Synthesis of ornithine lactams via diastereoselective photocyclization of 2-amino-4-oxo-4-phenyl-butanoyl amines

The diastereoselective synthesis of ornithine lactams 6-9 via photoinduced -hydrogen abstraction followed by cyclization of the corresponding 1,6-biradicals is described. A highly asymmetric 1,4-induction is observed.     

Intramolecular hydrogen bonding and hydrogen atom abstraction in gas-phase aliphatic amine radical cations

The intramolecular hydrogen atom abstraction by the nitrogen atom in isolated aliphatic amine radical cations is examined experimentally and with composite high-level ab initio methods of the G3 family. The magnitude of the enthalpy barriers toward H-atom transfer varies with the shape and size of the cyclic transition state and with the degree of substitution at the nitrogen and carbon atoms involved. The lower barriers are found for 1,5- and 1,6-abstraction, for chairlike transition states, for abstraction reactions in ionized primary amines, and for abstraction of H from tertiary carbon atoms. In most cases, the internal energy required for 1,4-, 1,5-, and 1,6-hydrogen atom abstraction to occur is less than that required for gas-phase fragmentation by simple cleavage of C-C bonds, which explains why H-atom transfer can be reversible and result in extensive H/D exchange prior to the fragmentation of many low-energy deuterium labeled ionized amines. The H-atom transfer to nitrogen is exothermic for primary amine radical cations and endothermic for tertiary amines. It gives rise to a variety of distonic radical cations, and these may undergo further isomerization. The heat of formation of the gauche conformers of the gamma-, delta-, and epsilon-distonic isomers is up to 25 kJ mol(-1) lower than that of the corresponding trans forms, which is taken to reflect C-H-N hydrogen bonding between the protonated amino group and the alkyl radical site.     

Photolysis of 1-alkylcycloalkanols in the presence of (diacetoxyiodo)benzene and I2. Intramolecular selectivity in the beta-scission reactions of the intermediate 1-alkylcycloalkoxyl radicals

The C-C beta-scission reactions of 1-alkylcycloalkoxyl radicals, generated photochemically by visible light irradiation of CH2Cl2 solutions containing the parent 1-alkylcycloalkanols, (diacetoxy)iodobenzene (DIB), and I2, have been investigated through the analysis of the reaction products. The 1-alkylcycloalkoxyl radicals undergo competition between ring opening and C-alkyl bond cleavage as a function of ring size and of the nature of the alkyl substituent. With the 1-propylcycloheptoxyl, 1-propylcyclooctoxyl,and 1-phenylcyclooctoxyl radicals, formation of products deriving from an intramolecular 1,5-hydrogen atom abstraction reaction from the cycloalkane ring has also been observed. The results are discussed in terms of release of ring strain associated to ring opening, stability of the alkyl radical formed by C-alkyl cleavage, and with cycloheptoxyl and cyclooctoxyl radicals, also in terms of the possibility of achieving a favorable geometry for intramolecular hydrogen atom abstraction.     

Photochemical preparation of highly functionalized 1-indanones

A series of o-alkylphenyl alkyl ketones 1 were synthesized by different methods. The presence of a leaving group X adjacent to the carbonyl group is the special peculiarity of these ketones. Upon irradiation the keto carbonyl group of these compounds undergoes an n-pi* excitation followed by a 1,5-hydrogen migration from the o-alkyl substituent to the carbonyl oxygen atom. The thus formed 1,4-diradicals are subject to a very rapid elimination of acid HX, giving 1,5-diradicals. We called this process spin center shift. After intersystem crossing these diradicals cyclize to 1-indanones 20 in good yields. Depending on the solvent and on substituents, o-alkoxyalkyl ketones 22 or benzo[c]furanes 21 are obtained as byproducts. The mechanism of the cyclization was elucidated by quantum chemical calculations and kinetic measurements.     

Destabilized carbenium ions: α-imidoyl carbenium ions and the electron impact mass spectra of α-haloaldimines and α-haloketimines

A series of α-chloro- and α-bromoketimines compounds (1-9) with different substituents at the α-position and at the imino group has been investigated by electron impact mass spectrometry as possible precursors of the correspondingly substituted α-imidoyl carbenium ion, an important class of destabilized carbenium ions. The main fragmentation of the molecular ions of compounds, 1-9 in the ion source corresponds to an α-cleavage at the imino group; however, fragment ions are also formed by loss of the α-halo substituent. These fragment ions correspond at least formally to α-imidoyl carbenium ions. Their further reactions in dependence on the type of substituents at the imino group and at the α-C atom, were studied by mass-analysed ion kinetic energy and collisional activation mass spectrometry. The results agree with the initial formation of destabilized α-imidoyl carbenium ions but indicate an easy rearrangement of these ions in the presence of suitable alkyl substituents by 1,2- and 1,4-hydrogen shifts to more stable isomers.     

EPR studies of amine radical cations, part 1: thermal and photoinduced rearrangements of n-alkylamine radical cations to their distonic forms in low-temperature freon matrices

The thermal and photochemical transformations of primary amine radical cations (n-propyl 1.+, n-butyl 5.+) generated radiolytically in freon matrices have been investigated by using low-temperature EPR spectroscopy. Assignment of the spectra was facilitated by parallel studies on the corresponding N,N-dideuterioamines. The identifications were supported by quantum chemical calculations on the geometry, electronic structure, hyperfine splitting constants and energy levels of the observed transient radical species. The rapid generation of the primary species by a short exposure (1-2 min) to electron-beam irradiation at 77 K allowed the thermal rearrangement of 1.+ to be monitored kinetically as a first-order reaction at 125-140 K by the growth in the well-resolved EPR signal of the distonic radical cation .C(2CH2CH2NH3+. By comparison, the formation of the corresponding .CH2CH2CH2CH2NH3+ species from 5.+ is considerably more facile and already occurs within the short irradiation time. These results directly verify the intramolecular hydrogen-atom migration from carbon to nitrogen in these ionised amines, a reaction previously proposed to account for the fragmentation patterns observed in the mass spectrometry of these amines. The greater ease of the thermal rearrangement of 5.+ is in accordance with calculations on the barrier heights for these intramolecular 1,5- and 1,4-hydrogen shifts, the lower barrier for the former being associated with minimisation of the ring strain in a six-membered transition state. For 1.+, the 1,4-hydrogen shift is also brought about directly at 77 K by exposure to approximately 350 nm light, although there is also evidence for the 1,3-hydrogen shift requiring a higher energy. A more surprising result is the photochemical formation of the H2C=N. radical as a minor product under hard-matrix conditions in which diffusion is minimal. It is suggested that this occurs as a consequence of the beta-fragmentation of 1.+ to the ethyl radical and the CH2=NH2+ ion, followed by consecutive cage reactions of deprotonation and hydrogen transfer from the iminonium group. Additionally, secondary ion-molecule reactions were studied in CFCl2CF2Cl under matrix conditions that allow diffusion. The propane-1-iminyl radical CH3CH2CH=N. was detected at high concentrations of the n-propylamine substrate. Its formation is attributed to a modified reaction sequence in which 1.+ first undergoes a proton transfer within a cluster of amine molecules to yield the aminyl radical CH3CH2CH2N.H. A subsequent disproportionation of these radicals can then yield the propane-1-imine precursor CH3CH2CH=NH, which is known to easily undergo hydrogen abstraction from the nitrogen atom. The corresponding butane-1-iminyl radical was also observed.     

Organic mass spectrometry—X. Electron impact fragmentations of alkylthio group in 2-alkylthio-5-aminothiazolo[5,4-d] pyrimidines

In order to discuss hydrogen transfer in the skeletal fragmentation of thioethers on electron impact, mass spectra of a series of 2-n-alkylthio-5-aminothiazolo [5,4-d]pyrimidines have been determined. To aid the interpretation of the hydrogen migration, deuterium-labeled compounds which are substituted with deuterium in each position of 2-n-butylthio-5-aminothiazolo-pyrimidines were studied. By correlation of the spectra obtained from such labeled compounds, the initial hydrogen migration in the fragmentation to produce [M ? SH], [MS ? CH₃] and m/e 184 ions is concluded to be as follows: migration of the α-hydrogen atom to the sulfur induces formation of the [M ? SH] ion; migration of the β-hydrogen atom to the sulfur or nitrogen atom by a McLafferty rearrangement induces formation of the m/e 184 ion; and migration of γ-hydrogen atom to the sulfur induces formation of the [M ? SCH₃] ion.     

Platinum(II)-catalyzed cyclization sequence of aryl alkynes via C(sp3)-H activation: a DFT study

The mechanism and intermediates of hydroalkylation of aryl alkynes via C(sp(3))-H activation through a platinum(II)-centered catalyst are investigated with density functional theory at the B3LYP/[6-31G(d) for H, O, C; 6-31+G(d,p) for F, Cl; SDD for Pt] level of theory. Solvent effects on reactions were explored using calculations that included a polarizable continuum model for the solvent (THF). Free energy diagrams for three suggested mechanisms were computed: (a) one that leads to formation of a Pt(II) vinyl carbenoid (Mechanism A), (b) another where the transition state implies a directed 1,4-hydrogen shift (Mechanism B), and (c) one with a Pt-aided 1,4-hydrogen migration (Mechanism C). Results suggest that the insertion reaction pathway of Mechanism A is reasonable. Through 4,5-hydrogen transfer, the Pt(II) vinyl carbenoid is formed. Thus, the stepwise insertion mechanism is favored while the electrocyclization mechanism is implausible. Electron-withdrawing/electron-donating groups substituted at the phenyl and benzyl sp(3) C atoms slightly change the thermodynamic properties of the first half of Mechanism A, but electronic effects cause a substantial shift in relative energies for the second half of Mechanism A. The rate-limiting step can be varied between the 4,5-hydrogen shift process and the 1,5-hydrogen shift step by altering electron-withdrawing/electron-donating groups on the benzyl C atom. Additionally, NBO and AIM analyses are applied to further investigate electronic structure changes during the mechanism.     

Mechanistic investigation of enediyne-connected amino ester rearrangement. Theoretical rationale for the exclusive preference for 1,6- or 1,5-hydrogen atom transfer depending on the substrate. A potential route to chiral naphthoazepines

Memory of chirality (MOC) and deuterium-labeling studies were used to demonstrate that the cascade rearrangement of enediyne-connected amino esters 1a and 1b evolved through exclusive 1,5- or 1,6-hydrogen atom transfer, subsequent to 1,3-proton shift and Saito-Myers cyclization, depending on the structure of the starting material. These results were independently confirmed by DFT theoretical calculations performed on model monoradicals. These calculations clearly demonstrate that in the alanine series, 1,5-hydrogen shift is kinetically favored over 1,6-hydrogen shift because of its greater exergonicity. In the valine series, the bulk of the substituent at the nitrogen atom has a major influence on the fate of the reaction. N-Tosylation increases the barrier to 1,5-hydrogen shift to the benefit of 1,6-hydrogen shift. The ready availability of 1,6-hydrogen atom transfer was explored as a potential route for the enantioselective synthesis of naphthoazepines.     

Zirconocene catalysis in the synthesis of 1,4-dimagnesium reagents: using competitive inhibition to suppress β-hydrogen abstraction

Substituted 1,4-dimagnesium reagents were synthesized by the zirconocene-catalyzed reaction of alkenes with ethylmagnesium reagents in the presence of a methylmagnesium containing additive. Improved selectivity for formation of dimagnesium reagents over monomagnesium reagents was obtained in the presence of the methylmagnesium containing additive. The ratio of mono- to dimagnesiated products was extrapolated from the ratio of alkene to diene in the products formed when the reaction was quenched with allyl bromide. The extent of the increase in the alkene/diene ratio was dependent on the type of organomagnesium halide, with greatest increases (59%) for the alkylmagnesium chlorides. A mechanism for improved selectivity by suppression of β-hydrogen abstraction in the catalytic cycle is presented. Quenching the 1,4-dimagnesium reagents with allyl bromide yielded decadienes.     

Visible-Light-Induced Palladium-Catalyzed Generation of Aryl Radicals from Aryl Triflates

A mild visible-light-induced Pd-catalyzed intramolecular C−H arylation of amides is reported. The method operates by cleavage of a C(sp²)−O bond, leading to hybrid aryl Pd-radical intermediates. The following 1,5-hydrogen atom translocation, intramolecular cyclization, and rearomatization steps lead to valuable oxindole and isoindoline-1-one motifs. Notably, this method provides access to products with readily enolizable functional groups that are incompatible with traditional Pd-catalyzed conditions.     

Abstraction of β-hydrogen vs. alkyl groups in reactions of dialkylzinc compounds and bis(oxazolinyl)borane

An ambiphilic bis(oxazolinyl)borane proligand and zinc dialkyls react via alkyl group transfer or β-hydrogen abstraction. The latter process is favored by formation of a bis(oxazolinyl)borane-zinc adduct that positions a β-hydrogen in the proximity of the Lewis acid center.     

Tantallaaziridines: from synthesis to catalytic applications

Tantallaaziridines are a class of organometallic compounds containing three-membered rings that include a tantalum, carbon and nitrogen atom. Closely related complexes containing the related iminoacyl ligand can be used as starting materials for tantallaaziridine synthesis. Tantallaaziridines can also be synthesized by reduction of imines or β-hydrogen abstraction of amides to give stable, isolable complexes. Tantallaaziridines possess a reactive Ta-C bond that can undergo stoichiometric transformations with unsaturated organic molecules to give new organometallic products. Upon quenching of such reactions with aqueous workup, selectively substituted small molecule amines can be prepared. Tantallaaziridines have also been proposed as catalytic intermediates in the direct α-alkylation of amines, hydroaminoalkylation, by exploiting the β-hydrogen abstraction route to regenerate the catalytically active species. Recent progress and remaining challenges in the field will be discussed.     

Hypochlorite-mediated fragmentation of hyaluronan, chondroitin sulfates, and related N-acetyl glycosamines: evidence for chloramide intermediates, free radical transfer reactions, and site-specific fragmentation

Myeloperoxidase released from activated phagocytes reacts with H(2)O(2) in the presence of chloride ions to give hypochlorous acid. This oxidant has been implicated in the fragmentation of glycosaminoglycans, such as hyaluronan and chondroitin sulfates. In this study it is shown that reaction of HOCl with glycosaminoglycans and model compounds yields chloramides derived from the N-acetyl function of the glycosamine rings. The results of EPR spin trapping and product studies are consistent with the formation of amidyl radicals from these chloramides via both metal ion-dependent and -independent processes. In the case of glycosaminoglycan-derived amidyl radicals, evidence has been obtained in studies with model glycosides that these radicals undergo rapid intramolecular abstraction reactions to give carbon-centered radicals at C-2 on the N-acetyl glycosamine rings (via a 1,2-hydrogen atom shift) and at C-4 on the neighboring uronic acid residues (via 1,5-hydrogen atom shifts). The C-4 carbon-centered radicals, and analogous species derived from model glycosides, undergo pH-independent beta-scission reactions that result in glycosidic bond cleavage. With N-acetyl glucosamine C-1 alkyl glycosides, product formation via this mechanism is near quantitative with respect to chloramide loss. Analogous reactions with the glycosaminoglycans result in selective fragmentation at disaccharide intervals, as evidenced by the formation of "ladders" on gels; this selectivity is less marked under atmospheric oxygen concentrations than under anoxic conditions, due to competing peroxyl radical reactions. As the extracellular matrix plays a key role in mediating cell adhesion, growth, activation, and signaling, such HOCl-mediated glycosaminoglycan fragmentation may play a key role in disease progression and resolution, with the resulting fragments modulating the magnitude and quality of the immune response in inflammatory conditions.     

Effect of secondary MO interaction on the regiospecificity in the reactions of tf-ionones with singlet oxygen

The ene reactions of a-ionones with singlet oxygen were examined to ascertain the effect of secondary MO interaction between the reactants on the reaction regiospecificity. Exclusive formation of 3-hydroxy-V-ionones found in the reactions reveals favorable interaction of singlet oxygen with the acyclic fl-hydrogen atom. On the other hand, no formation of 3-hydroxy-0-ionones implies that the steric requirement was not met for the bond formation between zwitterionic perepoxide with Ci-hydrogen in the process. The MMP21 and MNDO calculations indicate minus value of the secondary interaction energy for the acyclic a-hydrogen abstraction and a repulsion between the oxygen with C₁-hydrogen atom. Twisting tilting of the double bond may account for favorable attack of singlet oxygen on C3. An explanation of the excellent regiospecificity was addressed and placed in proper mechanic prospective.     

H‐atom abstraction from selected C?H bonds in 2,3‐dimethylpentanal, 1,4‐cyclohexadiene,and 1,3,5‐cycloheptatriene

The gas‐phase reactions of OH radicals with 1,4‐cyclohexadiene, 1,3,5‐cycloheptatriene, and 2,3‐dimethylpentanal have been investigated to determine the importance of H‐atom abstraction at specific positions in these molecules. Benzene was observed as a product of the reaction of OH radicals with 1,4‐cyclohexadiene in 12.5 ± 1.2% yield, in good agreement with a previous study and indicating that this is the fraction of the reaction proceeding by H‐atom abstraction from the allylic C? H bonds. In contrast, no formation of tropone from 1,3,5‐cycloheptatriene was observed, suggesting that in this case H‐atom abstraction is not important. For the reaction of OH radicals with 2,3‐dimethylpentanal, formation of 3‐methyl‐2‐pentanone was observed in 5.4 ± 1.0% yield (after correction for reaction of 3‐methyl‐2‐pentanone with OH radicals), and this product is predicted to be formed after initial H‐atom abstraction from the 2‐position CH group. Acetaldehyde and 2‐butanone were also observed as products, with initial yields of ～90% and ～26%, respectively, and their formation appeared to involve, at least in part, an intermediary acyl peroxy radical. Using a relative rate method, the measured rate constants for the reactions of OH radicals with 2,3‐dimethylpentanal, 3‐methyl‐2‐pentanone, and tropone are (in units of 10^?12 cm³ molecule^?1 s^?1) 2,3‐dimethylpentanal, 42 ± 7; 3‐methyl‐2‐pentanone, 6.87 ± 0.08; and tropone, 42 ± 6. © 2003 Wiley Periodicals, Inc. Int J Chem Kinet 35: 415–426, 2003     

H-abstraction prevails over α-cleavage in the solution and solid state photochemistry of cis-2,6-di(1-cyclohexenyl)cyclohexanone

The photochemistry of cis-2,6-di(1-cyclohexenyl)cyclohexanone was studied in solution and in crystals to determine its photoreactivity and chemoselectivity. Although 1,3-acyl shifts and the oxadi-π-methane rearrangement products are possible for the β,γ-unsaturated chromophore, an efficient intramolecular abstraction of an allylic γ-hydrogen and small amounts of α-cleavage and decarbonylation were observed. The mechanism of the Norrish type-II reaction and the selectivity of product formation were analyzed in terms of structural information obtained by X-ray diffraction analysis.     

A density-functional-theory study of atomic nitrogen abstraction from Si(100)-(2 x 1) by a gaseous O(3P) atom

We have employed density-functional theory (DFT) to investigate the abstraction of a nitrogen atom from the Si(100)-(2 x 1) surface by a gas-phase O(3P) atom for different initial bonding configurations of nitrogen at the surface. For the N-Si(100) structures investigated, nitrogen abstraction by an O(3P) atom is predicted to be exothermic by at least 1.9 eV. Abstraction in a single elementary step is found only for the interaction of an O(3P) atom with nitrogen bound in a coordinatively saturated configuration, and an energy barrier of 0.20 eV is computed for this reaction. For nitrogen bound in coordinatively unsaturated configurations, abstraction is predicted to occur by precursor-mediated pathways in which the initial O-surface collision results in the formation of a N-O bond and the concomitant release of between 2.7 and 4.8 eV of energy into the surface, depending on the initial N-Si(100) structure. This initial step produces different surface structures containing an adsorbed NO species, which can then undergo a series of elementary steps leading to NO desorption. Since the barriers for these steps are found to be less than 1 eV in all cases, a significant excess of energy is available from initial N-O bond formation that could activate NO desorption within no more than a few vibrational periods after the initial gas-surface collision. Nitrogen abstraction by such a pathway is essentially an Eley-Rideal process since NO desorption occurs rapidly after the initial gas-surface collision, without the reactants thermally accommodating with the surface. These computational results indicate that nitrogen abstraction by gaseous O(3P) atoms should be facile, even at low surface temperatures, if nitrogen is bound to the Si(100) surface in coordinatively unsaturated configurations.     

Flash vacuum pyrolysis of methoxy-substituted lignin model compounds

The flash vacuum pyrolysis (FVP) of methoxy-substituted beta-O-4 lignin model compounds has been studied at 500 degrees C to provide mechanistic insight into the primary reaction pathways that occur under conditions of fast pyrolysis. FVP of PhCH(2)CH(2)OPh (PPE), a model of the dominant beta-O-4 linkage in lignin, proceeds by C-O and C-C cleavage, in a 37:1 ratio, to produce styrene plus phenol as the dominant products and minor amounts of toluene, bibenzyl, and benzaldehyde. From the deuterium isotope effect in the FVP of PhCD(2)CH(2)OPh, it was shown that C-O cleavage occurs by homolysis and by 1,2-elimination in a ratio of 1.4:1, respectively. Methoxy substituents enhance the homolysis of the beta-O-4 linkage, relative to PPE, in o-CH(3)O-C(6)H(4)OCH(2)CH(2)Ph (o-CH(3)O-PPE) and (o-CH(3)O)(2)-C(6)H(3)OCH(2)CH(2)Ph ((o-CH(3)O)(2)-PPE) by a factor of 7.4 and 21, respectively. The methoxy-substituted phenoxy radicals undergo a complex series of reactions, which are dominated by 1,5-, 1,6-, and 1,4-intramolecular hydrogen abstraction, rearrangement, and beta-scission reactions. In the FVP of o-CH(3)O-PPE, the dominant product, salicylaldehyde, forms from the methoxyphenoxy radical by a 1,5-hydrogen shift to form 2-hydroxyphenoxymethyl radical, 1,2-phenyl shift, and beta-scission of a hydrogen atom. The 2-hydroxyphenoxymethyl radical can also cleave to form formaldehyde and phenol in which the ratio of 1, 2-phenyl shift to beta-scission is ca. 4:1. In the FVP of o-CH(3)O-PPE and (o-CH(3)O)(2)-PPE, products (ca. 20 mol %) are also formed by C-O homolysis of the methoxy group. The resulting phenoxy radicals undergo 1,5- and 1,6-hydrogen shifts in a ratio of ca. 2:1 to the aliphatic or benzylic carbon, respectively, of the phenethyl chain. In the FVP of (o-CH(3)O)(2)-PPE, o-cresol was the dominant product. It was formed by decomposition of 2-hydroxy-3-hydroxymethylbenzaldehyde and 2-hydroxybenzyl alcohol, which are formed from a complex series of reactions from the 2, 6-dimethoxyphenoxy radical. The key step in this reaction sequence was the rapid 1,5-hydrogen shift from 2-hydroxy-3-methoxybenzyloxy radical to 2-hydroxymethyl-6-methoxyphenoxy radical before beta-scission of a hydrogen atom to give the substituted benzaldehyde. The 2-hydroxybenzyl alcohols rapidly decompose under the reaction conditions to o-benzoquinone methide and pick up hydrogen from the reactor walls to form o-cresol.     

Communication: Double Bond Migration of a 1,5-Anhydro-3-C-p-Tolylsulfonyl-D-Hex-2-Enitol Derivative and the Corresponding 5a-Carba-Dl-Sulfonyl Sugar

Although the rate of proton abstraction (kinetic acidity) frequently plays an essential role in determination of reaction pathways and is of theoretical interest,¹ it is still controversial whether an oxygen atom activates or deactivates the abstraction of an α-hydrogen atom of an ether. For example, it is well known that oxidative elimination of a seleno group gives an allyl ether as the major product, indicating the oxygen atom deactivates the kinetic acidity.² Abstraction of the equatorial hydrogen atom at C-2 of 6-methyl-1,3-oxathiane-3,3-dioxide 1 is slower than that at C-4.³ On the other hand, the bridgehead hydrogen atom (H_b) adjacent to the oxygen atom of piperazinedione (2) is abstracted more readily than that of the alternative one (H_a).⁴