New C2-symmetric bis(sulfonamide)-cyclohexane-1,2-diamine-RhCp complex and its application in the asymmetric transfer hydrogenation (ATH) of ketones in water

C₂-symmetric bis(sulfonamide) ligands derived from trans-(1R,2R)-cyclohexane-1,2-diamine were synthesized and complexed with [Cp^∗RhCl₂]₂ in situ and used in the ATH of aromatic ketones with aqueous sodium formate as the hydrogen source. The chiral secondary alcohols were obtained with 90-99% enantioselectivity and in 50-100% yield. Reductions in water were faster than those in isopropanol/KOH.     

Water-soluble chiral monosulfonamide-cyclohexane-1,2-diamine-RhCp complex and its application in the asymmetric transfer hydrogenation (ATH) of ketones

Monosulfonamide ligands with heteroatom/heterocyclic systems were derived from trans-(1R,2R)-cyclohexane-1,2-diamine and complexed with [Ru(benzene)Cl₂]₂, [Cp^∗RhCl₂]₂ in situ and used in the ATH of aromatic ketones with aqueous sodium formate as the hydrogen source. The chiral secondary alcohols were obtained with >93% enantioselectivity and >89% yield. Reduction in water was faster than in isopropanol/KOH. Addition of surfactants showed little or no effects.     

Synthesis of (R)- and (S)-4-hydroxyisophorone by ruthenium-catalyzed asymmetric transfer hydrogenation of ketoisophorone

The first synthesis of (R)- and (S)-4-hydroxyisophorone by catalytic transfer hydrogenation of ketoisophorone is reported. Ruthenium catalysts containing commercially available chiral amino alcohols afforded 4-hydroxyisophorone in up to 97% selectivity and 97% ee. (R)- or (S)-4-Hydroxyisophorones with >99% ee were isolated by crystallization. The catalyst precursors [RuCl₂((S,R)-ADPE)(η⁶-p-cymene)] ((S,R)-ADPE=(1S,2R)-amino-1,2-diphenylethanol-N) and (R_Ru)-[RuCl((S,R)-ADPE⁻¹)(η⁶-p-cymene)] (ADPE⁻¹=amino-1,2-diphenylethanolato-N,O) were isolated for the first time and the X-ray crystal structure of the latter determined.     

Enantioselective conjugate addition of dialkylzinc to cyclic enones catalyzed by chiral binaphthyldiamine-copper(I) complexes

The enantioselective conjugate addition of dialkylzinc (R₂Zn) to cyclic enones was examined using chiral binaphthyldiamine-copper(I) catalysts. Under the present reaction conditions, chiral C₂-symmetric [RZn(II)]₂-diamine-Cu(I) complexes were formed from chiral binaphthyldiamine, R₂Zn, and copper(I or II) chloride in situ. The reaction of 2-cyclohexenone with Et₂Zn proceeded smoothly in the presence of the corresponding chiral copper(I) complex (5 mol %) and achiral 2,6-diphenylaniline (10 mol %), and the desired Et-adduct was obtained with up to 76% ee in 95% yield.     

Enantioselective diethylzinc addition to aromatic and aliphatic aldehydes using (3R,5R)-dihydroxypiperidine derivatives catalyst

A series of chiral (3R,5R)-dihydroxypiperidine derivatives 3a-f were conveniently prepared from trans-4-hydroxy-l-proline and applied to the catalytic enantioselective addition of diethylzinc to benzaldehyde and heptanal. Among them, 3d was found to show the best asymmetric induction in promoting the addition of Et₂Zn to various aldehydes, providing (R)-secondary alcohols in up to 98% ee.     

Umpolung of Methylenephosphonium Ions in Their Manganese Half‐Sandwich Complexes and Application to the Synthesis of Chiral Phosphorus‐Containing Ligand Scaffolds

Half‐sandwich manganese methylenephosphonium complexes [Cp(CO)₂Mn(η²‐R₂P?C(H)Ph)]BF₄ were obtained in high yield through a straightforward reaction sequence involving a classical Fischer‐type manganese complex and a secondary phosphine as key starting materials. The addition of various nucleophiles (Nu) to these species took place regioselectively at the double‐bonded carbon center of the coordinated methylenephosphonium ligand R₂P⁺?C(H)Ph to produce the corresponding chiral phosphine complexes [Cp(CO)₂Mn(κ¹‐R₂P? C(H)(Ph)Nu)], from which the phosphines were ultimately recovered as free entities upon simple irradiation with visible light. The synthetic potential of this umpolung approach is illustrated herein by the preparation of novel chiral pincer‐type phosphine–NHC–phosphine ligand architectures.     

Synthesis and characterization of palladium(II) complexes with chiral aminophosphine ligands: Catalytic behaviour in asymmetric hydrovinylation. Crystal structure of cis-[PdCl2(PPh((R)-NHCHCH3Ph)2)2]

Optically active ligands of type Ph₂PNHR (R = (R)-CHCH₃Ph, (a); (R)-CHCH₃Cy, (b); (R)-CHCH₃Naph, (c)) and PhP(NHR)₂ (R = (R)-CHCH₃Ph, (d); (R)-CHCH₃Cy, (e)) with a stereogenic carbon atom in the R substituent were synthesized. Reaction with [PdCl₂(COD)₂] produced [PdCl₂P₂] (1) (P = PhP(NHCHCH₃Ph)₂), whose molecular structure determined by X-ray diffraction showed cis disposition for the ligands. All nitrogen atoms of amino groups adopted S configuration. The new ligands reacted with allylic dimeric palladium compound [Pd(η³-2-methylallyl)Cl]₂ to gave neutral aminophosphine complexes [Pd(η³-2-methylallyl)ClP] (2a-2e) or cationic aminophosphine complexes [Pd(η³-2-methylallyl)P₂]BF₄ (3a-3e) in the presence of the stoichiometric amount of AgBF₄. Cationic complexes [Pd(η⁴3-2-methylallyl)(NCCH₃)P]BF₄ (4a-4e) were prepared in solution to be used as precursors in the catalytic hydrovinylation of styrene. ³¹P NMR spectroscopy showed the existence of an equilibrium between the expected cationic mixed complexes 4, the symmetrical cationic complexes [Pd(η³-2-methylallyl)P₂]BF₄ (3) and [Pd(η³-2-methylallyl)(NCCH₃)₂]BF₄ (5) coming from the symmetrization reaction. The extension of the process was studied with the aminophosphines (a-e) as well as with nonchiral monodentate phosphines (PCy₃ (f), PBn₃ (g), PPh₃ (h), PMe₂Ph (i)) showing a good match between the extension of the symmetrization and the size of the phosphine ligand. We studied the influence of such equilibria in the hydrovinylation of styrene because the behaviour of catalytic precursors can be modified substantially when prepared ‘in situ’. While compounds 3 and bisacetonitrile complex 5 were not active as catalysts, the [Pd(η³-2-methylallyl)(η²-styrene)₂]⁺ species formed in the absence of acetonitrile showed some activity in the formation of codimers and dimers. Hydrovinylation reaction between styrene and ethylene was tested using catalytic precursors solutions of [Pd(η³-2-methylallyl)LP]BF₄ ionic species (L = CH₃CN or styrene) showing moderate activity and good selectivity. Better activities but lower selectivities were found when L = styrene. Only in the case of the precursor containing Ph₂PNHCHCH₃Ph (a) ligand was some enantiodiscrimination (10%) found.     

Synthesis,crystal structure and reactivity of a new pentacoordinated chiral dioxomolybdenum(VI) complex

The novel tridentate chiral ligand 2,6-bis{[(1R,2S,4R)-2-hydroxy-1,3,3-trimethyl-bicyclo[2.2.1]hept-2-yl]}pyridine (1) was readily prepared by reaction of 2,6-dilithiopyridine with (R)-(−)-fenchone. Reaction of 1 with [MoO₂(acac)₂] resulted in the formation of the new metal-oxo five-coordinated complex [MoO₂(ONO)] (2) [ONO = (1 – 2H)]. The reactivity of 2 has been studied and the derivatives [MoS₂(ONO)] (3) and [MoO(O₂)(ONO)] (4) were prepared. The compounds 1–4 have been characterised by ¹H and ¹³C{¹H} NMR, microanalysis and IR spectroscopy. Furthermore, the molecular structures of 1 and 2 have been determined by single-crystal X-ray diffraction. The behaviour of 2 as catalyst in oxotransfer and in nucleophilic substitution of propargylic alcohols reactions has been tested.     

Chiral linker. Part 2: Synthesis and evaluation of a novel,reusable solid-supported open chain chiral auxiliary derived from m-hydrobenzoin for the diastereoselective reduction of α-keto esters

Three novel m-hydrobenzoin derived chiral hydrobenzoin mono-alkyl ethers were synthesized and evaluated as open chain chiral auxiliaries in the L-selectride^R/ZnCl₂ mediated stereoselective reduction of their corresponding phenyl glyoxylates, resulting in des of up to 91%. The optimized auxiliary structure was immobilized on commercially available Wang-resin by using the ether substituent as a sublinking unit and applied as a reusable solid-supported chiral auxiliary in the same type of reaction with only little loss of stereofacial selectivity.     

Asymmetric epoxidation of cis-1-propenylphosphonic acid (CPPA) catalyzed by chiral tungsten(VI) and molybdenum(VI) complexes

In the presence of 5.0 mol% chiral tungsten(VI) and molybdenum(VI) complexes, the catalytic asymmetric epoxidation of cis-1-propenylphosphonic acid (CPPA) with 30% aqueous H₂O₂ affording (1R,2S)-(−)-(1, 2)-epoxypropyl phosphonic acid (fosfomycin) was first described. The enantioselectivities of the tungsten and molybdenum catalysts depend strongly on the ligands, reaction temperature and solvent. In CH₂Cl₂ at 0 °C for 72 h, complex MoO₂[(+)-campy]₂ catalyzed the asymmetric epoxidation in a 100% conversion of CPPA with the highest 80% ee. The mechanism of the present epoxidation could be described as direct oxygen transfer occurred on the interface of the biphasic H₂O-nonprotic system.     

Asymmetric Hydrogenations (Nobel Lecture)

The start of the development of catalysts for asymmetric hydrogenation was the concept of replacing the triphenylphosphane ligand of the Wilkinson catalyst with a chiral ligand. With the new catalysts, it should be possible to hydrogenate prochiral olefins. Knowles and his co‐workers were convinced that the phosphorus atom played a central role in this selectivity, as only chiral phosphorus ligands such as (R,R)‐DIPAMP, whose stereogenic center lies directly on the phosphorus atom, lead to high enantiomeric excesses when used as catalysts in asymmetric hydrogenation reactions. This hypothesis was disproven by the development of ligands with chiral carbon backbones. Although the exact mechanism of action of the phosphane ligands is not incontrovertibly determined to this day, they provide a simple entry to a large number of chiral compounds.     

Highly enantioselective synthesis of terutroban key intermediate via asymmetric hydrogenation

A chiral (R) key intermediate of the biologically active form of terutroban has been prepared by asymmetric hydrogenation. The catalysts are based on very easily accessible ruthenium complexes modified by chiral phosphorous ligands. The use of the chiral catASium^®T ligands family allowed us to realize this transformation efficiently in terms of yield and enantioselectivity (ee up to 92%) with high substrate/catalyst ratios.     

Chiral and Nonchiral [OsX2(diphosphane)(diamine)] (X: Cl,OCH2CF3) Complexes for Fast Hydrogenation of Carbonyl Compounds

The osmium complexes trans‐[OsCl₂(dppf)(diamine)] (dppf: 1,1′‐bis(diphenylphosphino)ferrocene; diamine: ethylenediamine in 3 , propylenediamine in 4 ) were prepared by the reaction of [OsCl₂(PPh₃)₃] ( 1 ) with the ferrocenyl diphosphane, dppf and the corresponding diamine in dichloromethane. The reaction of derivative 3 with NaOCH₂CF₃ in toluene afforded the alkoxide cis‐[Os(OCH₂CF₃)₂(dppf)(ethylenediamine)] ( 5 ). The novel precursor [Os₂Cl₄(P(m‐tolyl)₃)₅] ( 2 ) allows the synthesis of the chiral complexes trans‐[OsCl₂(diphosphane)(1,2‐diamine)] ( 6 – 9 ; diphosphane: (R)‐[6,6′‐dimethoxy(1,1′‐biphenyl)‐2,2′‐diyl]bis[1,1‐bis(3,5‐dimethylphenyl)phosphane] (xylMeObiphep) or (R)‐(1,1′‐binaphthalene)‐2,2′‐diylbis[1,1‐bis(3,5‐dimethylphenyl)phosphane] (xylbinap); diamine=(R,R)‐1,2‐diphenylethylenediamine (dpen) or (R,R)‐1,2‐diaminocyclohexane (dach)), obtained by the treatment of 2 with the diphosphane and the 1,2‐diamine in toluene at reflux temperature. Compounds 3 – 5 in ethanol and in the presence of NaOEt catalyze the reduction of methyl aryl, dialkyl, and diaryl ketones and aldehydes with H₂ at low pressure (5 atm), with substrate/catalyst (S/C) ratios of 10 000–200 000 and achieving turnover frequencies (TOFs) of up to 3.0×10⁵ h^?1 at 70 °C. By employment of the chiral compounds 6 – 9 , different ketones, including alkyl aryl, bulky tert‐butyl, and cyclic ketones, have successfully been hydrogenated with enantioselectivities up to 99 % and with S/C ratios of 5000–100 000 and TOFs of up to 4.1×10⁴ h^?1 at 60 °C.     

Optically active rhodium complexes with indenyl-linked phosphane ligands

The optically active indenyl-linked phosphane ligands (S)-[2-(3H-inden-1-yl)-1-phenylethyl]diphenylphosphane (L₁) and (S)-[2-(4,7-dimethyl-3H-inden-1-yl)-1-phenyl-ethyl]diphenylphosphane (L₂) were synthesized in three steps from (R)-1-phenylethane-1,2-diol in excellent yields. Their lithium salts reacted with [Rh(μ-Cl)(η²-CH₂CH₂)₂]₂ at −78 °C in THF affording the planar chiral complexes (S,R_pl + S_pl)-[Rh(η⁵-indenyl-CH₂CH(Ph)PPh₂-kP)(η²-CH₂CH₂)] and (S,R_pl + S_pl)-[Rh(η⁵-4,7-dimethylindenyl-CH₂CH(Ph)PPh₂-kP)(η²-CH₂CH₂)] as 61:39 and 15:85 mixtures of diastereomers. The complexes were isolated in optically pure form by column chromatography. The stereochemical configuration of one of the diastereomers was determined by X-ray crystallography. The complexation of L₂ was studied in different solvents and with several Rh precursors and diastereomeric excesses up to 76% were achieved. The ability of the chiral ligands to control the stereochemistry at the metal center was tested by oxidative addition of methyl iodide. Diastereomeric excesses greater than 98% were observed.     

New C2-symmetric chiral phosphinite ligands based on amino alcohol scaffolds and their use in the ruthenium-catalysed asymmetric transfer hydrogenation of aromatic ketones

Asymmetric transfer hydrogenation processes of ketones with chiral molecular catalysts are attracting increasing interest from synthetic chemists due to their operational simplicity. C₂-symmetric catalysts have also received much attention and been used in many reactions. A series of new chiral C₂-symmetric bis(phosphinite) ligands has been prepared from corresponding amino acid derivated amino alcohols or (R)-2-amino-1-butanol through a three- or four-step procedure. Their structures have been elucidated by a combination of multinuclear NMR spectroscopy, IR spectroscopy and elemental analysis. ¹H-³¹P NMR, DEPT, ¹H-¹³C HETCOR or ¹H-¹H COSY correlation experiments were used to confirm the spectral assignments. In situ prepared ruthenium catalytic systems were successfully applied to ruthenium-catalyzed asymmetric transfer hydrogenation of acetophenone derivatives by iso-PrOH. Under optimized conditions, these chiral ruthenium catalyst systems serve as catalyst precursors for the asymmetric transfer hydrogenation of acetophenone derivatives in iso-PrOH and act as good catalysts, giving the corresponding optical secondary alcohols in 99% yield and up to 79% ee.     

8-Amino-5,6,7,8-tetrahydroquinolines as ligands in iridium(III) catalysts for the reduction of aryl ketones by asymmetric transfer hydrogenation (ATH)

Aqua iridium(III) complexes with 8-amino-5,6,7,8-tetrahydroquinolines CAMPY L1 and its derivatives as chiral ligands proved to be very efficient catalysts for the reduction of a wide range of prochiral aryl ketones, revealing a variety of behaviours in terms of reaction rate and stereoselectivity. As standard substrates, differently substituted acetophenones were studied and good enantioselectivity (86% ee) was achieved in the reduction of 1-(o-tolyl)ethan-1-one 6. Particularly interesting was the ATH reaction in the case of β-amino keto esters, precursors of β-lactams and azetidinones. The best results were obtained with [Cp¹Ir(H₂O)(L1)]SO₄ affording the corresponding diastereomeric alcohols in an (R,S)-configuration with an excellent 99% ee in the reduction of 2-(benzamido methyl)-3-oxo-3-(4-(trifluoromethyl)phenyl)propanoate 12.     

Two chiral mononuclear and one-dimensional cadmium(II) complexes constructed by (1R,2R)-N1,N2-bis(pyridinylmethyl)cyclohexane-1,2-diamine derivatives: Effect of positional isomerism

Reactions of (1R,2R)-N¹,N²-bis(pyridinylmethyl)cyclohexane-1,2-diamine derivatives, (1R,2R)-2-bpcd and (1R,2R)-3-bpcd [(1R,2R)-2-bpcd = (1R,2R)-N¹,N²-bis(pyridin-2-ylmethyl)cyclohexane-1,2-diamine, (1R,2R)-3-bpcd = (1R,2R)-N¹,N²-bis(pyridin-3-ylmethyl)cyclohexane-1,2-diamine], with CdI₂ in an analogous way led to the formation of a chiral discrete mononuclear complex and a chiral one-dimensional polymeric chain, respectively, which may be attributed to the positional isomerism of the ligands. The chiral organic ligands and complexes display luminescent properties indicating that they may have a potential application as optical materials. Powder second-harmonic generation (SHG) efficiency measurement shows that the SHG efficiency of the complexes is approximately 0.3 and 0.45 times that of KDP, respectively.     

Asymmetric Hydrolytic Kinetic Resolution with Recyclable Macrocyclic CoIII–Salen Complexes: A Practical Strategy in the Preparation of (R)‐Mexiletine and (S)‐Propranolol

A chiral cobalt(III) complex ( 1 e ) was synthesized by the interaction of cobalt(II) acetate and ferrocenium hexafluorophosphate with a chiral dinuclear macrocyclic salen ligand that was derived from 1R,2R‐(?)‐1,2‐diaminocyclohexane with trigol bis‐aldehyde. A variety of epoxides and glycidyl ethers were suitable substrates for the reaction with water in the presence of chiral macrocyclic salen complex 1 e at room temperature to afford chiral epoxides and diols by hydrolytic kinetic resolution (HKR). Excellent yields (47 % with respect to the epoxides, 53 % with respect to the diols) and high enantioselectivity (ee>99 % for the epoxides, up to 96 % for the diols) were achieved in 2.5–16 h. The Co^III macrocyclic salen complex ( 1 e ) maintained its performance on a multigram scale and was expediently recycled a number of times. We further extended our study of chiral epoxides that were synthesized by using HKR to the synthesis of chiral drug molecules (R)‐mexiletine and (S)‐propranolol.     

Screening of ligands in the asymmetric metallocenethiolatocopper(I)-catalyzed allylic substitution with Grignard reagents

Screening of metallocenethiolate ligands for copper(I)-catalyzed substitution of allylic acetates with Grignard reagents has been carried out. The previously used ligand, lithium (R,S_p)-2-(1-dimethylaminoethyl)ferrocenylthiolate (4a), possessing both central and planar chirality, was the starting point for the screening. It was found that the diastereomeric ligand lithium (R,R_p)-2-(1-dimethylaminoethyl)ferrocenylthiolate (4b) exhibiting reversed planar chirality gave increased enantioselectivity in the allylic substitution, at least when cinnamyl acetate was used as a substrate. The ruthenocene-based ligand lithium (R,S_p)-2-(1-dimethylaminoethyl)ruthenocenylthiolate (4c) gave an enhanced reaction rate, but lower chiral induction. The use of disulfide bis[(R,S_p)-2-(1-dimethylaminoethyl)ferrocenyl]disulfide (7a) as a ligand precursor worked well but resulted in lower enantioselectivity.     

Novel chiral C2-symmetric multidentate aminophosphine ligands for use in catalytic asymmetric reduction of ketones

A series of novel chiral C₂-symmetric multidentate aminophosphine ligands have been successfully synthesized by Schiff-base condensation of bis（o-formylphenyl）phenylphosphane and easily available monoprotected（1R,2R）-diaminocyclohexane.The catalytic properties of these ligands were investigated in Ir-catalyzed asymmetric transfer hydrogenation of various aromatic ketones,giving the corresponding optical active alcohols with up to 98%conversion and good ee under mild reaction conditions.