Nuclear hydroxylated metabolite of fluradoline (2-fluoro-11-[(β-methylamino)ethylthio]dibenz[b,f]oxepin hydrochloride). Identification and synthesis

Fluradoline (2-fluoro-11-[β-(methylamino)ethylthio]dibenz[b,f]oxepin), a novel analgesic with an unique profile, was found to be extensively metabolized in man as well as in other species. One of the major metabolites of this drug appeared to be a nuclear hydroxylated derivative of the parent compound, and the site of enzymatic hydroxylation was established to be C(7) by using high-field proton nuclear magnetic spectroscopy. This structural assignment was subsequently confirmed by the synthesis of an authentic sample of 2-fluoro-7-hydroxy-11-[β-(methylamino)ethylthio]dibenz[b,f]oxepin ( 2a ).     

Dibenz[b,f]oxepin and thiepin radical anions. Conjugative properties of sulfur in its different oxidation states

The radical anion of dibenz[b,f]oxepin has been investigated by esr spectroscopy and the relative coupling constants compared with dibenzo[b,f]thiepin. In both cases assignments were obtained using a theoretical method (INDO). In addition radicals from dibenzo[b,f]thiepin sulfoxide and sulfone could be detected and, unusually, the free electron density on carbon atoms of the radical anion containing a sulfonyl group is larger than that on carbons of radical anions containing a sulfide or a sulfoxide group.     

Dibenzo[b,f]oxepin‐10(11H)‐one and dibenzo[b,f]thiepin‐10(11H)‐one as useful synthons in the synthesis of various dibenzo[e,h]azulenes

The present review focuses on dibenzo[b,f]oxepin‐10(11H)‐one ( I , X = O) and dibenzo[b,f]thiepin‐10(11H)‐one ( I , X = S) as common synthons in the efficient synthesis of various dibenzoxepino[4,5‐ and dibenzothiepino[4,5]‐fused five‐membered heterocycles: [2,3] fused thiophene ( II ), [3,4] fused thiophene ( III ), furan ( IV ), pyrrole ( V ), imidazole ( VI ), pyrazole ( VII ), oxazole ( VIII ), and thiazole ( IX ). The potential of I to be converted into reactive intermediates that readily undergo heteroaromatic annulation reactions by cyclocondensation with proper binucleophiles allows formation of a range of enumerated functionalized dibenzo[e,h]azulene [4] structures ( II , III , IV , V , VI , VII , VIII , IX ). Dibenzo[e,h]azulenes as heterotetracyclic scaffold can be exploited in further modifications to obtain compounds with altered physicochemical and biological profile. J. Heterocyclic Chem., (2012).     

An example of a novel formation of an oxepin

A novel formation of an oxepin, namely 9,10,11,12-tetrafluoro-5,6-dihydrobenzo[b]naphth[2,1-f]oxepin (5) , starting from pentafluoroacetophenone and 1-tetralone is described. Also, the same synthesis using 1-indanone affords a very different ring system namely 1,2,3,4-tetrafluoro-5,11b-dihydro-7H-benzo[c]fluoren-7-one (10) . Both synthesis undergo an intramolecular nucleophilic substitution of an ortho-fluorine. In one case, the oxygen displaces the fluorine to afford the oxepin 5 and the other a carbon is used as the nucleophile to give the polycyclic ring system 10 .     

Beiträge zur Entwicklung psychotroper Stoffe, 5. Mitt.

Zusammenfassung N-Carbäthoxy-11-(3-monomethylamino-propyliden)-6, 11-dihydro-dibenzo[b, e]oxepin (III) und 11-(3-Dimethylaminopropyliden)-6, 11-dihydro-dibenzo [b, e]oxepin (II) isomerisieren bei längerer Einwirkung von HBr—Eisessig zu den 3-Arylindenderivaten V und VI. Strukturbeweis und Reaktionsmechanismus werden erläutert.4. Mittl.:K. Stach, M. Thiel undF. Bickelhaupt, Mh. Chem.93, 1090 (1962).     

Proton,carbon-13 and fluorine-19 NMR studies of 9,10,11,12-tetra-fluoro-5,6-dihydrobenzo[b]naphth[2,1-f]oxepin: ‘Through-space’ carbon-fluorine coupling was revealed

The ¹H, ¹³C and ¹⁹F nmr spectra of 9,10,11,12-tetrafluoro-5,6-dihydrobenzo[b]naphth[2,1-f]oxepin ( 1 ) were totally assigned using a combination of two-dimensional nmr techniques. Unequivocal interpretation of the spectral data allowed the complete assignments of the resonances. In addition, the spectra of compound 1 revealed an unusual through-space carbon-fluorine coupling which was further supported by NOE and modeling experiments.     

Synthesis,crystal structure and activity evaluation of novel 3,4‐dihydro‐1‐benzoxepin‐5(2H)‐one derivatives as protein–tyrosine kinase (PTK) inhibitors

Four new 3,4‐dihydro‐1‐benzoxepin‐5(2H )‐one derivatives, namely (E )‐4‐(5‐bromo‐2‐hydroxybenzylidene)‐6,8‐dimethoxy‐3,4‐dihydrobenzo[b ]oxepin‐5(2H )‐one, ( 7 ), (E )‐4‐[(E )‐3‐(5‐bromo‐2‐hydroxyphenyl)allylidene]‐6,8‐dimethoxy‐3,4‐dihydrobenzo[b ]oxepin‐5(2H )‐one, ( 8 ), (E )‐4‐(5‐bromo‐2‐hydroxybenzylidene)‐6‐hydroxy‐8‐methoxy‐3,4‐dihydrobenzo[b ]oxepin‐5(2H )‐one, C₁₈H₁₅BrO₅, ( 9 ), and (E )‐4‐[(E )‐3‐(5‐bromo‐2‐hydroxyphenyl)allylidene]‐6‐hydroxy‐8‐methoxy‐3,4‐dihydrobenzo[b ]oxepin‐5(2H )‐one, ( 10 ), have been synthesized and characterized by FT–IR, NMR and MS. The structure of ( 9 ) was confirmed by single‐crystal X‐ray diffraction. Crystal structure analysis shows that molecules of ( 9 ) are connected into a one‐dimensional chain in the [010] direction through classical hydrogen bonds and these chains are further extended into a three‐dimensional network via C—H…O interactions. The inhibitory activities of these compounds against protein–tyrosine kinases (PTKs) show that 6‐hydroxy‐substituted compounds ( 9 ) and ( 10 ) are more effective for inhibiting ErbB1 and ErbB2 than are 6‐methoxy‐substituted compounds ( 7 ) and ( 8 ). This may be because ( 9 ) and ( 10 ) could effectively bind to the active pockets of the protein through intermolecular interactions.     

Photochemische Umwandlungen, 45. Mitteilung [1] die 3σ → 3π-route zu oxepin-derivaten

Exemplifying with the 4.5-dicarbomethoxy oxepin 6a the authors describe an oxepin synthesis from furanes and acetylenic dienophiles via Diels-Alder reaction ( 4a ), photochemical oxanorbornadiene-oxaquadricyclane transformation ( 4a → 5a ), and thermal 3σ → 3π opening of the highly strained oxaquadricyclane 5a . With dimethylacetylenedicarboxylate, methylpropiolate, maleic anhydride, and di-methoxycarbonyl-oxanorbornadiene ( 4a ) 5a yields the 1:1 adducts 19a, 19b, 22, 23 and 26 (unstable) by strictly stereospecific addition to the α-positions of the oxygen bridge. With the same dienophiles the oxepin 6a reacts only through its valence-tautomeric benzene-oxide form 7a giving stereospecifically 27, 29, 30 and 31 . No definite conclusions are drawn with regard to the mechanistic implications of the photostep 4a → 5a , the thermal 3σ → 3π-transformation 5a → 6a/7a , and the bishomofurane cycloaddition reactions. Scope and limitations of this oxepin synthesis are briefly discussed.     

Reaction of 5-acetyl-10,11-didehydro-5H-dibenz[b,f]azepine with pyrrole,N-methylpyrrole,imidazole and N-methylimidazole: Cycloaddition versus michael addition

Reaction of 5-acetyl-10-bromo-5H-dibenz[b, f]azepine 1 with potassium t-butoxide results in the reactive intermediate 5-acetyl-10,11-didehydro-5H-dibenz[b, f]azepine ( 2 ). The intermediate 2 reacts with N-methylpyrrole to give a mixture of the Michael addition adduct 10-(2-N-methylpyrrolyl)-5H-dibenz[b, f]azepine ( 9 ) and the Diels-Alder/retro Diels Alder adduct 8H-(N-methylpyrrolo[3,4-d]dibenz[b, f]azepine ( 8a ). Reaction of 2 with pyrrole gives a mixture of two Michael addition adducts 10-(1-pyrrolyl)-5H-dibenz[b, f]azepine ( 16 ) and 10-(2-pyrrolyl)-5H-dibenz[b, f]azepine ( 18 ). Reaction of 2 with imidazole results in the Michael addition adduct 10-(1-imidazolyl)-5H-dibenz[b, f]azepine ( 21 ).     

Synthesis of indolizidinediones annelated to a furan ring

The furo[2,3(or 3,2)-f]indolizidinediones 4a,b were synthesized in five steps from glutamic acid in good yield. The ketones were converted into trans alcohols 5a,b or oximes 6a,b (either as syn-anti mixture or as single isomer). The selectivity of these reactions is discussed.     

Synthesis of 2-methylcarbamazepine,a new internal standard for chromatographic assays of carbamazepine (tegretol®)

The synthesis of 2-methyl-5H-dibenz[b,f]azepine-5-carboxamide (2-methylcarbamazepine, 2-MCBZ, 8), a promising internal standard for chromatographic assays of the antiepileptic agent carbamazepine (CBZ, 1), is described. N-(p-Tolyl)anthranilic acid (2) was utilized as a starting material for the synthesis of a key compound, 2,9-dimethylacridine (4), which was converted in two steps to 2-methyl-9-hydroxymethylacridan (6). The acridan 6, in the presence of poly-phosphoric acid, was ring-expanded to form 2-methyl-5H-dibenz[b,f]azepine (7), this latter compound being converted by conventional reactions to its 5-carbamyl derivative, 2-MCBZ (8).     

Strategy to Construct Stair‐Shaped Partially Reduced Naphtho[1,2‐b]pyrano[2,3‐d]oxepines and Dinaphtho[1,2‐b,d]oxepines

A concise and efficient base‐induced synthesis of stair‐shaped, 4‐methylthio‐2‐oxo‐5,6‐dihydro‐2H‐naphtho[1,2‐b]pyran[2,3‐d]oxepine‐3‐carbonitriles ( 3 ) has been delineated by the reaction of 3,4‐dihydronaphtho[1,2‐b]oxepin‐5(2H)‐one ( 1 ) and methyl 2‐cyano‐3,3‐dimethylthioacrylate in DMSO using powdered KOH as a base at room temperature. Amination of 3 has been achieved by reaction with secondary amine in ethanol at reflux temperature to yield 4‐sec‐amino‐2‐oxo‐5,6‐dihydro‐2H‐naphtho[1,2‐b]pyran[2,3‐d]oxepine‐3‐carbonitriles ( 4 ). Reaction of 3 with aryl methyl ketone ( 5 ) in DMSO at room temperature using powdered KOH as a base produced stair‐shaped 5‐aryl‐7,8‐dihydro‐1,4‐dioxa‐2,3‐dioxodinaphtho[1,2‐b,d]oxepine ( 6 ) in good yields. However, reaction of 6‐aryl‐2H‐pyran‐2‐one‐3‐carbonitrile ( 8 ) with 3,4‐dihydronaphtho[1,2‐b]oxepin‐5(2H)‐one ( 1 ) did not give similar product, but in lieu 4‐aryl‐5,6‐dihydronaphtho[1,2‐b]oxepino[4,5‐b]pyran‐2‐ylidene)acetonitrile ( 9 ) was isolated and characterized.     

Benzene Oxide-Oxepin Valence Tautomerism

Benzene oxide and the potential 8π-electron system oxepin exist in valence-tautomeric equilibrium with each other, to which both components contribute to approximately the same extent. NMR spectroscopic measurements show that the equilibrium is rapidly established (activation energies of the forward and reverse reactions 9.1 and 7.2 kcal mole^?1, respectively). The present knowledge of the properties of oxepin justifies its classification as a “heterotropilidene”. Benzene oxide-oxepin represents a system having fluctuating bonds, the equilibrium of which can be displaced from one extreme to the other by means of suitable substituents. The oxide component determines the reactions of the system with most agents. With 1,6-oxido[10]annulene, which is formally a 2,7-bridged oxepin, the oxepin character is completely suppressed by the formation of a delocalized 10π-electron system extending over the C₁₀ perimeter. The existence and aromatic character of 1,6-oxido[10]-annulene give rise to the conception of a homologous series of oxygen bridged annulenes (1,6; 8,13-bisoxido[14]annulene, 1,6; 8,17; 10,15-trisoxido[18]annulene etc.), which, like the parent acenes, possess a (4n + 2)π-electron system. Molecular models demonstrate that a considerable flattening of the C_4n+2 perimeter is achievable in the case of a syn or all-syn arrangement of the oxygen bridges, and that the requirement for aromaticity is thus satisfied. This is confirmed in a striking manner by the synthesis and properties of syn-1,6; 8,13-bisoxido[14]annulene.     

Cycloaddition of benzothiete and electron-deficient nitriles

The o-quinoid 8π electron system 2 , generated by thermal ring opening of benzothiete ( 1 ), enters regio-specific [8π + 2π] cycloaddition reactions with electron-deficient nitriles 3a-d , yielding the 4H-1,3-benzothiazines 4a-d. A competitive dimerization of 1 leads to 1,5-dibenzo[b,f]dithiocin (5). Depending on the nitrile further competitive or subsequent reactions (2 + 3b → 7b, 2 + 3d → 4d → 8d) can occur. The cycloadducts 10e and 11e gained from 3e anticipate a primary cleavage of 3e to methylisothiocyanate 9e which reacts at the C?N double bond as well as at the C?S double bond.     

Preparation of 8H-Furo[3,4-d]dibenz[b,f]azepine. A Novel Heterocyclic Ring system

The synthesis of 8H-furo[3,4-d]dibenz[b,f]azepine 8 from 5H-dibenz[b,f]azepine 1a is described. The preparation of 8 represents the synthesis of a new heterocyclic system.     

Synthesis of Carbo- and Heterocyclic Cycloprop[f]indenes via cycloaddition of dienes to cyclopropenes

The heterocyclic cycloprop[f]indene 19 was synthesized via cycloaddition of diene 10 to the cyclopropene 11a and subsequent base-induced aromatization. While 19 is isolable, although very short-lived, the oxa analogue 18 decomposed under the conditions required for its preparation. The difluoro derivatives 14 and 15 , in which the heterocyclic moiety is saturated, are accessible by the cycloaddition approach, but the corresponding dichlorides are again not isolable. Cycloprop[f]indenes carrying substituents at C(4) have been obtained via cycloaddition of 22b to 1-bromo-2-chlorocyclopropene. The key step of the sequence is a double Curtius degradation of the cycloadduct 23b to the ketone 27a . While aromatization of the alcohol 27b provided the cycloprop[f]indenol 28b , the reaction failed with 27a . Attempts to convert 28b to 1,3-dihydrocycloprop[f]indene ( 25 ) via the methanesulfonate 28d failed.     

Recyclable Palladium Catalysts for the Heck/Sonogashira Reaction under Microwave‐assisted Thermomorphic Conditions

The reaction of allyl palladium(II) chloride dimer and 4,4′‐bis(R_fCH₂OCH₂)‐2,2′‐bpy, 1a–b , in the presence of AgOT_f resulted in the synthesis of cationic palladium complex, [Pd(η³‐allyl)(4,4′‐bis‐(R_fCH₂OCH₂)‐2,2′‐bpy)](OT_f), 2a–b where R_f = C₉F₁₉ ( a ), C₁₀F₂₁ ( b ), respectively. The reaction of [PdCl₂(CH₃CN)] or K₂PdCl₄ with 1b , gave rise to the synthesis of [PdCl₂(4,4′‐bis‐(C₁₀F₂₁CH₂OCH₂)‐2,2′‐bpy)], 3b . The quantitatively determined solubility curves of 2a–b and 3b in DMF indicated dramatic increase of solubility for 2a – b and 3b from ?40 to 90 °C. The catalyst‐recoverable Pd‐catalyzed Heck/Sonogashira reactions were successfully achieved in DMF with microwave‐assistance. The cationic Pd‐catalyzed Heck arylation of methyl acrylate was selected to demonstrate the feasibility of recycling 2a–b using DMF as a solvent under microwave‐assisted thermomorphic conditions. At the end of each cycle, the product mixtures were cooled, and then the catalysts were recovered by decantation. The Heck arylation catalyzed by 2b under microwave‐assisted mode exhibited good recycling results favoring the trans product. To our knowledge, this is the first example of cationic Pd‐catalyzed Heck arylation under microwave‐assisted thermomorphic conditions. Additionally, recoverable 3b ‐catalyzed Sonogashira reactions were also achieved successfully in DMF. The reactions under microwave‐assistance gave much better results in yield and in efficiency than that under conventional thermal heating.     

Synthesis of novel coumarin and benzocoumarin derivatives and their biological and photophysical studies

Several derivatives of coumarin‐3N‐carboxamides ( 3‐21 ) have been prepared via the reaction of the coumarin‐3‐carbonyl chloride ( 1 ) with a number of nucleophiles. Novel double‐headed coumarin‐3N‐carboxamides ( 26‐33 ) were also produced using the same method. The Pechmann‐Duisberg reaction was applied to prepare new benzo[f]‐ benzo[h]coumarins and 4‐(chloromethyl)‐pyrano[3,2‐c]coumarin‐2‐one ( 36‐42 ). The reaction of 1‐chloromethylbenzo[f]coumarins ( 36 ) with cyanide anion under different reaction conditions was also investigated in order to assess its suitability for nucleophilic substitution reactions as well as ring transformation products ( 43‐49 ). Synthesis of 1‐((benzo[d]thiazol‐2‐yl)methyl)‐9‐hydroxybenzo[ f ]coumarin ( 50 ) represented the first example of methylene bridge‐head heterocyclecontaining benzo[f]coumarin. Some of the newly prepared coumarins exhibited anti‐bacterial activity against Gram Positive and Gram negative bacteria. Compound 36d was found to be active against all the screened bacteria. Photophysical studies were performed on selected fluorescent benzo[f]‐ and benzo[h]coumarin and the quantum yields were also calculated. All new compounds were characterized by IR, MS, ¹H and ¹³C NMR, as well as elemental analysis.     

Structural elucidation and NMR assignments of four aromatic lactones from a mangrove endophytic fungus (No. GX4‐1B)

Two new aromatic lactones, 6‐hydroxy‐4‐hydroxymethyl‐8‐methoxy‐3‐ methylisocoumarin (1) and 1,10‐dihydroxy‐8‐methyl‐dibenz[b, e]oxepin‐6,11‐dione (2), together with two known compounds, 1,10‐dihydroxy‐dibenz[b, e]oxepin‐6,11‐dione (3) and 3‐hydroxymethyl‐6,8‐dimethoxycoumarin (4), were isolated from a mangrove endophytic fungus (No. GX4‐1B) collected from the South China Sea. Their structures were elucidated and the data of ¹H and ¹³C NMR were assigned completely by HREIMS, 1D and 2D NMR experiments including HMQC, HMBC and NOESY. Copyright © 2010 John Wiley & Sons, Ltd.     

Synthesis of 3-substituted 2-hydroxybenz[f]indolequinones and benz[f]isatinquinone - A new π-acceptor system

Starting from 2,3-dichloro-1,4-naphthaquinone a series of 2-hydroxy-1-methylbenz[f]indolequinones bearing benzyl-, amino- and hydroxy substituents in position 3 , and benz[f]isatinquinone have been synthesised and their reactions have been studied.