N-Alkylation amines

The treatment of sulfonyl chlorides with ammonia or amines is the usual way of preparing sulfonamides. Primary amines give N-alkyl sulfonamides, and secondary amines give N,N-dialkyl sulfonamides. The reaction is the basis of the Hinsberg test for distinguishing between primary, secondary, and tertiary amines. N-Alkyl sulfonamides, having an acidic hydrogen, are soluble in alkali, while N,N-dialkyl sulfon-... 

The reactions of most of known Nu (tertiary amines, N-alkylated azoles, etc.) with BENA proceed through the pathway (a). This interpretation is additionally confirmed by the fact that the reaction of N-methylimidazole with unsymmet-rical BENA (434a) produces exclusively trimethylsilyl salt (512"), whereas the pathway (b) would afford salt (512 ). 

N-Nitroso-N-alkylhydroxyl-amine, N-Alkyl-hydroxylamine Anwesenheit von H-Donator NO y-NH-OH 106, 119) H... 

Allylic amines N-Alkyl-p-aminothylphos phonium bromides. Bis(methoxycarbonyl)sulfur diimidc. Chloramine-T. N-Chlorosuccinimidc. 

A significant improvement in the alkylation of ketone and aldehyde enamines involves the use of sterically hindered amines . N-Alkylation is prevented with consequent increase in C-alkylation. For example, reaction of the -butylisobutylamine enamine of cyclohexanone (29) with methyl iodide in boiling acetonitrile (Scheme 16), or trimethy-loxonium tetrafluoroborate at room temperature gave 2-methylcyclohexanone in increased yields of 56% and 74%, respectively (compare Scheme 10). 

Moreover, the catalysts promoted by alkaline or alkaline-earth species are more stable than the unpromoted CuCr. For example, barium impregnated on copper chromite increases the stability of the active CuCr02 phase (13). Furthermore, the presence of barium or calcium on copper chromite catalysts influences strongly the selectivity to the methylation of amines N-alkylation/N-methylation. 

When the reaction was carried out in the absence of a tertiary amine, N-alkylation of the isothiazole 84 took place and the 2-(chloroacetyl)isothiazolium chloride 85 was precipitated by the addition of ether (85BSB149, Scheme 26). The treatment of... 

Fragmentations of heterocycles have played an important role in the preparation of amide derivatives. Moderate to good yields of a-hydroxy-amides were obtained on reaction of a-hydroxy-acid aceto-nides with primary amines.N-Alkyl-2-methyl-2-oxazolinium salts (obtained by mixing alkyl halides and 2-methyl-2-oxazoline in dichloromethane) were found to react with sodium benzeneselenolate to yield -(2-phenylselenoethyl)-t -alkylacetamides, which after oxidation to ] -vinyl analogues with sodium metaperiodate in methanol, gave secondary amides on sequential treatment with mercuric acetate in aqueous tetrahydrofuran and sodium borohydride/3M... 

Ohtani B, Osaki H, Nishimoto S, Kagiya T (1986) A novel photocatalytic process of amine N-alkylation by platinized semiconductor particles suspended in alcohols. J Am Chem Soc 108(2) 308-310... 

The reaction is applicable to the preparation of amines from amides of aliphatic aromatic, aryl-aliphatic and heterocyclic acids. A further example is given in Section IV,170 in connexion with the preparation of anthranilic acid from phthal-imide. It may be mentioned that for aliphatic monoamides containing more than eight carbon atoms aqueous alkaline hypohalite gives poor yields of the amines. Good results are obtained by treatment of the amide (C > 8) in methanol with sodium methoxide and bromine, followed by hydrolysis of the resulting N-alkyl methyl carbamate ... 

Purines, N-alkyl-N-phenyl-synthesis, 5, 576 Purines, alkylthio-hydrolysis, 5, 560 Mannich reaction, 5, 536 Michael addition reactions, 5, 536 Purines, S-alkylthio-hydrolysis, 5, 560 Purines, amino-alkylation, 5, 530, 551 IR spectra, 5, 518 reactions, 5, 551-553 with diazonium ions, 5, 538 reduction, 5, 541 UV spectra, 5, 517 Purines, N-amino-synthesis, 5, 595 Purines, aminohydroxy-hydrogenation, 5, 555 reactions, 5, 555 Purines, aminooxo-reactions, 5, 557 thiation, 5, 557 Purines, bromo-synthesis, 5, 557 Purines, chloro-synthesis, 5, 573 Purines, cyano-reactions, 5, 550 Purines, dialkoxy-rearrangement, 5, 558 Purines, diazoreactions, 5, 96 Purines, dioxo-alkylation, 5, 532 Purines, N-glycosyl-, 5, 536 Purines, halo-N-alkylation, 5, 529 hydrogenolysis, 5, 562 reactions, 5, 561-562, 564 with alkoxides, 5, 563 synthesis, 5, 556 Purines, hydrazino-reactions, 5, 553 Purines, hydroxyamino-reactions, 5, 556 Purines, 8-lithiotrimethylsilyl-nucleosides alkylation, 5, 537 Purines, N-methyl-magnetic circular dichroism, 5, 523 Purines, methylthio-bromination, 5, 559 Purines, nitro-reactions, 5, 550, 551 Purines, oxo-alkylation, 5, 532 amination, 5, 557 dipole moments, 5, 522 H NMR, 5, 512 pJfa, 5, 524 reactions, 5, 556-557 with diazonium ions, 5, 538 reduction, 5, 541 thiation, 5, 557 Purines, oxohydro-IR spectra, 5, 518 Purines, selenoxo-synthesis, 5, 597 Purines, thio-acylation, 5, 559 alkylation, 5, 559 Purines, thioxo-acetylation, 5, 559... 

I-Substituted 3,5-Dinitro-4-pyridonyl, 360 SPECIAL -NH PROTECTIVE GROUPS N-Alkyl and A-Aryl Amines... 

A surpnsing feature of the reactions of hexafluoroacetone, trifluoropyruvates, and their acyl imines is the C-hydroxyalkylation or C-amidoalkylaOon of activated aromatic hydrocarbons or heterocycles even in the presence of unprotected ammo or hydroxyl functions directly attached to the aromatic core Normally, aromatic amines first react reversibly to give N-alkylated products that rearrange thermally to yield C-alkylated products. With aromatic heterocycles, the reaction usually takes place at the site of the maximum n electron density [55] (equaUon 5). 

The acid-catalyzed reaction of acetophenone with acyclic secondary amines results in the formation of the expected enamine and a rearrangement product. The latter product arises from the transfer of one of the amino N-alkyl groups to the cnamine s carbon to produce a ketimine (53a). 

Carbamates are formed from an amine with a wide variety of reagents, the chlo-roformate being the most common amides are formed from the acid chloride. n-Alkyl carbamates are cleaved by acid-catalyzed hydrolysis A-alkylamides are cleaved by acidic or basic hydrolysis at reflux and by ammonolysis, conditions that cleave peptide bonds. 

The reaction of potassium phthalimide 1 with an alkyl halide 2 leads to formation of a N-alkyl phthalimide 3/ which can be cleaved hydrolytically or by reaction with hydrazine (Ing-Manske variant) to yield a primary amine 5. This route owes its importance as a synthetic method to the fact that primary amines are prepared selectively, not contaminated with secondary or tertiary amines. 

The solvent for ammonia may have an important influence. In reduction of C,o unsaturated dinitriles to primary amines over ruthenium-on-alumina, ammonia-/-butanol proved the preferred system normal alcohols gave poor rates and secondary alcohols produced N-alkylated products 18). 

Another alternative for preparing a primary amine from an alkyl halide is the Gabriel amine synthesis, which uses a phthalimide alkylation. An imide (—CONHCO—) is similar to a /3-keto ester in that the acidic N-H hydrogen is flanked by two carbonyl groups. Thus, imides are deprotonated by such bases as KOH, and the resultant anions are readily alkylated in a reaction similar to the acetoacetic ester synthesis (Section 22.7). Basic hydrolysis of the N-alkylated imide then yields a primary amine product. The imide hydrolysis step is analogous to the hydrolysis of an amide (Section 21.7). 

This reaction is rapid and can, under anhydrous conditions, be carried out at mild temperatures (60-120°C). The type of leaving group has a strong effect on attainable molecular weights. The polyamide melt syndtesis with dimediyl tereph-thalate has however not been so successful, because N-methylation takes place at high temperatures. This N-methylation is due to die mediyl ester alkylation of die amines and not due to the presence of medianol.28 40 This N-mediylation reaction is significant at temperatures over 200°C. Widi odier esters, N-alkylation takes place to a much lower extent. 

Many pharmacologically active compounds have been synthesized using 5-bromoisoquinoline or 5-bromo-8-nitroisoquinoline as building blocks.6 7 8 9 10 11 The haloaromatics participate in transition-metal couplings 81012 and Grignard reactions. The readily reduced nitro group of 5-bromo-8-nitroisoquinoline provides access to an aromatic amine, one of the most versatile functional groups. In addition to N-alkylation, TV-acylation and diazotiation, the amine may be utilized to direct electrophiles into the orthoposition. 

N-Alkyl-dimethyl-amine konnen in einem Eintopfverfahren aus Isothiocyanaten mit Lithiumalanat und nachfolgendes Kochen mit Ameisensaure-athylester erhalten werden (s.a. S. 242f.)3 ... 

In vielen Fallen erbringt jedoch die Reaktionsfolge ausgehend von einem Carbonsau-re-amid bzw. Lactam bessere Ausbeuten1 4 allerdings muB in diesem Fall das Acyl-amin bereits die gewiinschten N-Alkyl-Gruppen enthalten. 

Die Reduktion von Hydroxylaminen mit Hydriden lauft analog der Reaktion von Nitro-so-Verbindungen bzw. Oximen. N-Alkyl-hydroxylamine werden durch Lithiumanalanat in der Regel zu prim. Aminen umgesetzt8, doch konnen auch Umlagerungen zum sek. Amin ablaufen9. 

In recent studies, we found that primary and secondary amines, alone or somehow faster in the presence of the soft Lewis acid Ag+ (refs. 7-9) substitute the bromine in (S)-2-bromopropanamides, in an organic solvent, at room temperature, and yield N-alkyl-, and N,N -dialky 1-aminopropanamides, with inversion of configuration and high enantiomeric excess. Conversely, in the presence of silver oxide (Ag20), much faster reactions occur with retention of configuration, giving... 

Alkyl halides or sulfuric or sulfonic esters can be heated with sodium or potassium thiocyanate to give alkyl thiocyanates, though the attack by the analogous cyanate ion (10-66) gives exclusive N-alkylation. Primary amines can be converted to thiocyanates by the Katritzky pyrylium-pyridinium method (pp. 447, 489). "... 

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