Iridium complexes of dehydroamino acids: The kinetic resolution of racemic diphosphines and their application in catalytic asymmetric hydrogenation

The reaction of chiral diphosphines with a configurationally pure cationic bis-enamide complex of iridium, bis(menthyl (Z)-α-benzamidocinnamate)-iridium tetrafluoroborate, is described. When the reactant ligand is racemic then kinetic resolution occurs with high specificity under the appropriate conditions. Since the iridium diphosphine complex is catalytically inactive in homogeneous hydrogenation, the residual enantiomer may be reacted with bis(norbornadiene)-rhodium tetrafluoroborate to produce an active catalyst. This effects the hydrogenation of methyl (Z)-α-acetamidocinnamate in optical yields comparable with those obtained separately with the enantiomerically pure ligand rhodium complex. The reaction of pure (+)- or (-)-enantiomer of bis(menthyl (Z)-α-benzamidocinnamate)-iridium tetrafluoroborate with enantiomerically pure diphosphines has been studied. Invariably one hand of the diphosphine reacts rapidly with a given enantiomer of the iridium complex to give a stable diphosphine iridium enamide complex in which the original configuration of the coordinated olefin is maintained. The other combination of enantiomers reacts much more slowly, in keeping with the kinetic resolution work, and produces an enamide complex which is unstable in solution, isomerising to a second diastereomer. Since the absolute configuration of the iridium bis-enamide complex has been established by X-ray crystallography, this experiment affords a method of determining the configuration of rhodium enamide complexes in asymmetric hydrogenation (assuming structural homology between Rh and Ir). In all cases the disfavoured enamide complex was the one involved in the catalytic pathway.     

The hydrogenation and hydroformylation of alkenes as catalyzed by polymer-anchored rhodium trichloride under water gas shift reaction conditions

The ‘heterogenized’ water gas shift catalyst Rh/P4VP, prepared from the reaction of RhCl₃ with poly(4-vinylpyridine), is also active for hydrogenation and hydroformylation of 1-hexene and cyclohexene in aqueous ethoxyethanol under mild shift reaction conditions (typically 0.9 atm. P_CO at 100°C). The catalytic activities for these systems were studied as functions of several experimental variables. Hydroformylation rates increased with the P_CO but exhibited saturation behavior in the 1.5 atm. range. Rates for cyclohexane and hexane production were inhibited by CO at higher pressures. Cyclohexene hydroformylation and hydrogenation turnover frequencies were independent of the polymer-loading (50–150 μM RhCl₃/1.0 g P4VP) indicating that the active species are of the same nuclearity as the principal species present. The temperature dependence did not follow simple Arrhenius behavior, but appeared segmented. These data are discussed in terms of possible mechanisms.     

Labeling of steroids with tritium

Conditions have been elaborated for the tritium labeling of some steroids to a molar activity of the order of 1 TBk/mol by heterogeneous catalytic isotopic exchange. For steroids without a keto group, isotopic exchange with gaseous tritium is most effective in neutral solvents, whereas for steroids with a keto group an alkaline medium is preferable. At certain pH values it was possible to void hydrogenation of the double bonds in the compounds.     

Synthesis, characterization and application of Ru(BINAP) (Acac) (MNAA) (MeOH), a highly effective catalyst for the asymmetric hydrogenation of 2-(6′-methoxynaphth-2′-yl)acrylic acid

Ru(S-BINAP) (Acac) (MNAA) (MeOH) (1) (where MNAA (2) = 2-(6′-methoxynaphth-2′-yl)acrylate anion), a highly effective catalyst for the asymmetric hydrogenation of 2-(6′-methoxynaphth-2′-yl) acrylic acid (3), was isolated from a dichloromethane/methanol (vol./vol. = 1/4) solution of Ru(S-BINAP) (Acac)₂ and excess of 2-(6′-methoxynaphth-2′-yl)acrylic acid after the solution was exposed to visible light for 2 weeks. On side by side comparison studies, the rate of the hydrogenation of 3 catalyzed by 1 was found to be substantially faster than the same reaction catalyzed by Ru(S-BINAP) (OAc)₂. The molecular structure of 1 was unambiguously characterized by single crystal X-ray diffraction.     

Reactions of agostic manganese complexes with molecular hydrogen

Reactions between manganese agostic species having (Mn---C---H) interactions and molecular hydrogen have been investigated. Treatment of the bridging agostic cyclooctenylmanganese tricarbonyl, 3, and butenylmanganese tricarbonyl, 5, with hydrogen in benzene results in the formation of the cyclohexadienylmanganese tricarbonyl compound 4. This suggests that the hydrogen molecule is highly reactive toward organometallic manganese complexes containing an agostic C---H bond. In these reactions (η²-H₂) bonded species are plausible intermediates but these are not detected by NMR. The results indicate that the suggested intermediates in the reactions may be useful as hydrogenation catalysts and as precursors to prepare new manganese compounds which may not be accessible by other pathways.     

Mechanistic aspects of dihydrogen activation and transfer during asymmetric hydrogenation in supercritical carbon dioxide

A new "CO2-philic" chiral rhodium diphosphinite complex was synthesized and applied as catalyst precursor in the asymmetric hydrogenation of dimethyl itaconate in scCO2, scC2H6 and various liquid organic solvents. Deuterium labeling studies and parahydrogen-induced polarization (PHIP) NMR experiments were used to provide the first detailed mechanistic insight into the activation and transfer of the dihydrogen molecule during hydrogenation in scCO2. Chemical interactions between CO2 and reactive intermediates of the catalytic pathway could be excluded as possible explanations for the experimentally verified difference in the catalytic behavior in scCO2 and hexane.     

The synthesis and reactivity of electrophilic iridium (III) complexes containing bis (diphenylphosphino) ethane

The complex Ir(CH₃) (CO) (CF₃SO₃)₂ (dppe) (1) has been synthesized from the reaction of Ir(CH₃)I₂(CO) (dppe) and silver triflate. Methane and IrH(CO) (CF₃SO₃)₂ (dppe) (2) are formed when a methylene chloride solution of 1 is placed under 760 torr dihydrogen. Conductivity studies indicate that methylene chloride solutions of complexes 1 and 2 are weak electrolytes and only partially ionized at concentrations above 1 mM. Complex 2 is an effective hydrogenation catalyst for ethylene and 1-hexene while acetone hydrogenation is inhibited by the formation of [IrH₂(HOCH(CH₃)₂) (CO) (dppe)] (OTf) (3). Linear dimerization and polymerization of styrene occurs via a carbocationic mechanism initiated by triflic acid elimination from 2. Treatment of an acetonitrile solution of Ir(CH₃)I₂(CO) (dppe) with silver hexafluorophosphate produces the solvent promoted carbonyl insertion product [Ir(C(O)CH₃) (NCCH₃)₃ (dppe)] [PF₆]₂ (7) which readily undergoes deinsertion in methylene chloride to form [Ir(CH₃) (CO) (NCCH₃)₂ (dppe)] [PF₆]₂ (8) and acetonitrile.     

Relating catalytic activity and electrochemical properties: The case of arene-ruthenium phenanthroline complexes catalytically active in transfer hydrogenation

The electrochemical properties of cationic complexes [(η⁶-arene)Ru(N ∩ N)Cl]Cl (arene/N ∩ N = C₆H₆/1,10-phenanthroline (1), p-MeC₆H₄Prⁱ/1,10-phenanthroline (2), C₆Me₆/1,10-phenanthroline (3), C₆Me₆/5-NO₂-1,10-phenanthroline (4), and C₆Me₆/5-NH₂-1,10-phenanthroline (5)) were studied by cyclic voltammetry in order to rationalize catalytic activity in transfer hydrogenation of the respective aqua complexes [(η⁶-arene)Ru(N ∩ N)(OH₂)](BF₄)₂ (6-10). Complexes 1-5 were chosen because the ‘true’ catalysts 6-10 are unstable under the conditions of the measurement. The electrochemical behaviour of 1-5 in acetonitrile solution is rather complicated due to consecutive and parallel chemical reactions that accompany electron transfer processes. Nonetheless, interpretation of the electrochemical data allowed to assess the influence of the structure and substitution on the redox and catalytic properties: the catalytic ability correlates with the reduction potentials, indicating the decisive role of the η⁶-arene ring directly bonded to the catalytic centre (Ru).     

Synthesis, immobilization and catalytic activity of some silylated cyclopentadienyl rhodium(I) complexes

The mixture of isomers of silylated cyclopentadiene derivative C₅H₅CH₂CH₂Si(OMe)₃ (1) has been used for the syntheses of the mononuclear Rh(I) complexes [η⁵-C₅H₄(CH₂)₂Si(OMe)₃]Rh(CO)₂ (3). [η⁵-C₅H₄(CH₂)₂Si(OMe)₃]Rh(COD) (4) and [η⁵-C₅H₄(CH₂)₂Si(OMe)₃]Rh(CO)(PPh₃) (5). Upon entrapment of 3–5 in silica sol-gel matrices, air stable, leach-proof and recyclable catalysts 6–8 resulted. Their catalytic activities in some hydrogenation processes were compared with those of the non-immobilized complexes 3–5, as well as with those of homogeneous and heterogenized non-silylated analogs, 9–14.     

Activation of dihydrogen without transition metals

The metal-free hydrogenase from methanogenic archaea (Hmd) is a unique enzyme: it catalyzes the reaction of its substrate, methenyl-tetrahydromethanopterin, with molecular hydrogen without the aid of a transition metal. In other words, Hmd is currently the only example of a purely organic hydrogenation catalyst. Recent results from various fields have shed new light on this enzyme. In biochemistry, there is experimental proof that a tightly bound (and metal-free) cofactor exists. Ab initio calculations have revealed that the concerted action of the Lewis-acidic substrate and a Br?nsted-base appears to induce facile heterolysis of the hydrogen molecule. In chemical model studies, a transition-metal-free hydrogenation of ketones was achieved in the presence of catalytic base. Taken together, the experimental results available to date point to an enzymatic mechanism in which the hydrogen molecule is heterolyzed by the joint action of the Lewis-acidic substrate methenyl-tetrahydromethanopterin and a Br?nsted-base in the active site (i.e. by bifunctional catalysis).     

Synthesis of modified tuftsins containing monosaccharides or monosaccharide derivatives

Synthesis of some modified tuftsins is described in which a monosaccharide or a monosaccharide derivative was incorporated in the molecule. Acylation of H-Thr-Lys(Z)-Pro-Arg(NO2)-OBzl with D(+)-gluco-1,5-lactone followed by catalytic hydrogenation gave N alpha-gluconyl-tuftsin. Glycosylation of the carboxyl function of the C-terminal arginine has been achieved by reacting, through the mixed anhydride procedure, Boc-Thr-Lys(Z)-Pro-OH with 2-deoxy-2-(NG-nitroargininamido)-D-glucopyranose followed by catalytic hydrogenation and trifluoroacetic acid treatment. O-Glucosyl-tuftsin has been prepared by reacting o-nitrophenyl N-benzyloxycarbonyl-O-[(alpha + beta) 2,3,4,6-tetra-O-benzyl-D-glucopyranosyl]-threoninate with H-Lys(Z)-Pro-Arg(NO2)-OBzl in the presence of 1-hydroxybenzotriazole. Flash chromatography on silica gel allowed a partial separation of the diastereoisomers, one of which has been isolated in a reasonable yield. The single diastereoisomer and the alpha + beta anomeric mixture were separately deblocked by catalytic hydrogenation and purified by RP-HPLC.     

Cooperative catalysis of a trinuclear ruthenium(II) complex in transfer hydrogenation of ketones by formic acid

A novel TPA derivative (TPA = tris(2-pyridylmethyl)amine) having two 1,10-phenanthroline (phen) moieties via amide linkage was synthesized and this ligand reacted with [Ru(hmb)Cl₂]₂ (hmb: hexamethylbenzene) to give a trinuclear Ru(II) complex, [RuCl(TPA-{phenRuCl(hmb)}₂-H⁺)](PF₆)₂ (1-Cl), in a moderate yield. The complex involves a deprotonated and oxygen-coordinated amide linkage, which exhibits reversible protonation-deprotonation equilibrium. The chlorido complex was converted to be an aqua complex, [Ru(H₂O)(TPA-{phenRu(H₂O)₂(hmb)}₂-H⁺)](SO₄)_5/2 (1-H₂O), by the reaction of 1-Cl with Ag₂SO₄ in H₂O. Transfer hydrogenation of ketones was examined by using 1-Cl as a catalyst and HCOONa as a hydride source in H₂O/CH₃OH (1:1 v/v) at 50 °C under Ar. The time-course of the transfer hydrogenation of cyclohexanone to give cyclohexanol revealed that 1-Cl showed a cooperative effect on the catalytic reactivity as compared with that of mononuclear [RuCl(hmb)(phen)] (3-Cl) and [RuCl((1-Naph)₂-TPA)]PF₆ in H₂O/CH₃OH (1:2 v/v) under the same conditions. The detailed kinetic study has revealed that the catalytic transfer hydrogenation proceeds via the formato complex, which interacts with a substrate rather than via the hydrido complex. The two Ru centers placed at close proximity in 1-H₂O enhanced the interaction of the formato complex with a substrate, resulting in an increase in the catalytic reactivity as compared with the mononuclear complex.     

DNA methylation and development.

(1) Isolated rat liver mitochondria were subjected to catalytic hydrogenation using a water-soluble Pd complex and molecular H2. This treatment resulted in a reduction of double bonds on phospholipid acyl chains as judged by gas chromatography of fatty acid methyl esters and HPLC of dinitrobenzoyldiacylglycerols. (2) After hydrogenation, mitochondria lost their ability to hydrolyze endogenous phospholipids in alkaline, Ca2+ containing medium, while phospholipase A2 retained full activity against exogenous substrates, regardless of whether those substrates were hydrogenated or not. (3) Inhibition by hydrogenation of endogenous phospholipid hydrolysis correlated with the loss of polyunsaturated fatty acyls, rather than with changes of the bulk membrane fluidity as measured by ESR and fluorescence studies. (4) These data suggest that the unsaturation of mitochondrial membrane lipids might be important for regulation of phospholipid breakdown by endogenous phospholipases. In particular, polyunsaturated molecular species seem to be involved in making phospholipids accessible to phospholipase A-mediated hydrolysis.     

Enantioselective hydrogenation of α‐ketoesters catalyzed by cinchona alkaloid stabilized Rh nanoparticles in ionic liquid

The heterogeneous enantioselective hydrogenation of α‐ketoesters catalyzed by rhodium nanoparticles (Rh NPs) in ionic liquid was studied with the stabilization and modification of cinchona alkaloids. TEM characterization showed that well‐dispersed Rh NPs of about 1.96 nm were obtained in ionic liquid. The results showed that cinchona alkaloids not only had good enantiodifferentiating ability but also accelerated the catalytic reaction. Under the optimum reaction conditions, the enantiomeric excess in ethyl benzoylformate hydrogenation could reach as high as 60.9%.     

Tuning of Catalytic Activity by Thermoelectric Materials for Carbon Dioxide Hydrogenation

An innovative use of a thermoelectric material (BiCuSeO) as a support and promoter of catalysis for CO₂ hydrogenation is reported here. It is proposed that the capability of thermoelectric materials to shift the Fermi level and work function of a catalyst lead to an exponential increase of catalytic activity for catalyst particles deposited on its surface. Experimental results show that the CO₂ conversion and CO selectivity are increased significantly by a thermoelectric Seebeck voltage. This suggests that the thermoelectric effect can not only increase the reaction rate but also change chemical equilibrium, which leads to the change of thermodynamic equilibrium for the conversion of CO₂ in its hydrogenation reactions. It is also shown that this thermoelectric promotion of catalysis enables BiCuSeO oxide itself to have a high catalytic activity for CO₂ hydrogenation. The generic nature of the mechanism suggests the possibility that many catalytic chemical reactions can be tuned in situ to achieve much higher reaction rates, or at lower temperatures, or have better desired selectivity through changing the backside temperature of the thermoelectric support.     

Solution and crystal structure of the dihydrogen complex [Ru(H2)(H)(PMe2Ph)4]PF6, an active alkyne hydrogenation catalyst

The complex [Ru(H₂)(H)(PMe₂Ph)₄]PF₆ (1) has been prepared by reaction of [Ru(H)(PMe₂Ph)₅] FP₆ (2) in THF with 1 atm H₂ and characterised by variable temperature ³¹P and ¹H NMR. It undergoes four distinct fluxional processes listed in order of decreasing activation energy: (i) exchange of H₂ in solution with the dihydrogen ligand above 273 K; (ii) isomerisation of cis and trans isomers of 1 above 230 K; (iii) exchange of H atoms between H₂ and hydride in trans-1 above 180 K; (iv) rapid H₂/hydride exchange in cis-1 to below 180 K. A single crystal X-ray diffraction study of 1 at 173 K shows that the complex has the cis geometry in the solid state but does not clearly reveal the positions of the hydrogen ligands. Complex 1 starts out as a catalyst of high activity for the selective hydrogenation of 1-alkynes to 1-alkenes (RC≡CH; R=¹¹Bu, Ph) but it is rapidly deactivated, possibly because of formation of the enynyl complex [Ru(η³RC₃CHR)(PMe₂Ph)₄]⁺. Complex 1 efficiently catalyzes the hydrogenation of internal alkynes (3-hexyne, 2-pentyne) to internal cis-alkenes with little deactivation, although some isomerisation of the alkene produced is observed. These observations are consistent with those of Nkosi, Coville, Albers and Singleton who reported that complex 2 must dissociate one PMe₂Ph ligand to produce the species active for alkyne hydrogenation. Complex 2 catalyses these hydrogenations with slower initial rates than complex 1 but deactivates less readily. In contrast to 1, complex 2 does not appear to cause the isomerisation of internal alkenes.     

Synthetic libraries of tyrosine-derived bacterial metabolites

The preparation of a collection of 131 small molecules, reminiscent of families of long chain N-acyl tyrosines, enamides and enol esters that have been isolated from heterologous expression of environmental DNA (eDNA) in Escherichia coli, is reported. The synthetic libraries of N-acyl tyrosines and their 3-keto counterparts were prepared via solid-phase routes, whereas the enamides and enol esters were synthesized in solution-phase.     

The Binding Site of the V-ATPase Inhibitor Apicularen Is in the Vicinity of Those for Bafilomycin and Archazolid

The investigation of V-ATPases as potential therapeutic drug targets and hence of their specific inhibitors is a promising approach in osteoporosis and cancer treatment because the occurrence of these diseases is interrelated to the function of the V-ATPase. Apicularen belongs to the novel inhibitor family of the benzolactone enamides, which are highly potent but feature the unique characteristic of not inhibiting V-ATPases from fungal sources. In this study we specify, for the first time, the binding site of apicularen within the membrane spanning V(O) complex. By photoaffinity labeling using derivatives of apicularen and of the plecomacrolides bafilomycin and concanamycin, each coupled to (14)C-labeled 4-(3-trifluoromethyldiazirin-3-yl)benzoic acid, we verified that apicularen binds at the interface of the V(O) subunits a and c. The binding site is in the vicinity to those of the plecomacrolides and of the archazolids, a third family of V-ATPase inhibitors. Expression of subunit c homologues from Homo sapiens and Manduca sexta, both species sensitive to benzolactone enamides, in a Saccharomyces cerevisiae strain lacking the corresponding intrinsic gene did not transfer this sensitivity to yeast. Therefore, the binding site of benzolactone enamides cannot be formed exclusively by subunit c. Apparently, subunit a substantially contributes to the binding of the benzolactone enamides.     

Efficiently Enhancing Oxygen Reduction Electrocatalytic Activity of MnO2 Using Facile Hydrogenation

Improving the electrocatalytic oxygen reduction reaction (ORR) activity of transition metal oxides is important for the development of non‐noble metal catalysts that are used in metal‐air batteries and fuel cells. Here, a novel facile strategy of hydrogenation to significantly enhance the ORR performance of MnO₂. The hydrogenated MnO₂ (H‐MnO₂), which is prepared through a simple heat treatment in hydrogen gas, shows characteristics of modified lattice/surface structures and increased electrical conductivity. In 0.1 M KOH aqueous solution, the prepared H‐MnO₂ exhibits high activity toward the oxygen electrocatalysis with more positive onset potential (≈60 mV), ≈14% larger of limiting current, lower yield of peroxide species, and better durability than the pristine oxide. Further conductivity testing and density functional theory (DFT) studies reveal the faster kinetics of ORR after hydrogenation is due to the formation of hydrogen bonds and altered microstructure and improved electronic properties. These results highlight the importance of hydrogenation as a facile yet effective strategy to improve the catalytic activity of transition metal oxides for ORR‐based applications.     

Natural alkaloids and synthetic relatives as chiral templates of the Orito's reaction

The enantioselective hydrogenation of methyl or ethyl pyruvate over cinchona‐platinum catalyst system (Orito's reaction) is one of the most intensively studied heterogeneous catalytic asymmetric hydrogenation reactions. Studies aiming at systematic changes of the chiral template have played a crucial role in creating hypotheses for the mechanism of Orito's reaction. It is very important to clarify which structural unit of the alkaloid takes part in the enantiodifferentiation, and learn about the role of the different structural units of chiral templates. In this article, we made an attempt to describe the behavior of natural alkaloids, their synthetic derivatives, and analogues as chiral templates in the heterogeneous catalytic asymmetric hydrogenation of activated ketones. Chirality, 2010. © 2009 Wiley‐Liss, Inc.