Synthesis of phosphodiesterase IVb inhibitors 2. Stereoselective synthesis of hexahydro-3H-pyrrolo[1,2-c]imidazol-3-one and tetrahydro-1H-pyrrolo[1,2-c][1,3]oxazol-3-one derivatives

The total stereoselective synthesis of two highly potent phosphodiesterase IVb inhibitors from nitroethane, isovanillin, and ethyl vinyl ether was developed. The compounds obtained are the derivatives of hexahydro-3H-pyrrolo[1,2-c]imidazol-3-one and tetrahydro-1H-pyrrolo[1,2-c][1,3]oxazol-3-one. The strategy proposed involves silylation of six-membered cyclic nitronates as a key step leading to 5,6-dihydro-4H-1,2-oxazines with the group CH₂FG (FG = N₃ or OH) at the C(3) atom.     

Formation of Heptaleno[1,2-c]furans and Heptaleno[1,2-c]furanones

The dehydrogenation reaction of the heptalene-4,5-dimethanols 4a and 4d , which do not undergo the double-bond-shift (DBS) process at ambient temperature, with basic MnO₂ in CH₂Cl₂ at room temperature, leads to the formation of the corresponding heptaleno[1,2-c]furans 6a and 6d , respectively, as well as to the corresponding heptaleno[1,2-c]furan-3-ones 7a and 7d , respectively (cf. Scheme 2 and 8). The formation of both product types necessarily involves a DBS process (cf. Scheme 7). The dehydrogenation reaction of the DBS isomer of 4a , i.e., 5a , with MnO₂ in CH₂Cl₂ at room temperature results, in addition to 6a and 7a , in the formation of the heptaleno[1,2-c]-furan-1-one 8a and, in small amounts, of the heptalene-4,5-dicarbaldehyde 9a (cf. Scheme 3). The benzo[a]heptalene-6,7-dimethanol 4c with a fixed position of the C?C bonds of the heptalene skeleton, on dehydrogenation with MnO₂ in CH₂Cl₂, gives only the corresponding furanone 11b (Scheme 4). By [²H₂]-labelling of the methanol function at C(7), it could be shown that the furanone formation takes place at the stage of the corresponding lactol [3-²H₂]- 15b (cf. Scheme 6). Heptalene-1,2-dimethanols 4c and 4e , which are, at room temperature, in thermal equilibrium with their corresponding DBS forms 5c and 5e , respectively, are dehydrogenated by MnO₂ in CH₂Cl₂ to give the corresponding heptaleno[1,2-c]furans 6c and 6e as well as the heptaleno[1,2-c]furan-3-ones 7c and 7e and, again, in small amounts, the heptaleno[1,2-c]furan-1-ones 8c and 8e , respectively (cf. Scheme 8). Therefore, it seems that the heptalene-1,2-dimethanols are responsible for the formation of the furan-1-ones (cf. Scheme 7). The methylenation of the furan-3-ones 7a and 7e with Tebbe's reagent leads to the formation of the 3-methyl-substituted heptaleno[1,2-c]furans 23a and 23e , respectively (cf. Scheme 9). The heptaleno[1,2-c]furans 6a, 6d , and 23a can be resolved into their antipodes on a Chiralcel OD column. The (P)-configuration is assigned to the heptaleno[1,2-c]furans showing a negative Cotton effect at ca. 320 nm in the CD spectrum in hexane (cf. Figs. 3–5 as well as Table 7). The (P)-configuration of (–)- 6a is correlated with the established (P)-configuration of the dimethanol (–)- 5a via dehydrogenation with MnO₂. The degree of twisting of the heptalene skeleton of 6 and 23 is determined by the Me-substitution pattern (cf. Table 9). The larger the heptalene gauche torsion angles are, the more hypsochromically shifted is the heptalene absorption band above 300 nm (cf. Table 7 and 8, as well as Figs. 6–9).     

Thermal Cyclization of 2-Acyl-1-azido-3-phenalenones to Phenaleno[1,2-c]isoxazol-7-ones

1-Azido-3-phenalenones 5 with acyl substituents in position 2, obtained by acylation and azidation of 1-hydroxy-3-phenalenones 1 , cyclized by thermolysis to give phenaleno[1,2-c]isoxazol-7-ones 9 . The thermolysis conditions were studied by differential scanning calorimetry.     

Polymethyl derivatives of furo[3,4-c]pyran4-one,furo[3,4-c] pyridin-4-one and pyrrolo[3,4-c]pyran-4-one

The: title compounds were prepared from Michael adducts, obtained from acetoacetic esters and trans-3-hexene-2,5-dione, and from the corresponding dehydration products, by direct cyclization to oxygen rings or by reaction with ammonia (or methylamine) to give nitrogen rings.     

Reactions of 3-acetyltropolone and its methyl ethers with hydroxylamine. Formation of 8H-cyclohept[d]isoxazol-8-one and 8H-cyclohept[c]isoxazol-8-one

The reaction of 3-acetyltropolone ( 1 ) with hydroxylamine under the acidic condition gave 3-methyl-8H-cyclohept[d]isoxazol-8-one ( 4 ) and its oxime ( 5 ), and under the neutral condition gave 4 and 3-acetyltropolone oxime ( 6 ). The reaction of 3-acetyl-2-methoxytropone ( 2a ) with hydroxylamine under the acidic condition gave 4, 5 , and 4-methyl-1H-2,3-benzoxazin-1-one ( 7 ), and under the neutral condition gave 4, 7 , 3-methyl-8H-cyclohept[c]isoxazol-8-one ( 8 ), and its oxime ( 9 ). The reaction of 7-acetyl-2-methoxytropone ( 2b ) with hydroxylamine under the acidic condition gave 4 and 5 , and under the neutral condition gave 5, 7 , and 9 .     

Facile Regioselective Synthesis of 2-Methyl Furo [3,2-c][1] benzopyran-4-one 2-Methyl Furo[2,3-c] [1]benzopyran-4-one

The title compounds (7 &8) were obtained in excellent yields from 4-[2′-chloroprop-2′-enyloxy] [1] benzopyran-2-one (5) and 3-[2′-chloroprop-2-enyloxy][1]benzopyran-2-one (6) via [3,3] sigmatropic rearrangement and cyclisation of the intermediate chloroallylic enols with conc. H₂SO₄. The reaction was also studied in N,N-dimethyl aniline.     

由N-苯基[1,3]苯并噁嗪正离子与烯烃[4+2]反应合成喹啉并[1,2-c][1,3]苯并噁嗪-6-酮衍生物

以BF3·OEt2 为催化剂, 在室温下通过4-羟基-N-苯基[1,3]苯并噁嗪-2-酮的脱羟基产生N-苯基[1,3]苯并噁嗪正离子, 然后与富电子烯烃发生Diels-Alder反应, 合成出了一系列喹啉并[1,2-c][1,3]苯并噁嗪-6-酮和喹啉并[1,2-c][1,3]萘并噁嗪-6-酮衍生物.     

3-Benzoyl-2-hydroxy-9-methylpyrido[1,2-A] pyrimidin-4-one

The single aberrant product of the reaction between 2-amino-3-methylpyridine ( 2 ) and ethyl benzoylacetate ( 4 ) in diethylbenzene at ca. 180° was 3-benzoyl-2-hydroxy-9-methylpyrido-[1,2-a]pyrimidin-4-one ( 5 ). When administered to naive rats, 5 induced behavioral effects strikingly similar to those manifested by morphine-addicted rats who have been deprived of that analgetic.     

Annulation reactions of 3-aminoisoquinolin-l(2H)-one. Synthesis of pyrimido[1,2-b]isoquinolines,pyrido-[2,3-c]isoquinolines and pyrrolo[2,3-c]isoquinolines

Reactions of the title compound with the malonic acid derivatives diethyl ethoxymethylenemalonate (EMME), ethyl ethoxymethylenecyanoacetate (EMCA) and ethoxymethylenemalononitrile (EMMN) are reported. Condensations occur at the amino group or C-4, depending on conditions and the former intermediate was successfully cyclized to the pyrimido[1,2-b]isoquinoline system. Reactions with 2,4-pentanedione and p-bromophenacyl bromide gave only the angular systems, pyrido[2,3-c]isoquinoline and pyrrolo[2,3-c]isoquin-oline, respectively.     

Synthesis of some isomeric 4,11-dihydro-5H-[1]benzoxocino[4,3-d] or [3,4-c]isoxazol-5-ones and isomeric 4,5,10,11-tetrahydrobenzo[5,6]-cycloocta[2,1-d] or [1,2-c]isoxazol-5-ones

The title compounds were prepared by acid-catalyzed cyclization of aryloxymethyl- or (2-arylethyl)-4-carboxymethylisoxazoles which in turn were synthesized from aryloxymethyl- or (2-arylethyl)isoxazole-4-carboxylic acids by Arndt-Eistert homologation.     

Novel polycyclic heterocycles. XI. Synthesis of 11,12-dihydropyrido[2,1-b] [1,3]benzodiazepines, 6H-pyrido[1,2-c] [1,3,5]benzoxadiazepines,and 6H-Pyrido[1,2-c] [1,3,5]benzothiadiazepines

An unusually facile dehydrobromination, involving the ortho-bromine atom and the = NH proton of a 2-imino-1-(phenethyl)-, 2-imino-1-(phenoxymethyl)-, or 2-imino-1-(phenylthiomethyl)-pyridine ( 2a-e ) has led to the synthesis of three novel bridgehead nitrogen tricyclic systems: 11,12-dihydropyrido[2,1-b] [1,3]benzodiazepines ( 3a,b ), 6H-pyrido[1,2-c] [1,3,5]benzoxadiazepines ( 3c,d ) and 6H-pyrido[1,2-c][1,3,5]benzothiadiazepines ( 3e ). As anticipated, these cyclizations required a base, e.g., potassium carbonate, and a catalyst, e.g., copper bronze. What was unusual, was that these reactions occurred in methanol or n-propanol, under reflux, either under anhydrous conditions, or in the presence of large amounts of water. The pmr spectra of these compounds are discussed.