Amino acetophenone

Aldehydes and ketones may frequently be identified by their semicarbazones, obtained by direct condensation with semicarbazide (or amino-urea), NH,NHCONH a compound which is a monacidic base and usually available as its monohydrochloride, NHjCONHNH, HCl. Semicarbazones are particularly useful for identification of con jounds (such as acetophenone) of which the oxime is too soluble to be readily isolated and the phenylhydrazone is unstable moreover, the high nitrogen content of semicarbazones enables very small quantities to be accurately analysed and so identified. The general conditions for the formation of semicarbazones are very similar to those for oximes and phenylhydrazones (pp. 93, 229) the free base must of course be liberated from its salts by the addition of sodium acetate. 

Amino-4-phenylthiazole when heated with Raney Ni is reported to yield acetophenone (469). In the course of a general study on reductive cleavage in heterocyclic systems Hoff et al. studied the reaction of 2-amino-4-methylthiazole with Na in liquid ammonia. Two equivalents of Na are necessary to obtain a mixture of 4-methyl-3-thiazoline (240) and... 

Ary] 2-amino-5-(p-aminophenyl)thia2oles of the general formula 116 were prepared by condensing phenylthiosemicarbazides (115) with either w-bromoacetophenone by refluxing in alcohol for 2 hr (Method A) or with acetophenones and iodine on a steam bath for 8 hr (Method B) Scheme 53 (517), with R = para Me, MeO, Cl, Br, I, NOj, NHj, Ph ortho Me, NOjl or meta Br, I, NO. Yields ranged from 55 to 90% from Method A and 40 to 70% from Method B. 

This example demonstrates the most challenging problem of flavor chemistry, ie, each flavor problem may require its own analytical approach however, a sensory analysis is always required. The remaining unknown odorants demand the most sensitive and selective techniques, and methods of concentration and isolation that preserve the sensory properties of complex and often dehcate flavors. Furthermore, some of the subtle odors in one system will be first identified in very different systems, like o-amino acetophenone in weasels and fox grapes. 

Synthesis and Properties. Polyquinolines are formed by the step-growth polymerization of o-aminophenyl (aryl) ketone monomers and ketone monomers with alpha hydrogens (mosdy acetophenone derivatives). Both AA—BB and AB-type polyquinolines are known as well as a number of copolymers. Polyquinolines have often been prepared by the Friedlander reaction (88), which involves either an acid- or a base-catalyzed condensation of an (9-amino aromatic aldehyde or ketone with a ketomethylene compound, producing quinoline. Surveys of monomers and their syntheses and properties have beenpubhshed (89—91). 

Amino-2-isoxazolines were prepared by the condensation of acrylonitriles with N-hydroxyurea (73BSF1138) or of urea and acetophenones, as shown in Scheme 127 (78ZOR2000). 

The most successful of the Lewis acid catalysts are oxazaborolidines prepared from chiral amino alcohols and boranes. These compounds lead to enantioselective reduction of acetophenone by an external reductant, usually diborane. The chiral environment established in the complex leads to facial selectivity. The most widely known example of these reagents is derived from the amino acid proline. Several other examples of this type of reagent have been developed, and these will be discussed more completely in Section 5.2 of part B. 

The hydride-donor class of reductants has not yet been successfully paired with enantioselective catalysts. However, a number of chiral reagents that are used in stoichiometric quantity can effect enantioselective reduction of acetophenone and other prochiral ketones. One class of reagents consists of derivatives of LiAlH4 in which some of die hydrides have been replaced by chiral ligands. Section C of Scheme 2.13 shows some examples where chiral diols or amino alcohols have been introduced. Another type of reagent represented in Scheme 2.13 is chiral trialkylborohydrides. Chiral boranes are quite readily available (see Section 4.9 in Part B) and easily converted to borohydrides. 

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). 

Substitution of an alicyclic ring for one of the aromatic rings in the amino alcohols such as 32 or 39 produces a series of useful antispasmodic agents that have found some use in the treatment of the symptoms of Parkinson s disease. Mannich reaction of acetophenone with formaldehyde and piperidine affords the amino-ketone, 44a. Reaction of the ketone with cyclohexylmagnesium... 

A compound closely related to classical adrenergic agonists in which the para hydroxy function is however replaced by an amino group has been investigated for its activity as a growth promoter in domestic animals. Acylation of the aniline derivative 26 with chloracetyl chloride will afford acetophenone 27 the amino-ketone 28 is obtained on reaction with isopropylamine. Removal of the protecting group (29) followed by reduction of the ketone affords cimaterol (30) 5J. 

A solution of N-(2-aminobenzvl)-1-phenyl-2-metKylaminoethanol-1 was prepared by the reaction of a-bromo-acetophenone and (2-nitrobenzyl)methylamine, followed by hydrogenation of the nitro group by means of nickei on diatomaceous earth at room temperature and reduction of the CO group by means of sodium borohydride. The intermediate thus produced was dissolved in 100 ml of methylene chloride and introduced dropwise into 125 ml of sulfuric acid at 10° to 15°C. After a short standing, the reaction mixture was poured onto ice and rendered alkaline by means of a sodium hydroxide solution. Dy extraction with ether, there was obtained 1,2,3,4-tetrahydro-2-methyl-4-phenyl-8-amino-iso-quinoline. The base is reacted with maleic acid to give the maleate melting point of the maleate 199° to 201°C (from ethanol). 

Mit aquivalenten Mengen Diboran wird dagegen die Cyan-Gruppe selektiv hydriert, so erhalt man z.B. aus Phenyl-glyoxylsaure-nitril 61% d.Th. to-Amino-acetophenon (s.S.159) ... 

Auch Kalium-tetracarbonyl-hydrido-ferrat(O) reduziert in Athanol 2-Nitro-acetophe-non selektiv zu 2-Amino-acetophenon 2-Nitro-zimtaldehyd wird in quantitativer Aus-beute reduktiv zu Chinolin cyclisiert6 ... 

Amino-2-quinoxalinecarbaldehyde (186) and acetophenone (187) gave 2-phenylpyrido[2,3-h]quinoxaline (188) (NaOH, EtOH, H2O, briefly % many analogs likewise). 

C7H, N303 55559-70-1) see Cidofovir 6-amino-2,4-dihydroxypyrimidine (C4H5N3O2 143505-00-4) see Sulfadimethoxine 2-amino-2, 5 -dimethoxy acetophenone (Ck,H 3N03) see Midodrine 2-amino-4,5-dimethoxybenzamide (C,j1I 2N203 5004-88-6) see Alfuzosin... 

In the same study, these authors also described the synthesis of other S/N ligands derived from various amino acids, such as proline, valine and cysteine. These dithioether and azathioether ligands were further tested as potential palladium ligands for the reduction of acetophenone, but no significant induction was observed in each case of ligand (Scheme 8.26). 

In the same study, these authors have prepared another series of amino-sulf(ox)ide ligands based on the (Nor)ephedrine and 2-aminodiphenylethanol skeletons, bearing two chiral centres in the carbon backbone.Their application to the iridium-catalysed hydrogen-transfer reduction of acetophenone generally gave better yields, but the enantioselectivity never exceeded 65% ee (Scheme 9.4). 

Scheme 9.6 Ir-catalysed reduction of acetophenone with 2-azanorbornyl amino-sulf(ox)ide ligands.

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