N-methyl benzylamine and 400 ml of anhydrous ethanol in the presence of 42.4 grams (0.4 mol) of anhydrous sodium carbonate was heated at the boiling temperature and under reflux for a period of 17 hours. 

The ureas, e.g. 28 (R = NMe2), derived from the corresponding 2-(l-arylviny )benzylamines by reaction with (dimethylamino)carbamoyl chloride (Me2NCOCl) in the presence of triethyl-amine, undergo cyclization in refluxing phosphoryl chloride to the 5-aryl-3-(dimethylamino)-l//-2-benzazepin-3-amines. e.g. 29a.84 Prepared similarly are the 3-(4-methylpiperazin-l-yl) compound 29b and the 3-methyl derivative 29c from the corresponding urea and amide, respectively. 

In contrast, aqueous ethanolic ammonia effects initial nucleophilic displacement of bromide, which is followed by ring closure of the benzylamine so-formed at the aldehyde group to give 5//-dibenz[f, f]azepines 48.85 The (1-bromoethyl) aldehyde 47 undergoes ring closure with benzylamine to give 6-benzyl-5-methyl-5//-dibenz[c t>]azepinium bromide (49, R = Me), whereas the (bromomethyl) aldehyde 45 yields a mixture of the quaternary salt 50 and the aldimine 51, which cyclizes in situ to the aziridinophenanthrene 52 in low yield (9%). 

More recently, other substituted benzylidene derivatives of the enantiomers of a-methyl-benzylamine have been converted with substituted benzaldehydes to the corresponding phenyl-glycinonitriles using sodium cyanide in aqueous methanol44. 

B. Polymeric Urea [Benzene, diethenyl-, polymer with ethenylbenzene, [[[[(1 methylethyl)amino]carbonyt]amino]methyl] deriv.] A 10.0-g. portion of benzylamine polymer beads prepared as in Part A and 125 ml. of tetrahydrofuran (Note 6) are combined in a 300-ml., three-necked, round-bottomed flask equipped with a magnetic stirrer, a dropping funnel, and a condenser fitted with a gas-inlet tube A nitrogen atmosphere is established in the system, and the slurry is stirred while 1.35 g. (0.0159 mole) of isopropyl isocyanate [Propane, 2-isocyanato-] is added. This causes an exothermic reaction, which subsides after about 20 minutes. The mixture is then stirred at room temperature for 22 hours and at reflux for an additional 4 hours. The beads are collected by filtration, washed with 150-ml. portions of tetrahydrofuran (Note 6) and methanol, and dried under reduced pressure over calcium chloride to yield 9.09 g, of the isopropyl urea polymer. 

Analog erhalt man aus 4-Methyl-benzoesaure-nitril 4-Methyl-benzylamin (63% d.Th.). 

Bis - [2-methyl-propyl]-aluminiumhydrid und Tris-[2-methyl-propyl]-aluminium reduzieren Nitrile zu primaren Aminen3,4 (z.B.Benzylamin s. Bd. XIII/4, S. 221), Dinitrile zu 1, [Pg.112]

Dioxo-4,8-diphenyl-l,3,5,7-tetraaza-bicyclof3.3.0]octan laBt sich durch Lithium-alanat in5-Hydroxy-3- phenyl-1,2,4- triazolidin (14% d.Th.), N-Methyl- benzylamin auf-spalten4 ... 

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