Relative reactivity of peracids versus dioxiranes (DMDO and TFDO) in the epoxidation of alkenes. A combined experimental and theoretical analysis

Comparative analysis of the calculated gas-phase activation barriers (DeltaE++) for the epoxidation of ethylene with dimethyldioxirane (DMDO) and peroxyformic acid (PFA) [15.2 and 16.4 kcal/mol at QCISD(T)// QCISD/6-31+G(d,p)] and E-2-butene [14.3 and 13.2 kcal/mol at QCISD(T)/6-31G(d)//B3LYP/6-311+G(3df,2p)] suggests similar oxygen atom donor capacities for both oxidants. Competition experiments in CH(2)Cl(2) solvent reveal that DMDO reacts with cyclohexene much faster than peracetic acid/acetic acid under scrupulously dried conditions. The rate of DMDO epoxidation is catalyzed by acetic acid with a reduction in the classical activation barrier of 8 kcal/mol. In many cases, the observed increase in the rate for DMDO epoxidation in solution may be attributed to well-established solvent and hydrogen-bonding effects. This predicted epoxidative reactivity for DMDO is not consistent with what has generally been presumed for a highly strained cyclic peroxide. The strain energy (SE) of DMDO has been reassessed and its moderated value (about 11 kcal/mol) is now more consistent with its inherent gas-phase reactivity toward alkenes in the epoxidation reaction. The unusual thermodynamic stability of DMDO is largely a consequence of the combined geminal dimethyl- and dioxa-substitution effects and unusually strong C-H and C-CH(3) bonds. Methyl(trifluoromethyl)dioxirane (TFDO) exhibits much lower calculated activation barriers than DMDO in the epoxidation reaction (the average DeltaDeltaE++ values are about 7.5 kcal/mol). The rate increase relative to DMDO of approximately 10(5), while consistent with the higher strain energy for TFDO (SE approximately 19 kcal/mol) is attributed largely to the inductive effect of the CF(3) group. We have also examined the effect of alkene strain on the rate of epoxidation with PFA. The epoxidation barriers are only slightly higher for the strained alkenes cyclopropene (DeltaE++ = 14.5 kcal/mol) and cyclobutene (DeltaE++ = 13.7 kcal/mol) than for cyclopentene (DeltaE++ = 12.1 kcal/mol), reflecting the fact there is little relief of strain in the transition state. Alkenes strained by twist or pi-bond torsion do exhibit much lower activation barriers.     

The kinetic regularities, products, and mechanism of the thermal decomposition of dimethyldioxirane. The contribution of molecular and radical reaction channels

The products and kinetics of the thermal decomposition of dimethyldioxirane (DMDO) were studied. The reaction proceedsvia three parallel pathways: isomerization to methyl acetate, oxygen atom insertion into the C−H bond of a solvent molecule (acetone), and the solvent-induced homolysis of the O−O bond in the DMDO molecule. The contribution of the latter reaction channel isca. 23% at 56°C. The overall kinetic parameters of DMDO thermolysis in oxygen atmosphere were determined. The free radical-induced DMDO decomposition occurs in an inert atmosphere. The formal kinetics of this reaction was investigated. The mechanism of the DMDO thermolysis is discussed. Dedicated to Professor E. T. Denisov on the occasion of his 70th Birthday. Published inIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 8, pp. 1344–1354, August, 2000.     

Effect of geminal substitution on the strain energy of dioxiranes. Origin of the low ring strain of dimethyldioxirane

The strain energies (SE) for dioxirane (DO) dimethyldioxirane (DMDO) and related dioxiranes have been examined by several methods using high-level computational schemes (G2, G2(MP2), CBS-Q). A series of calculated O-O, C-O, and O-H bond dissociation energies (G2) point to special problems associated with classical homodesmotic reactions involving peroxides. The relative SEs of DO, DMDO, methyl(trifluoromethyl)dioxirane (TFDO), and difluorodioxirane (DFDO) have been estimated by combination of the dioxirane with cyclopropane to form the corresponding 1,3-dioxacyclohexane. The relative SE predicted for DMDO (2) is 7 kcal/mol lower than that of DO, while the SE of 1,1-difluorodioxirane (4) is 8 kcal/mol higher. The most reactive dioxirane, methyl (trifluoromethyl)dioxirane (3), has an estimated SE just 1 kcal/mol greater than that of DO but 8 kcal/mol greater than that of DMDO. Six independent methods support the proposed SE for DO of 18 kcal/mol. The SE of the parent dioxirane (DO) has been estimated relative to six-membered ring reference compounds by dimerization of dioxirane and or its combination with cyclopropane. The relative SE of cyclic hydrocarbons, ethers and peroxides have been predicted by the insertion/extrusion of -CH(2)- and -O- fragments into their respective lower and next higher homologues. The moderated SE of DMDO (approximately equal to 11 kcal/mol) has also been estimated on the basis of group equivalent reactions. The unusual thermodynamic stability of DMDO is largely a consequence of combined geminal dimethyl and dioxa substitution effects and its associated strong C-H bonds and C-CH(3) bonds. The data clearly demonstrate that the reference compounds used to estimate the SE for highly substituted small ring cyclic compounds should reflect their molecular architecture having the same substitutents on carbon.     

Oxyfunctionalization products of terpenoids with dimethyldioxirane and their biological activity

Oxyfunctionalization of the bioactive terpenoids, ursolic acid acetate (1), oleanolic acid acetate (5), lupeol acetate (12), and kaurenic acid (17), with dimethyldioxirane (DMDO) was investigated. Treatment of the terpenoids with DMDO under mild conditions afforded a variety of oxidation and oxydegradation products to yield naturally occurring and/or novel compounds in one step. After chromatographic separation, the structures of the individual isolated products were determined using spectroscopic methods including several homonuclear (1H-1H) and heteronuclear (1H-13C) shift-correlated 2D-NMR techniques. The inhibitory activity of the terpenoid derivatives against alpha-glucosidase was investigated and compounds 1, 3, 7, and 9 were found to exhibit potent activity.     

Synthesis and characterization of energetic 3-nitro-1,2,4-oxadiazoles

All new: 3-Nitro-5-guanidino-1,2,4-oxadiazole (NOG) was synthesized from diaminoglycoluril with in situ generated dimethyldioxirane (DMDO). The impact sensitivity of NOG is more than 40?J with a decomposition temperature of 290?°C. Some other energetic derivatives have been prepared and characterized.     

The effect of substitutents on the strain energies of small ring compounds

The effect of substitutents on the strain energy (SE) of cyclic molecules is examined at the CBS, G2, and G2(MP2) levels of theory. Alkyl substitutents have a meaningful effect upon the SE of small ring compounds. gem-Dimethyl substitution lowers the strain energy of cyclopropanes, cyclobutanes, epoxides, and dimethyldioxirane (DMDO) by 6-10 kcal/mol relative to an unbranched acyclic reference molecule. The choice of the reference compound is especially important for geminal electronegative substitutents. The SE of 1,1-difluorocyclopropane is estimated to be 20.5 kcal/mol relative to acyclic reference molecule 1,3-difluoropropane but is 40.7 kcal/mol with respect to the thermodynamically more stable (DeltaE = -20.2 kcal/mol) isomeric reference compound 2,2-difluoropropane. The SE of dioxirane (DO) is estimated to be approximately 18 kcal/mol while the SE of DMDO is predicted to be approximately equal to 11 kcal/mol by using homodesmotic reactions that maintain a balanced group equivalency. The total energy (CBS-APNO) of DMDO is 2.6 kcal/mol lower than that of isomeric 1,2-dioxacyclopentane that has an estimated SE of 5 kcal/mol. The thermodynamic stability of DMDO is a consequence of its relatively strong C-H (BDE = 102.7 kcal/mol) and C-CH(3) (BDE = 98.9 kcal/mol) bonds. By comparison, the calculated sec-C-H and -C-CH(3) G2 bond dissociation energies in propane are 100.3 and 90.5 kcal/mol.     

柚皮苷半合成生物活性黄酮醇和橙酮类化合物研究

以柚皮苷为原料,经过糖苷水解、脱氢、苄基保护、O-甲基化、过氧丙酮(DMDO)氧化或阿尔格-弗林-大山田(Algar-Flynn-Oyamada)反应和脱苄基保护等反应步骤,半合成了山萘酚(1,Kaemferol),5,7,4’-三甲氧基黄酮醇(2)、3,5-二羟基-7,4’-二甲氧基黄酮醇(3),鼠李柠檬素(4,Rhamnocitrin)等4种天然黄酮醇类和4,6,4’-三羟基二氢橙酮(5)、4-羟基-6,4’-二甲氧基二氢橙酮(6)两种新的橙酮类化合物.重点探讨了过氧丙酮(DMDO)直接氧化黄酮制备黄酮醇和Algar-Flynn-Oyamada反应制备橙酮的合成方法,改进优化了反应条件.所有合成化合物的结构已通过1H NMR,MS和IR等波谱方法进行了确认.该合成途径原料易得,工艺简便,收率较高,具有较高的应用价值.     

NMR studies on epoxidations of allenamides. Evidence for formation of nitrogen-substituted allene oxide and spiro-epoxide via trapping experiments

Two epoxidations of chiral allenamides are described here. While treatment with m-CPBA led to highly stereoselective formation of an alpha-keto aminal that can be useful synthetically, DMDO oxidation led to conclusive evidence for both nitrogen-substituted allene oxide (via mono-epoxidation) and spiro-epoxide (via bis-epoxidation) using intramolecular nucleophilic trapping experiments. NMR studies provide reliable evidence for a 3-oxetanone that can be derived from the spiro-epoxide and also suggest the presence of an allene oxide. Despite a facile second epoxidation as evidenced by the predominant formation of the 3-oxetanone, in the presence of furan, [4 + 3] cycloaddition of the nitrogen-substituted allene oxide or oxyallyl cation with furan occurs faster than the second epoxidation efficiently leading to cycloadducts. This rate difference plays an invaluable role for the success of a stereoselective sequential epoxidation-[4 + 3] cycloaddition reaction via DMDO epoxidations of chiral allenamides.     

An efficient methodology to substituted furans via oxidation of functionalized α-diazo-β-ketoacetates

DMDO oxidation of functionalized α-diazo-β-ketoacetates, formed by zinc triflate catalyzed Mukaiyama-aldol condensation of methyl diazoacetoacetate with aldehydes, occurred in quantitative yield to form dihydrofuranols that undergo acid catalyzed dehydration under mild conditions to generate 3-methoxyfuran-2-carboxylates in good yield.     

Use of dimethyldioxirane in the epoxidation of the main constituents of the essential oils obtained from Tagetes lucida, Cymbopogon citratus, Lippia alba and Eucalyptus citriodora

Dimethyldioxirane (DMDO), a widely used oxidant in organic synthesis is considered an environmentally friendly oxygen transfer reagent because acetone is the only byproduct formed in its oxidation reactions. This work describes the isolation of the main constituents (terpenes) in the essential oils obtained from Tagetes lucida, Cymbopogon citratus, Lippia alba and Eucalyptus citriodora, their epoxidation with DMDO in acetone solution and the characterization of the resulting epoxides by GC-MS (EI) and NMR. This is one of the first reports involving the application of dioxirane chemistry to essential oils in order to generate modified compounds with potential uses in several areas of medicine and industry.     

From azides to nitro compounds in a few seconds using HOF.CH3CN

HOF.CH3CN, a very efficient oxygen-transfer agent, was reacted with various azides to form the corresponding nitro compounds in excellent yields and in very short reaction times. The respective nitroso derivatives were found to be intermediates in this reaction. When the azides were reacted with MCPBA or DMDO, no reaction took place, and the starting materials were fully recovered.     

New oxidative tools for the functionalization of the cephalostatin north 1 hemisphere

Dimethyldioxirane (DMDO) C-H oxidation of ketone 17 to hemiketal 18 (82%), bis-dehydration to vinyl ether 21 (77%), and DMDO again provides C-23 axial alcohol 23 (99%). Routine processing, including a double-stereoselective Sharpless AD reaction (de >98%), gives alcohols 7 and 32. C-23 deoxy substrate 7 undergoes Suarez hypoiodite oxidative cyclization to (natural) beta spiroketal 34, but compound 32, bearing a C-23 silyl ether, generates unnatural spiroketal 33. [reaction: see text]     

Use of acyl substituents to favour 2,3-epoxidation of 5,7-dioxygenated flavones with dimethyldioxirane

The reaction of 5,7-dimethoxyflavone with dimethyldioxirane (DMDO) gives the 2,3-epoxide rapidly at first. However, low levels of ring A hydroxylated by-products are also formed. With increasing proportions of DMDO, demethylation at C-5 becomes apparent and consumption of substrate is not matched by further significant build-up of the epoxide. Deactivation of ring A by the use of acyl groups removes this complication. 5,7-Diacylflavones give excellent yields of epoxides and monoacyl derivatives also react in good yield. Ionization potential maps derived from density functional theory calculations (B3LYP/6-31G^∗), provide good visual indicators of the relative reactivity of the key nucleophilic loci. The epoxides may be isolated as such, or transformed into flavonols by treatment with p-toluenesulfonic acid.     

Stereoselective Synthesis of syn-and anti-3a-Hydroxyl-1,2,3,3a,8,8a-hexahydropyrrolo[2,3-b] indole-2-carboxylic Acid

The structure of syn-and anti-N^b-(p-toluenesulfonyl)-3a-hydroxyl-1,2,3,3a,8,8a-hexahydro pyrrolo[2,3,-b]indole-2-carboxylic t-butyl ester was stercoselectively synthesized by oxidative ring formation of N^b-(p-toluenesulfonyl)-L-tryptophan t-butyl ester in methylene chloride containing dimethyldioxirane(DMDO),the p-toluenesulfonly group and t-butyl group can be easily removed by sodium naphthalenide and trifluoroacetic acid,respectively.     

Synthesis of alpha-keto-imides via oxidation of ynamides

A de novo preparation of alpha-keto-imides via ynamide oxidation is described. With a number of alkyne oxidation conditions screened, a highly efficient RuO2-NaIO4 mediated oxidation and a DMDO oxidation have been identified to tolerate a wide range of ynamide types. In addition to accessing a wide variety of alpha-keto-imides, the RuO2-NaIO4 protocol provides a novel entry to the vicinal tricarbonyl motif via oxidation of push-pull ynamides, and imido acylsilanes from silyl-substituted ynamides. Chemoselective oxidation of ynamides containing olefins can be achieved by using DMDO, while the RuO2-NaIO4 protocol is not effective. These studies provide further support for the synthetic utility of ynamides.     

Controlled epoxidation of poly(styrene‐b‐isoprene‐b‐styrene) block copolymer for the development of nanostructured epoxy thermosets

To be used as templates for nanostructured thermosets, a commercial poly(styrene‐b‐isoprene‐b‐styrene) (SIS) block copolymer (BCP) was epoxidized by three different epoxidation procedures. An exhaustive analysis of methodologies using metal catalyzed/hydrogen peroxide, dimethyldioxirane (DMDO), and meta‐chloroperbenzoic acid (m‐CPBA) was performed to obtain reactive BCPs. The DMDO approach was the best strategy to obtain highly epoxidized SIS BCP (85 mol %) without formation of side products. Careful control in BCP epoxidation by metal catalyzed/hydrogen peroxide and m‐CPBA approaches led to a maximum epoxidation degree (ED) of approximately 60 mol % without the formation of side products. The ED by metal catalyzed/hydrogen peroxide strategy could be further increased to 69 mol %, but a significant amount of crosslinking, ring opening, and polymer chain scission reactions were detected by spectroscopic and chromatographic techniques. The miscibility of epoxidized BCPs with diglycidyl ether of bisphenol‐A epoxy system before and after curing was analyzed to develop nanostructured epoxy thermosets. For ED higher than 69 mol %, BCPs were miscible, while those with lower ED presented macrophase separation. Highly epoxidized BCPs obtained by the DMDO methodology were successfully used to obtain ordered nanodomains inside the epoxy matrix, as determined by atomic force microscopy. © 2011 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem, 2011     

Oxidation of ethers with dimethyldioxirane

Oxidation of a series of tert-butyl ethers Bu^tOR (R = Me, Et, CH₂CH₂Cl, Prⁱ, Buⁱ), diethyl ether, diisopropyl ether, 1,2-dimethoxyethane, diisobutoxymethane, 1,4-dioxane, and tetrahydrofuran with dimethyldioxirane (DMDO) was studied. The reaction kinetics obeys the second-order equation w = k[DMDO][ether]. The rate constants in a range of 5–50 °C and the activation parameters of the reaction were determined. The solvent effect on the oxidation rate was studied. The oxidation products are the corresponding alcohols and carbonyl compounds. The competition between the nonradical (oxygen insertion) and radical mechanisms of the reaction is discussed. The reactions of the parent dioxirane and DMDO with a series of methyl ethers MeOr’ (r’ = Me, Et, CH₂CH₂F, Prⁱ) were studied by the density functional theory (DFT). The (U)B3LYP-6-311G(d,p) method was employed to calculate the geometry and energies of the reactants and transition states. The data obtained indicate a possible increase in the probability of oxidation via the radical route and an increase in the activation barrier for the substrates containing electron-withdrawing substituents. Published in Russian in Izvestiya Akademii Nauk. Seriya Khimicheskaya, No. 10, pp. 2309–2318, October, 2005.     

Selective Epoxidation of Polar Substrates by Dimethyldioxirane

epoxides of highly inactivated double bounds can be obtained using DMDO, after transformation of deactivating esters into tetrabutylammonium salts. Reactions are quantitative and no further purification is required.     

Dye-sensitized photooxygenation of sugar-furans as synthetic strategy for novel C-nucleosides and functionalized exo-glycals

The methylene blue-sensitized photooxygenation of β-ribofuranosyl furan 1e followed by in situ Et₂S treatment afforded the conformationally stable β-ribofuranoside 4e almost quantitatively. The latter was converted to pyridazine C-nucleoside 6e by cyclization with NH₂NH₂ and to pyrazoline 7e through a 1,3-dipolar cycloaddition with diazomethane. Attempts to epoxidize the double bond failed both by dimethyldioxirane (DMDO), which left 4e unchanged, and by NEt₃/t-BuOOH or NaOO-t-Bu which respectively afforded the new and unexpected exo-glycals E,Z-8e and the novel furan derivative 9.     

Developing a diastereoselective intramolecular [4+3] cycloaddition of nitrogen-stabilized oxyallyl cations derived from N-sulfonyl-substituted allenamides

Efforts toward achieving a practical and diastereoselective intramolecular [4+3] cycloaddition of nitrogen-stabilized oxyallyl cations with tethered dienes are described. Epoxidation of N-sulfonyl substituted allenamides with dimethyldioxirane (DMDO) generates nitrogen-stabilized oxyallyl cations that readily undergo stereoselective [4+3] cycloaddition with dienes. Selectivity is found to depend on the tethering length as well as the stability of the oxyallyl cation intermediate, whether generated from N-carbamoyl- or N-sulfonyl-substituted allenamides. The use of chiral N-sulfonyl-substituted allenamides provided minimal diastereoselectivity in the cycloaddition, while high diastereoselectivity can be achieved with a stereocenter present on the tether. These studies provide further support for the synthetic utility of allenamides.