Hydrazines 3-amino

So erhiilt man aus 2-Mercapto-5-(4-pyridyl)-l,3,4-oxadiazolen mit Hydrazin 3-Amino-2-mer-capto-5-(4-pyridylJ-i,2,4-lriazol [55% Schmp. 240° (Zers.)]714 ... 

Oxidation of the 1,1-disubstituted hydrazine, 3-amino-2-oxazolidinone (1), with bromine water, with potassium iodate-HN03, or with potassium bromate in 6 N HC1 affords a compound melting at 299° and now recognized as the trans-3,3 -azobis(2-oxazolidinone) of formula (2). Forgione et al. 5 explored oxidation with yellow mercuric oxide in dioxane or THF at 25° and obtained an isomeric product, m.p. 171°, in 50% yield along with a little of the trans isomer (2). Infrared, UV,... 

The reactions of 3-amino groups in pyridines and 5-amino groups in pyrimidines, by contrast, are close to those of the amino group in aniline. The diazonium salts are reasonably stable and undergo coupling and replacement reactions and can be reduced to hydrazines. Amino groups in the 3-position of isoquinolines (727) are subject to bond fixation and react in a manner intermediate between those of a- and p-amino groups they can be diazotized under the conditions normally employed. 

In our opinion, the reactions of chalcones 141 with some or /zo-diamines containing a hydrazine amino group (1,2-diaminobenzimidazole 142, 3,4-diaminotriazoles 143 and 1,2,4-triaminotriazoles 144) [122, 123, 124] are more interesting from both a practical and a theoretical viewpoint. The possibility to obtain the derivatives of azolopyrimidine 145—147 but not the triazepine systems in such reactions was demonstrated [124]. In this case the cyclocondensation is accompanied by the elimination of not only a molecule of water but also a molecule of ammonia. The proposed mechanism of the cyclocondensation [122] implies formation of a dihydroazolopyrimidine system with its subsequent heteroaromatization by amino-group elimination (Scheme 4.45). 

The reaction of 4,5-diphenylimidazole-1,2-diamine 152 with substituted chalcones 153 in dimethylformamide for 1 h proceeds with the elimination of the hydrazine amino group, oxidation and formation of the appropriate 2,3,5,7-tetraaryl-5,6-dihydroimidazo[l,2-a]pyrimidin-6-ol 154 in low or moderate yields [126] (Scheme 4.47). The treatment of the same diamine with dibromo derivatives 155 produced imidazo[l,2-a]pyrimidines 156 [126]. 

Compounds of the general formula 1 (Scheme 1) containing a hydrazine amino acid (Saragovi et al., 1991 Kahn, 1993) represent a landmark in the development of biologically active 0-turn mimetics [16]. Compound 2 imi-... 

Hydrazine perchlorate/hydrazine/amino alcohol/ water 60.2/9.3/10.0/20.5 1.38... 

The renaissance of the catalytic Ullmann coupling has also led to numerous new methods allowing the condensation of aryl iodides and bromides, with aliphatic amines, anilines, hydrazines, amino alcohols, noncyclic amides, and other substrates (Scheme 3). 

The modified procedure involves refluxing the N-substituted phthaUmide in alcohol with an equivalent quantity of hydrazine hydrate, followed by removal of the alcohol and heating the residue with hydrochloric acid on a steam bath the phthalyl hydtazide produced is filtered off, leaving the amine hydrochloride in solution. The Gabriel synthesis has been employed in the preparation of a wide variety of amino compounds, including aliphatic amines and amino acids it provides an unequivocal synthesis of a pure primary amine. 

Supplement 1953 3242-3457 Hydroxy-carboxylic acids, 190 In i doxylic acid, 226. Carbonyl-carboxylic acids, 284. i Sulphonic acids, 386 Quinoline sul-phonic acid, 390. Amines, 419 2-Aminopyridine, 428. Amino-carboxylic acids, 541 Tryp- tophane, 545. Hydrazines, 563. Azo. compounds, 572. Diazo compounds, 590. ... 

Supplement 1955 3634-3793 Sulphonic acids Indigo-disulphonic acid (indigocarmine), 304. Amines, 308. Keto-ammes Pyramidone, 452. Allan-toin, 474. Murexide, 499. Amino-carboxylic acids Histidine, 513. j Hydrazines, 531. Azo compounds, 535. 1... 

Benzylthio or 2-benzyloxy derivatives of A-2-thiazoline-5-one (224) are readily opened by amines to give the amide derivatives (225) (Scheme 115) (459. 471). Compound 225 can be cyclized thermally to the corresponding thiohydantoins (459). Similarly, treatment of 4-substituted-2-phenylthiazol-5(4H)-ones (226) with amino acids, peptides, or hydrazine affords the corresponding Nfcti-thiobenzamidoacetylated derivatives (227) (Scheme 116) (455). 

This reaction forms the basis of one method of terminal residue analysis A peptide is treated with excess hydrazine in order to cleave all the peptide linkages One of the terminal amino acids is cleaved as the free amino acid and identified all the other ammo acid residues are converted to acyl hydrazides Which amino acid is identified by hydrazmolysis the N terminus or the C terminus ... 

Aluminum chloride [7446-70-0] is a useful catalyst in the reaction of aromatic amines with ethyleneknine (76). SoHd catalysts promote the reaction of ethyleneknine with ammonia in the gas phase to give ethylenediamine (77). Not only ammonia and amines, but also hydrazine [302-01-2] (78), hydrazoic acid [7782-79-8] (79—82), alkyl azidoformates (83), and acid amides, eg, sulfonamides (84) or 2,4-dioxopyrimidines (85), have been used as ring-opening reagents for ethyleneknine with nitrogen being the nucleophilic center (1). The 2-oxopiperazine skeleton has been synthesized from a-amino acid esters and ethyleneknine (86—89). 

Amino-4-nitropheno1 is produced commercially by the partial reduction of 2,4-dinitrophenol This reduction may be achieved electrolyticaHy using vanadium (159) or chemically with polysulftde, sodium hydrosulftde, or hydrazine and copper (160). Alternatively, 2-acetamidophenol or 2-methylbenzoxazole may be nitrated in sulfuric acid to yield a mixture of 4- and 5-nitro derivatives that are then separated and hydrolyzed with sodium hydroxide (161). 

Industrial production is by reduction of the corresponding nitrophenol with iron or hydrazine (167,168). 2-Amino-4,6-dichlorophenol finds important use as an azo-dye intermediate (see Azo dyes). 

Reaction of 4-amino-l-azabutadienes (45) with various hydrazine salts at 60°C leads to the expected pyrazoles (46) without isolation of the hydrazone intermediate (eq. 8) (39). 

Derivatization is useful for detection of compounds such as amino acids and amines that lack easily detectable groups. For similar reasons, saccharides, as a class of compound, ehcit much interest. Two derivatization schemes have been reported using benzamide (61) and FMOC—hydrazine (62) to produce fluorescent products. 

Monochloramine is also used in organic synthesis for preparation of amines, substituted hydrazines, etc. For example, reaction of NH2CI with 3-azabicyclo [3.3.0]octane [5661-03-0] yields A/-amino-3-azabicyclo[3.3.0]octane [54528-00-6] a pharmaceutical intermediate (38). 

Hydroxyl Group. The OH group of cyanohydrins is subject to displacement with other electronegative groups. Cyanohydrins react with ammonia to yield amino nitriles. This is a step in the Strecker synthesis of amino acids. A one-step synthesis of a-amino acids involves treatment of cyanohydrins with ammonia and ammonium carbonate under pressure. Thus acetone cyanohydrin, when heated at 160°C with ammonia and ammonium carbonate for 6 h, gives a-aminoisobutyric acid [62-57-7] in 86% yield (7). Primary and secondary amines can also be used to displace the hydroxyl group to obtain A/-substituted and Ai,A/-disubstituted a-amino nitriles. The Strecker synthesis can also be appHed to aromatic ketones. Similarly, hydrazine reacts with two molecules of cyanohydrin to give the disubstituted hydrazine. 

There are several examples of replacement of methoxy and ethoxy groups in substituted pyridazine N- oxides, with ammonia or hydrazine producing the corresponding amino and hydrazino compounds. 

Phthalic anhydride and diethyl phthalate are easily converted with hydrazine into 4-hydroxyphthalazin-l(2/f)-one. Its substituted derivatives have been prepared using substituted hydrazines, substituted phthalic anhydrides, or diesters or disodium salts of substituted phthalic acids (Scheme 81). However, condensation of phenylhydrazine with phthalic anhydride gives only a small amount of the corresponding phthalazine, the main product being 2-anilinophthalimide. This can be rearranged in the presence of base into the phthalazine derivative. For the preparation of 2,3-disubstituted derivatives, 1,2-disub-stituted hydrazines are reacted with the appropriate phthalic anhydrides or phthaloyl chlorides. Derivatives of 4-amino- or 4-hydrazino-phthalazin-l(2iT)-one have been prepared either from the corresponding monothiophthalimide and 3-aminoisoindolin-3-one (1S4) or from ethyl 2-cyanobenzoate (155) and hydrazine hydrate (Scheme 82). Similarly,... 

Hydroxyphthalazin-l(2//)-one is obtained in a smooth reaction between phthalic anhydride and hydrazine hydrate and this is again the starting compound for many 1-substituted and/or 1,4-disubstituted phthalazines. The transformations of 1,4-dichloro-phthalazine, which is prepared in the usual manner, follow a similar pattern as shown for pyridazines in Scheme 110. On the other hand, phthalonitrile is the preferential starting compound for amino- and hydrazino-phthalazines. The most satisfactory synthesis of phthalazine is the reaction between a,a,a, a -tetrachloro-o-xylene and hydrazine sulfate in sulfuric acid (67FRP1438827), alt iough catalytic dehalogenation of 1-chloro- or 1,4-dichloro-phthalazine or oxidation of 1-hydrazinophthalazine also provides the parent compound in moderate yield. 

Amino groups are formed by reduction of nitro groups in aryl substituents and behave normally (62JCS1671), but when attached directly to the pyridopyridazine ring they may be removed by acid hydrolysis or treatment with nitrous acid, or replaced by hydrazine. 

The only other synthesis of a benzo fused derivative involves the pyridazino[4,3-cjisoquinoline series, the isoquinoline derivative (377) reacting with hydrazine to give (378) (74YZ607), although an s-triazolo-fused pyrido[2,3-tf Ipyridazine was obtained in the reaction of l-amino-3-iminoisoindolenine with hydrazine and formic acid (56GEP951993). 

The imonium salt (199), obtained from ynamines and phosgeneimonium chloVide, underwent ready reaction with monosubstituted hydrazines to give the 3,5-bis(dimethyl-amino)pyrazole (200) (68T4217, 69T3453). Similarly, the adduct (201), resulting from the addition of phosgene to ynamines, likewise reacted with sym-disubstituted hydrazines to give pyrazoles (202). With hydroxylamine derivatives the isoxazolinone (203) was obtained. 

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