Copper‐Catalyzed Aerobic Oxidations of 3‐N‐Hydoxyaminoprop‐1‐ynes to Form 3‐Substituted 3‐Amino‐2‐en‐1‐ones: Oxidative Mannich Reactions with a Skeletal Rearrangement

Cu‐catalyzed aerobic oxidations of readily available 3‐N‐hydroxyaminopro‐1‐ynes with water, alcohols, or thiols to form diverse 3‐substituted 3‐amino‐2‐en‐1‐ones are described. The utility of this catalysis is manifested by a wide scope of applicable N‐hydroxyl propargylamines and nucleophiles, thus enabling the design of one‐pot cascade or two‐step sequential reactions. Besides synthetic significances, such oxidative Mannich reactions are mechanistically interesting because structurally reorganized products were obtained. Our mechanistic studies reveal that the aerobic oxidations involve initial formation of nitrone intermediates, followed by the attack of nucleophiles. Herein, water and MeOH implement the conversion of nitrone intermediates to reaction products in two distinct pathways.     

Photochemical Transformations of Some 2‐(5‐Methylthiophen‐2‐yl)‐3‐[(naphthalen‐2‐yl)methoxy]‐4H‐chromen‐4‐ones Involving Type‐II Process

Photo‐irradiation of 2‐(5‐methylthiophen‐2‐yl)‐3‐[(naphthalen‐2‐yl)methoxy]‐4H‐chromen‐4‐ones yielded the fascinating angular tetracyclic products via cyclization involving both 2‐thienyl ring and naphthylmethoxy group via 1,4‐biradical generated in the Norrish type‐II process. The stereochemical dispositions of the products were determined by MM2 energy minimized programme and spectroscopic analysis.     

Fingerprinting DNA Oxidation Processes: IR Characterization of the 5‐Methyl‐2′‐Deoxycytidine Radical Cation

Methylated cytidine plays an important role as an epigenetic signal in gene regulation. Its oxidation products are assumed to be involved in active demethylation processes but also in damaging DNA. Here, we report the photochemical production of the 5‐methyl‐2′‐deoxycytidine radical cation via a two‐photon ionization process. The radical cation is detected by time‐resolved IR spectroscopy and identified by band assignment using density functional theory calculations. Two final oxidation products are characterized with liquid chromatography coupled to mass spectrometry.     

Photochemical Reactions of Regioisomeric 2,2‐Dimethyl‐5,5‐diphenyl‐ and 5,5‐Dimethyl‐2,2‐diphenyl‐Substituted Diazo Ketones of a Tetrahydrofuran Series

The principal direction of conventional photolysis of the regioisomeric 2,2‐dimethyl‐5,5‐diphenyl‐ and 5,5‐dimethyl‐2,2‐diphenyl‐substituted 4‐diazodihydrofuran‐3(2H)‐ones 1a and 1b , respectively, is the Wolff rearrangement, while other photochemical processes, which are giving rise to the formation of C? H‐insertion, 1,2‐alkyl‐ or ‐aryl‐shifts, as well as H‐atom‐abstraction products occur to a much lower degree (Schemes 2 and 3). The ratio of similar reaction products from both regioisomers 1a and 1b is essentially independent of their structure, and a substantial effect of the relative position of the Ph and diazo group to each other on the yield of C? H‐insertion products does not occur. Based on stereochemical considerations, the Wolff rearrangement of diazodihydrofuran‐3(2H)‐ones apparently proceeds in a concerted manner, whereas the appearance in the reaction mixture of 1,2‐shift and H‐atom‐abstraction products points to the parallel generation during photolysis of singlet and triplet carbenes (Schemes 4 and 5).     

Aza‐Quaternary Scaffolds from Selective Bond Cleavage of Bridgehead‐Substituted 7‐Azabicyclo[2.2.1]heptane: Total Synthesis of (+)‐Cylindricines C–E and (−)‐Lepadiformine A

A novel bridgehead‐substituted aza‐bicyclic framework has been designed and developed in both enantiomeric forms through an asymmetric desymmetrization reaction. Strategic exploitation of the ring strain in the aza‐bicyclic framework has been utilized for the construction of the chiral aza‐quaterenary scaffolds by selective bond fragmentation processes. Furthermore, a strategically designed precursor is employed for selective bond cleavage to initiate a cascade rearrangement for the total synthesis of the 1‐azaspirotricyclic marine alkaloids (+)‐cylindricines C, D, and E, as well as (?)‐lepadiformine A. An oxidation/retro‐aldol/aza‐Michael sequence generated three new chiral centers with the required configuration in one pot.     

Visible Light Promoted β‐C—H Alkylation of β‐Ketocarbonyls via a β‐Enaminyl Radical Intermediate

A 5πe carbonyl activation mode is reported on the basis of photo‐induced single‐electron‐transfer (SET) oxidation of a secondary enamine. The resultant β‐enaminyl radical intermediate was trapped by a wide range of Michael acceptors, producing β‐alkylation products of β‐ketocarbonyls in a highly efficient manner.     

Photochemistry of Tricyclo[5.2.2.02,6]undeca‐4,10‐dien‐8‐ones: An Efficient General Route to Substituted Linear Triquinanes from 2‐Methoxyphenols. Total Synthesis of (±)‐Δ9(12)‐Capnellene

An efficient and short entry to polyfunctionalized linear triquinanes from 2‐methoxyphenols is described by utilizing the following chemistry. The Diels–Alder reactions of masked o‐benzoquinones, derived from 2‐methoxyphenols, with cyclopentadiene afford tricyclo[5.2.2.0^2,6]undeca‐4,10‐dien‐8‐ones. Photochemical oxa‐di‐π‐methane (ODPM) rearrangements and 1,3‐acyl shifts of the Diels–Alder adducts are investigated. The ODPM‐rearranged products are further converted to linear triquinanes by using an O‐stannyl ketyl fragmentation. Application of this efficient strategy to the total synthesis of (±)‐Δ⁹⁽¹²⁾‐capnellene was accomplished from 2‐methoxy‐4‐methylphenol in nine steps with 20 % overall yield.     

A Concise Total Synthesis of (+)‐Tetrabenazine and (+)‐α‐Dihydrotetrabenazine

Highly concise asymmetric total syntheses of (+)‐tetrabenazine ( 1 ), a drug for the treatment of chorea associated with Huntington’s disease, and of (+)‐α‐dihydrotetrabenazine ( 2 ), an active metabolite of 1 , have been accomplished. Our synthetic route features a trans‐selective enol etherification, followed by an unprecedented cation‐dependent aza‐Claisen rearrangement to establish the carbon framework and two stereogenic centers of tetrabenazine. The syntheses consist of seven steps (34 % overall yield) for (+)‐ 2 and eight steps (22 % overall yield) for (+)‐ 1 .     

Spectroelectrochemical Study on the Electrooxidation in Aqueous Medium of some 1,4‐Dihydropyridines: Effects of Substitution in 1‐Position and 4‐Position

Spectroelectrochemical and HPLC characterization of the electrochemical oxidation in aqueous medium of a series of six N‐1 and C‐4 substituted 1,4‐dihydropyridines is presented. Based on the analysis of spectra obtained by in situ spectroscopic measurements it was possible to detect the generation of final oxidation products, which resulted in differences depending of the nature of the substitution on the nitrogen in the dihydropyridine ring. Controlled potential electrolysis (CPE) in aqueous medium was followed by the HPLC technique using EC and PDA detectors. This latter resulted adequately to follow the parent 1,4‐DHP derivatives and their respective oxidation products. Electrochemical oxidation of parent N‐H substituted 1,4‐dihydropyridines generated the corresponding neutral pyridine derivative as final oxidation product. However, the N‐ethyl substituted 1,4‐dihydropyridine derivatives gave rise to the pyridinium salt derivatives.     

Liquid-Phase Synthesis of Methyl （2Z）-2-Arylsulfonylmethyl-2-alkenoates from PEG-Supported a-Phenylselenopropionate

Treatment of lithio derivativ e of novel PEG-supported a-phenylselenopropionate with aldehydes, followed by oxidation-elimination with 30% hydrogen peroxide, formed Baylis-Hillman products, which were then reacted with sodium arylsulfinate. The resulting sulfonylated products were cleaved from the PEG efficiently affording methyl （2Z）-2-arylsulfonylmethyl-2-alkenoates in good yields and high purities.     

Highly trans‐Selective Arylation of Achmatowicz Rearrangement Products by Reductive γ‐Deoxygenation and Heck–Matsuda Reaction: Asymmetric Total Synthesis of (−)‐Musellarins A–C and Their Analogues

Fully functionalized pyranuloses derived from Achmatowicz rearrangement (AR) are versatile building blocks in organic synthesis. However, access to trans‐2,6‐dihydropyrans from pyranuloses remains underexplored. Herein, we report a new two‐step trans arylation of AR products to access 2,6‐trans‐dihydropyranones. This new trans‐arylation method built on numerous plausible, but unsuccessful, direct arylation reactions, including Ferrier‐type and Tsuji–Trost‐type reactions, was finally enabled by an unprecedented, highly regioselective γ‐deoxygenation of AR products by using Zn/HOAc and a diastereoselective Heck–Matsuda coupling. The synthetic utility of the reaction was demonstrated in the first asymmetric total synthesis of (?)‐musellarins A–C and 12 analogues in 11–12 steps. The brevity and efficiency of our synthetic route permitted preparation of enantiomerically pure musellarins and analogues (>20 mg) for preliminary cytotoxicity evaluation, which led us to identify two analogues with three‐to‐six times greater potency than the musellarins as promising new leads.     

Cycloaddition Reaction of 1,4‐Dihydronaphthalene 1,4‐Epoxide with Cyclooctatetraene: Cope Rearrangement in an Adduct

The reaction of 1,4‐dihydro‐1,4‐epoxynaphthalene with cyclooctatetraene at 130±5° for 14 days gave the four products 2a,3,3a,4,9,9a,10,10a‐octahydro‐4,9‐epoxy‐3,10‐ethenocyclobuta[b]anthracene ( 13 ), 25‐oxanonacyclo[10.10.2.2^5,9.1^14,21.0^2,11.0^3,10.0^4,6.0^13,22.0^15,20]heptacosa‐7,15,17,19,23,26‐hexaene ( 14 ), 5,5a,6,6a,6b,6c,12a,12b,12c,13,13a,14‐dodecahydro‐5,14‐epoxy‐6,13‐ethenocycloocta[3′,4′]cyclobuta[1′,2′:3,4]cyclobuta[1,2‐b]anthracene ( 15 ) and bis‐adduct 16 . The structures of the products were determined by spectroscopic methods. It was observed that adduct 14 undergoes a Cope rearrangement. The Cope rearrangement of this adduct was investigated in the temperature range of ?85° to 100° by NMR spectroscopy.     

Aging of a donor conjugated polymer: Photochemical studies of the degradation of poly[2‐methoxy‐5‐(3′,7′‐dimethyloctyloxy)‐1,4‐phenylenevinylene]

This article is devoted to the study of the photoaging and thermal aging of poly[2‐methoxy‐5‐(3′,7′‐dimethyloctyloxy)‐1,4‐phenylenevinylene] (MDMO–PPV; also called OC1C10–PPV) used in organic solar cells. Thin MDMO–PPV films (thickness < 1 μm) were exposed to ultraviolet‐light irradiation (λ > 300 nm) in the presence of air or thermooxidized at 60 °C. The modifications of the chemical structure of the matrix were analyzed with ultraviolet–visible and infrared spectroscopy. The oxidation products that formed were identified by postirradiation treatments, including chemical derivatization reactions. On the basis of the identification of the various products formed, a two‐step radical mechanism is proposed to account for the modification of the chemical structure of the polymeric matrix. It involves first the oxidation of the ether substituent followed by the oxidation of the double bonds. These reactions are responsible for a loss of conjugation of MDMO–PPV, chain scissions, and a decrease in the visible absorbance, which are anticipated to drastically impair the photovoltaic properties of the material. © 2006 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 45: 317–331, 2007     

Synthesis of Iridoid Monoterpenes and Prostaglandins,via Photochemical Rearrangement of Bicyclo[2.2.1]hept‐5‐en‐2‐One

The synthesis of cyclopentanoid natural products, iridoid monoterpenes and prostaglandins, was achieved from a common intermediate 2 , which was obtained from 1 via photochemical rearrangement.     

Concise Stereoselective Synthesis of Oxaspirocycles with 1‐Tosyl‐1,2,3‐triazoles: Application to the Total Syntheses of (±)‐Tuberostemospiroline and (±)‐Stemona‐lactam R

A 4‐substituted‐1‐tosyl‐1,2,3‐triazole‐based stereoselective synthesis of structurally diverse oxaspirocycles is reported. The synthesis involves Rh‐catalyzed loss of nitrogen from 4‐substituted‐1‐tosyl‐1,2,3‐triazoles, Grignard reaction, and a ring‐closing metathesis reaction as key steps. By employing readily available and stable 4‐substituted‐1‐tosyl‐1,2,3‐triazoles as surrogates of diazo compounds and nitrogen sources, two types of oxaspirocycles were obtained. The latter compounds, which contain adjacent nitrogen stereocenters, could serve as the core structures of many natural products. This chemistry has been successfully applied to the total syntheses of (±)‐tuberostemospiroline and (±)‐stemona‐lactam R.     

From Ynamides to Highly Substituted Benzo[b]furans: Gold(I)‐Catalyzed 5‐endo‐dig‐Cyclization/Rearrangement of Alkylic Oxonium Intermediates

A series of arylynamides with alkyloxy groups at the ortho position of the aryl group was prepared through a short alkylation/cross‐coupling/amidation sequence. The gold‐catalyzed conversion of these substrates combined both C? O and C? C formation steps, thus providing benzofurans with amine functionalities at the 2‐position and alkyl groups at the 3‐position. Cross‐over experiments showed that the alkyl‐migration step was an intermolecular process. X‐ray crystal‐structure analysis of two of the products supported our structural assignment. In some cases, the corresponding benzofurans without the alkyl group at the 3‐position were obtained as side‐products, which were formed through a competing protodeauration process.     

Oxydation ausgewählter δ,ϵ- und ϵ,ξ-ungesättigter Alkohole mit Blei(IV)-acetat

The lead tetraacetate (LTA) oxidation of dihydro-γ-jonol ( 2 ) gives the new bicyclic ether 4 in high yield. On the other hand, LTA oxidation of the alcohols 8, 14, 20 , results in the formation of complex mixtures of oxidation products, from which the spiro compounds 10, 16, 22 , the bicyclic ethers 11, 12, 17, 18, 23 , and the carbonyl compounds 13, 19 have been isolated.     

Asymmetric α‐Hydroxylation of Tetralone‐Derived β‐Ketoesters by Using a Guanidine–Urea Bifunctional Organocatalyst in the Presence of Cumene Hydroperoxide

Highly enantioselective catalytic oxidation of 1‐tetralone‐derived β‐keto esters was achieved by using a guanidine–urea bifunctional organocatalyst in the presence of cumene hydroperoxide (CHP), a safe, commercially available oxidant. The α‐hydroxylation products were obtained in 99 % yield with up to 95 % enantiomeric excess (ee). The present oxidation was successfully applied to synthesize a key intermediate of the anti‐cancer agent daunorubicin ( 2 ).     

Diversity Oriented Synthesis of Indoloazepinobenzimidazole and Benzimidazotriazolobenzodiazepine from N1‐Alkyne‐1,2‐diamines

A one‐pot protocol for the diversity oriented synthesis of two N‐polyheterocycles indoloazepinobenzimidazole and benzimidazotriazolobenzodiazepine from a common N¹‐alkyne‐1,2‐diamine building block is described. The approach involves sequential formation of benzimidazole through cyclocondensation and oxidation, which is followed by the formation of either an azepine ring (through alkyne activation and 6‐endo‐dig cyclization, 1,2‐migration with ring expansion, and re‐aromatization), or diazepine and triazole rings through 1,3‐dipolar cycloaddition.     

Fluorine in Peptides: The Synthesis of α‐Fluoro‐β‐Amino Dipeptides by Direct Deoxofluorination/Rearrangement of N‐Seryl Dipeptides

This article describes the stereo‐ and regioselectivity of the deoxofluorination of N‐terminal dipeptides bearing a serine residue to generate, after rearrangement, α‐fluoro‐β‐amine‐terminated dipeptides. The ratio of the rearranged α‐fluorinated regioisomer is increased, relative to the non‐rearranged β‐fluoro isomer, with N‐alkylated amides. Otherwise, an intramolecular H‐bond between the free amine and the amide NH suppresses formation of the key aziridinium intermediate required for α‐fluorination. N‐Methyl and N‐allyl amides give exclusively α‐fluorination products. Subsequent deprotection of the N‐allyl amide to give a α‐fluoro‐β‐amino dipeptide product is demonstrated.