Substituted 4/7-3,1-benzoxazines

The l,2,3,4,4 ,5-hcxahydro-pyrazino[2,l-t ][l,4]benzoxazinc 350 was prepared from the appropriately substituted benzoxazine 349, as shown in Scheme 56 <1997BML763, 2003JME2877>. Diethyl oxalate <2001USP6169086> and dibromoethane <2002W02002/020533> were also utilized to build the pyrazino ring of [l,4]oxazino[4,3-tf]quinoxalines. 

Scheme 6.264 Multistep synthesis of substituted benzoxazine derivatives.

Aminopyridine can be prepared by the reaction of 4-chloro-l,3-benzoxazines (47) with pyridine TV-oxides. Here it is proposed that an ion or radical pair is formed initially, which through displacement of hydrogen chloride and rearrangement leads to an TV-substituted benzoxazine (48). Finally, acid hydrolysis gives 2-aminopyridine and salicylic acid (49 Scheme 14) (80CPB465). 

Finally, the N- -H distance in the hydrogen bonding arrangement adopted by a pair of methyl-substituted benzoxazine dimers has been determined by solid state NMR to be 1.94 A [148]. 

As a first example, we show how rotor-synchronized H DQ MAS spectra can distinguish between the solid-state hydrogen-bonded structures adopted by two different alkyl-substituted benzoxazine dimers [7V,./V-bis(3,5-dimethyl-2-hydroxybenzyl) R amine, where R = methyl or ethyl], 1, in the solid state.21... 

SCHEME 31. Reaction between generalized W-(hydroxyphenyl)succinimides and HMTA to form substituted benzoxazines... 

Condensation of anthranilic acid with various ort/zo-esters and reaction of semicarbazides, gave 2-substituted benzoxazin-4-ones and also by the reaction of hydrazones with aryl-/alkyl-ureas and by salicylaldehyde or 2-hydroxyacetophenones with 4-aryl-/alkyl-semicarbazides. Hydrolysis of o-aminoesters and subsequent treatment with phosgene gave 40. Fused oxazine with bridge head nitrogen 41 and triazolo[3,4-Z>]thiazines 42 were also prepared . The 2,3-dihydrobenzoxazine 43, thiomorpholines 44 and phenothiazines 45 were prepared. ... 

Returning to the grasses, we now have positive identifications of phytoalexins in oats and rice. In oats, avenalumins I, II and III have been isolated from leaves Infected with the crown rust fungus. These three compounds are benzoxazin-4-ones substituted in the 2-position with hydroxycinnamyl residues (37), Again there is a parallel with phytoalexins of dicotyledons A simple 2-phenyl substituted benzoxazin-4-one dlanthalexln was Isolated from infected carnation leaves by French scientists in 1983 (38). 

An efficient method for the synthesis of 2-substituted benzoxazin-4-ones was performed by the condensation of anthranilic acid (436) with various orthoesters by classical heating for 1 2h to give 75 91% yields. But under MWI in an open vessel, a rapid formation of benzoxazin-4-ones 439 in high yields (76-94%) took place within 1-5 min (Scheme 86). The reaction may proceed through the imidic ester intermediate 437, which upon nucleophilic attack by the carboxyl oxygen produced the cycKzed intermediate 438 that then eliminated a molecule of alcohol to give 439 (97JCR(S)286). 

A qualitative study carried out by these authors, on different N substituted benzoxazines and various phenols, revealed two Important features, namely the orthohydroxy selectivity of the reaction and the important steric effect of the N substituent of benzoxazines. 

Isoxazoles substituted in the 3-position, but unsubstituted in the 5-position, react under more vigorous conditions to give acids and nitriles (Scheme 24). Anthranils unsubstituted in the 3-position are similarly converted into anthranilic acids by bases (Scheme 25) (67AHC(8)277). Attempted acylation of anthranils gives benzoxazine derivatives via a similar ring opening (Scheme 26) (67AHC(8)277). 

Pyrano[3,2-g]benzoxazine, dihydrosynthesis, 3, 714 Pyranobenzoxazines synthesis, 6, 190 Pyranobenzoxazoles mass spectra, 3, 615 Pyrano[2,3-a]carbazoles synthesis, 4, 235 Pyrano[2,3- 6]carbazoles synthesis, 4, 235 Pyrano[3,2-a]carbazoles synthesis, 4, 235 Pyranochromones synthesis, 3, 821 Pyranochromones, dihydrosynthesis, 3, 81 817 Pyranocoumarins crystal data, 3, 623 mass spectra, 3, 610 Pyranodipyranones synthesis, 3, 794 Pyrano[3,2-6]indol-4-ones synthesis, 4, 302 Pyran-2-ol, dihydrodehydration, 3, 762 Pyran-2-ol, 3-methyltetrahydro-synthesis, 3, 775 Pyran-2-ol, tetrahydro-6-substituted synthesis, 3, 775 Pyran-4-ol, tetrahydro-IR spectra, 3, 594 Raman spectra, 3, 594 Pyranols, tetrahydro-bond lengths, 3, 621 synthesis, 3, 777... 

Enantiopure (7 )-3-alkylpiperidines (38, R = Me, Et) were obtained when perhydropyrido[2,l-Z)][l,3]benzoxazin-9-ones (37, R = H, Me) were treated first with an excess of AIH3, then with PCC, followed by a 2.5 N solution of KOH (99TL2421). Treatment of optically active perhydropyr-ido[2,l-Z)][l,3]benzoxazines 39 and 40 with LAH in the presence of AICI3 and DIBALH (if R = COOEt) yielded 3-substituted piperidines 41 (00TA2809). 

Depending upon the structure of the substrates 49, 52, and 56 hexahydropyrido[l,2-n]-[3,l]benzoxazines 50, 54, 2-aminobenzaldehyde 53, 1-substituted piperidones 51, 55, 57, 3,4,5,6-tetrahydropyridinium salt 58, or their mixture was obtained during the oxidation of 1-(2-hydroxymethyl-, 2-formyl- and 2-acetylphenyl)piperazines (49, 52, 56) with Hg(II)-EDTA complex (Schemes 6-8) (79AP219, 98ZN(B)37, 98ZN(B)1369). 

The respective amide was prepared from 7-substituted 5-oxo-2,3-dihydro-5//-pyrido[l,2,3-de]-l,4-benzoxazine-6-carboxylic acids via acid chlorides with different benzylamines (00M1P3). 6-Carboxamides were N-benzylated, and a side-chain phenolic hydroxy group was O-alkylated. 7-Aryl-5-oxo-2,3-dihydro-5//-pyrido[l, 2,3-r/e]-1,4-benzoxazine-6-carboxylic acid was obtained from the ethyl ester by alkalic hydrolysis. 

Heating of a mixture of ethyl 9-substituted 7-oxo-7//-pyrido[l,2,3-e/e]-l,4-benzoxazine-6-carboxylates and 4-chlorobenzylamine yielded iV-(4-chlor-obenzyl)amides (01MIP2). 

Oxo-2,3,6,7-tetrahydro-5//-pyrido[l,2,3- /e]-l,4-benzoxazine-2-carbox-ylates (291, X = H2) were obtained by hydrogenation of 4-substituted 3, 4-dihydro-2//-1,4-benzoxazine-2-carboxylates (290, X = H2) over 10% Pd/C catalyst, then by the treatment of free acids with (CF3C0)20 (99EUP894796). 5,7-Dioxo-2,3,6,7-tetrahydro derivatives 291 (X = 0) were prepared similarly from 290 (X = O). The products 291 (X = O) exist in 7-hydroxy-5-oxo-2,3-dihydro-5// tautomeric form. 

In 1984, we demonstrated that A-alkoxy-A-acyl nitrenium ions 15 could be generated by the reaction of A-alkoxy-A-chloroamides 14 with Lewis acids such as Ag + and Zn2+ and used these to form heterocycles by intramolecular aromatic substitution reactions (Scheme 2).90 In this manner, several novel A-acyl-3,4-dihydro-2,l-benzoxazines 16a and A-acyl-4,5-dihydro-( I //,3//)-2,1-benzoxazepines 16b were made. Subsequent work91,92 and that of Kikugawa93 96 produced numerous syntheses involving alkoxynitrenium ions including formation of natural products.97 99... 

Tandem mass spectrometry has been used to demonstrate that M+ as well as MH+ of substituted A-(ort/zo-cyclopropylphenyl)benzamides isomerizes before the fragmentation, with formation of 3-aryl-1-ethyl-lH-benzoxazines and 5-ethyl-2-oxodi-benzoazepines (Scheme 5.14). The methyl group in /V-[ortho-( 1 -methylcvclopropyl )-phenyl]benzamides quenches the latter process, leaving the formation of benzoxazines as the only cyclization reaction. A subsequent chemical experiment in solution confirmed the mass spectral predictions [24]. A similar study confirmed the analogy of cyclization of substituted A-(ort/zo-cyclopropylphenyl)-A -aryl ureas and N- ortho-cyclopropylphenyl)-A -aiyl thioureas in the ion source of mass a spectrometer and in solution [25]. 

Lf abbtetal. elaborated a very short and efficient pathway to [l,2,4]thiadiazolo[l,4]benzoxazines, which, interestingly, follows a quite complicated pathway <1994T7019, 1996J(P1)225>. The starting compound is the cyano-substituted... 

Condensation of [3- or "y-amino alcohols with aldehydes or ketones RR CO gives the product 27. In solution the position of the equilibrium varies with R and R, and with the solvent (73). When the carbonyl reactant is a substituted benzaldehyde, the solid is found (IR, KBr) to comprise molecules of the open-chain structure 27a, whereas aliphatic aldehydes and ketones give crystals of dihydro- 1,3-benzoxazines, 27b. An interesting case is that of the condensation product of o-hydroxybenzylamine with cyclopentanone, for which McDonagh and Smith (73) suggest that ring and chain tautomers coexist in the solid. 

A study of the regioselectivity of the 1,3-dipolar cycloaddition of aliphatic nitrile oxides with cinnamic acid esters has been published. AMI MO studies on the gas-phase 1,3-dipolar cycloaddition of 1,2,4-triazepine and formonitrile oxide show that the mechanism leading to the most stable adduct is concerted. An ab initio study of the regiochemistry of 1,3-dipolar cycloadditions of diazomethane and formonitrile oxide with ethene, propene, and methyl vinyl ether has been presented. The 1,3-dipolar cycloaddition of mesitonitrile oxide with 4,7-phenanthroline yields both mono-and bis-adducts. Alkynyl(phenyl)iodonium triflates undergo 2 - - 3-cycloaddition with ethyl diazoacetate, Ai-f-butyl-a-phenyl nitrone and f-butyl nitrile oxide to produce substituted pyrroles, dihydroisoxazoles, and isoxazoles respectively." 2/3-Vinyl-franwoctahydro-l,3-benzoxazine (43) undergoes 1,3-dipolar cycloaddition with nitrile oxides with high diastereoselectivity (90% de) (Scheme IS)." " ... 

Perhydro derivatives of pyrido[l,2-6][l,2]oxazines are frequently applied in the total synthesis of various alkaloids to control the stereochemistry, and 4-(substituted amino)-5-fluoro-7-oxo derivatives of 3,7-dihydro-2//-pyrido[3,2,l-f7][2,l]benzoxazine- and l,2,3,7-tetrahydropyrido[3,2,l-//]cin-noline-8-carboxylic acids are considered as a subfamily of the third generation of antibacterial quinolones. 

The 4-fluoro atom of 4,5-difluoro-7-oxo-2,3-dihydro-7//-pyrido[3,2,l-t ]-[2,l]benzoxazine-8-carboxylate (40) was regioselectively substituted by cyclic amines in DMSO at 100-110 C [92JAP(K)92/208288, 92JAP(K)92/ 210656],... 

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