Applications of transition metal complexes containing aminophosphine ligand to transfer hydrogenation of ketones

Hydrogen transfer reduction processes are attracting increasing interest from synthetic chemists in view of their operational simplicity. Reaction of [Ph₂PNHCH₂‐C₄H₃S] with [Ru(η⁶‐benzene)(µ‐Cl)Cl]₂, [Rh(µ‐Cl)(cod)]₂ and [Ir(η⁵‐C₅Me₅)(µ‐Cl)Cl]₂ gave a range of new monodendate complexes [Ru(Ph₂PNHCH₂‐C₄H₃S)(η⁶‐benzene)Cl₂], 1, [Rh(Ph₂PNHCH₂‐C₄H₃S)(cod)Cl], 2, and [Ir(Ph₂PNHCH₂‐C₄H₃S)(η⁵‐C₅Me₅)Cl₂], 3, respectively. All new complexes were fully characterized by analytical and spectroscopic methods. ¹H? ³¹P NMR, ¹H? ¹³C HETCOR or ¹H? ¹H COSY correlation experiments were used to confirm the spectral assignments. 1–3 are suitable catalyst precursors for the transfer hydrogenation of acetophenone derivatives. Notably [Ru(Ph₂PNHCH₂‐C₄H₃S)(η⁶‐benzene)Cl₂], 1, acts as an excellent catalyst, giving the corresponding alcohols in 98–99% yields in 30 min at 82 °C (TOF ≤200 h^?1) for the transfer hydrogenation reaction in comparison to analogous rhodium or iridium complexes. This transfer hydrogenation is characterized by low reversibility under these conditions. Copyright © 2011 John Wiley & Sons, Ltd.     

The application of tunable tridendate P‐based ligands for the Ru(II)‐catalysed transfer hydrogenation of various ketones

Two novel versatile tridendate aminophosphine–phosphinite and phosphinite ligands were prepared and their trinuclear neutral ruthenium(II) dichloro complexes were found to be effective catalysts for the transfer hydrogenation of various ketones in excellent conversions up to 99% in the presence of 2‐propanol/NaOH in 0.1 M isopropanol solution. Particularly, [Ru₃(PPh₂OC₂H₄)₂ N–PPh₂(η⁶‐p‐cymene)₃Cl₆] acts as an excellent catalyst giving the corresponding alcohols in excellent conversion up to 99% (turnover frequency ≤ 1176 h^?1). A comparison of the catalytic properties of the complexes is also discussed briefly. Furthermore, the structures of these ligands and their corresponding complexes have also been clarified using a combination of multinuclear NMR spectroscopy, infrared spectroscopy and elemental analysis. ¹H–¹³C HETCOR or ¹H–¹H COSY correlation experiments were used to confirm the spectral assignments. Copyright © 2014 John Wiley & Sons, Ltd.     

New iminophosphine–Ru(II) complexes and their application in hydrogenation and transfer hydrogenation

Ruthenium complexes [RuCl₂L₂] were prepared by treating [RuCl₂(p‐cymene)]₂ with structurally similar N‐(2‐(diphenylphosphino)benzylidene)‐3‐methylpyridin‐2‐amine, 4‐(2‐(diphenylphosphino)benzylideneamino)‐3‐methylphenol and 4‐(2‐(2‐(diphenylphosphino)benzylideneamino)ethyl)phenol refluxed in toluene. These complexes were used as catalysts for the transfer hydrogenation of acetophenones in 2‐propanol and for the direct hydrogenation of styrenes under hydrogen pressure. The results of the catalytic studies provide evidence that these complexes function as excellent catalysts for hydrogenation and transfer hydrogenation. Copyright © 2014 John Wiley & Sons, Ltd.     

Synthesis of 2‐aminomethylpiperidine ruthenium(II) phosphine complexes and their applications in transfer hydrogenation of aryl ketones

The complex trans,cis‐[RuCl₂(PPh₃)₂(ampi)] (2) was prepared by reaction of RuCl₂(PPh₃)₃ with 2‐aminomethylpiperidine(ampi) (1). [RuCl₂(PPh₂(CH₂)_nPPh₂)(ampi) (n = 3, 4, 5)] (3–5) were synthesized by displacement of two PPh₃ with chelating phosphine ligands. All complexes (2–5) were characterized by ¹ H, ¹³C, ³¹P NMR, IR and UV‐visible spectroscopy and elemental analysis. They were found to be efficient catalysts for transfer hydrogen reactions. Copyright © 2012 John Wiley & Sons, Ltd.     

Enantioselective transfer hydrogenation of pro-chiral ketones catalyzed by novel ruthenium and iridium complexes of well-designed phosphinite ligand

Abstract

The interaction of [Ru(η⁶-arene)(μ-Cl)Cl]₂ and Ir(η⁵-C₅Me₅)(μ-Cl)Cl]₂ with a new Ionic Liquid-based phosphinite ligand, [(Ph₂PO)-C₆H₉N₂Ph]Cl, (2) gave [Ru((Ph₂PO)-C₆H₉N₂Ph)(η⁶-p-cymene)Cl₂]Cl (3), [Ru((Ph₂PO)-C₆H₉N₂Ph)(benzene)Cl₂]Cl (4) and [Ir((Ph₂PO)-C₆H₉N₂Ph)(C₅Me₅)Cl₂]Cl (5), complexes. All the compounds were characterized by a combination of multinuclear NMR and IR spectroscopy as well as elemental analysis. Furthermore, the Ru(II) and Ir(III) catalysts were applied to asymmetric transfer hydrogenation of acetophenone derivatives using 2-propanol as a hydrogen source. The results showed that the corresponding alcohols could be obtained with good activity (up to 55% ee and 99% conversion) under mild conditions. Notably, [Ir((Ph₂PO)-C₆H₉N₂Ph)(C₅Me₅)Cl₂]Cl (5) is more active than the other analogous complexes in the transfer hydrogenation (up to 81% ee).     

Ruthenium(II) complexes bearing pyridine‐based tridentate and bidentate ligands: catalytic activity for transfer hydrogenation of aryl ketones

Ru(II) complexes of the general formula [RuCl₂(′′)(L)] (1: ′N = N_b, L = MeOH; 2: ′N = N_b, L = CH₃CN; 3: ′N = N_d, L = CH₃CN; 4: ′N = N_p, L = CH₃CN), [Ru(p‐cymene)(_a–b)Cl]Cl (5a: N N_a = 2,2′‐bipyridine; 5b: N N_b = 4,4′‐dimethyl–2,2′‐bipyridine), [Ru(′′)(_a–b)Cl]Cl (6a: ′N = N_b, _a = 2,2′‐bipyridine; 6b: ′N = N_b, _b = 4,4′‐dimethyl‐2,2′‐bipyridine; 7a: ′N = N_d, _a = 2,2′‐bipyridine; 7b: ′N = N_d, _b = 4,4′‐dimethyl‐2,2′‐bipyridine; 8a: ′N = N_p, _a = 2,2′‐bipyridine; 8b: ′N = N_p, _b = 4,4′‐dimethyl‐2,2′‐bipyridine) and [Ru(′′)(_a)Cl]BF₄ (9a: ′N = N_b; _a = 2,2′‐bipyridine) were synthesized from the corresponding [RuCl₂(p‐cymene)]₂ dimer, ′′ and _a–b ligands. The compounds were characterized by elemental analysis, IR and NMR. Complex 9a was studied by X‐ray diffraction, confirming its cationic‐mononuclear [RuCl(_bb)(_a)]⁺ nature. The synthesized Ru(II) complexes (1–8) were employed as catalysts for the transfer hydrogenation of ketones to secondary alcohols in the presence of KOH using 2‐propanol as a hydrogen source at 82°C. The rates of the transfer hydrogenation reactions strongly depended on the type of and ancillary ligands. Copyright © 2012 John Wiley & Sons, Ltd.     

Half‐sandwich Ru (II) complexes containing (N,O) Schiff base ligands: Catalysts for base‐free transfer hydrogenation of ketones

Two new half‐sandwich Ru (II)(p‐cymene) complexes ( 1 and 2 ) containing dopamine‐based (N, O) Schiff base ligands ( L ¹ H and L ² H ) were synthesized and characterized by FT‐IR, UV–Visible and ¹H & ¹³C NMR spectral techniques, and elemental analyses. The spectroscopic and analytical data revealed monobasic bidentate coordination of the ligands with Ru ion. The molecular structures of L ¹ H , L ² H and 2 were further confirmed by single crystal X‐ray diffraction study. Complexes 1 and 2  have been employed as catalysts in the transfer hydrogenation of ketones using 2‐propanol as a hydrogen source at 85 °C under base‐free condition. Good to the excellent yield of secondary alcohols, gram scale synthesis, and high TON and TOF made this catalytic system interesting.     

Ferrocene based chiral binuclear η6‐benzene‐Ru(II)‐phosphinite complexes: Synthesis,characterization and catalytic activity in asymmetric reduction of ketones

In the present study, a series of chiral C₂‐symmetric ferrocenyl based binuclear η⁶‐benzene‐Ru(II) complexes bearing diphenylphosphinite and diisopropylphosphinite moieties have been synthesised. The new binuclear η⁶‐benzene‐Ru(II)‐phosphinite complexes were characterised based on nuclear magnetic resonance (¹H, ¹³C, ³¹P–NMR), FT‐IR spectroscopy and elemental analysis. Then, these complexes have been screened as catalytic precursors in the transfer hydrogenation of acetophenone with 2‐propanol as both the hydrogen source and solvent in the presence of KOH. The corresponding optically active secondary alcohols were obtained in excellent conversion rates between 96 and 99% and moderate to good enantioselectivities (up to 78% ee). The complex 5 was the most efficient catalyst among the four new complexes investigated herein.     

A modular design of metal catalysts for the transfer hydrogenation of aromatic ketones

The ability of transition metal catalysts to add or remove hydrogen from organic substrates by transfer hydrogenation is a valuable synthetic tool. Towards a series of novel metal complexes with a P―NH ligand, [Ph₂PNHCH₂―C₄H₃O] derived from furfurylamine were synthesized. Reaction of [Ph₂PNHCH₂―C₄H₃O] 1 with [Ru(η⁶‐p‐cymene)(μ‐Cl)Cl]₂, [Ru(η⁶‐benzene)(μ‐Cl)Cl]₂, [Rh(μ‐Cl)(cod)]₂ and [Ir(η⁵‐C₅Me₅)(μ‐Cl)Cl]₂ gave a range of new monodentate complexes [Ru(Ph₂PNHCH₂―C₄H₃O)(η⁶‐p‐cymene)Cl₂] 2 , [Ru(Ph₂PNHCH₂―C₄H₃O)(η⁶‐benzene)Cl₂] 3 , [Rh(Ph₂PNHCH₂‐C₄H₃O)(cod)Cl] 4 , and [Ir(Ph₂PNHCH₂‐C₄H₃0)(η⁵‐C₅Me₅)Cl₂] 5 , respectively. All new complexes were fully characterized by analytical and spectroscopic methods. ³¹P‐{¹H} NMR, distortionless enhancement by polarization transfer (DEPT) or ¹H‐¹³C heteronuclear correlation (HETCOR) experiments were used to confirm the spectral assignments. Following activation by KOH, compounds 1 , 2 , 3 , 4 catalyzed the transfer hydrogenation of acetophenone derivatives to 1‐phenylethanol derivatives in the presence of iso‐PrOH as the hydrogen source. Notably [Ru(Ph₂PNHCH₂‐C₄H₃O)(η⁶‐benzene)Cl₂] 3 acts as an excellent catalyst, giving the corresponding alcohols in 98–99% yield in 20 min at 82°C (time of flight ≤ 297 h^?1) for the transfer hydrogenation reaction in comparison to analogous rhodium or iridium complexes. Copyright © 2012 John Wiley & Sons, Ltd.     

Novel half‐sandwich η5‐Cp *–rhodium(III) and η5‐Cp *–ruthenium(II) complexes bearing bis(phosphino)amine ligands and their use in the transfer hydrogenation of aromatic ketones

Two new half‐sandwich η⁵‐Cp*–rhodium(III) and η⁵‐Cp*–ruthenium(II) complexes have been prepared from corresponding bis(phosphino)amine ligands, thiophene‐2‐(N,N‐bis(diphenylphosphino)methylamine) or furfuryl‐2‐(N,N‐bis(diphenylphosphino)amine). Structures of the new complexes have been elucidated by multinuclear one‐ and two‐dimensional NMR spectroscopy, elemental analysis and IR spectroscopy. These Cp*–rhodium(III) and Cp*‐ruthenium(II) complexes bearing bis(phosphino)amine ligands were successfully applied to transfer hydrogenation of various ketones by 2‐propanol. Copyright © 2013 John Wiley & Sons, Ltd.     

Transfer hydrogenation of ketones catalysed by half‐sandwich (η6‐p‐cymene) ruthenium(II) complexes incorporating benzoylhydrazone ligands

Neutral half‐sandwich η⁶‐p ‐cymene ruthenium(II) complexes of general formula [Ru(η⁶‐p ‐cymene)Cl(L)] (HL = monobasic O, N bidendate benzoylhydrazone ligand) have been synthesized from the reaction of [Ru(η⁶‐p ‐cymene)(μ‐Cl)Cl]₂ with acetophenone benzoylhydrazone ligands. All the complexes have been characterized using analytical and spectroscopic (Fourier transform infrared, UV–visible, ¹H NMR, ¹³C NMR) techniques. The molecular structures of three of the complexes have been determined using single‐crystal X‐ray diffraction, indicating a pseudo‐octahedral geometry around the ruthenium(II) ion. All the ruthenium(II) arene complexes were explored as catalysts for transfer hydrogenation of a wide range of aromatic, cyclic and aliphatic ketones with 2‐propanol using 0.1 mol% catalyst loading, and conversions of up to 100% were obtained. Further, the influence of other variables on the transfer hydrogenation reaction, such as base, temperature, catalyst loading and substrate scope, was also investigated.     

钌(II)-吡啶基NNN配合物催化酮的室温(不对称)氢转移反应

合成了一种基于吡啶骨架含有苯并咪唑和手性咪唑啉基团的三齿NNN配体及其二价钌(II)配合物,通过核磁共振波谱学和X射线单晶晶体结构测定确认了钌(II)配合物的分子结构.这些配合物在室温下催化酮的氢转移反应,表现出了优异的催化活性,收率和ee值最高分别可达99%和97%.     

Water soluble Ru (II)–p‐cymene complexes of chiral aroylthiourea ligands derived from unprotected D/L‐alanine as proficient catalysts for asymmetric transfer hydrogenation of ketones

The newfangled chiral aroylthiourea ligands (L1‐L6) were produced from unprotected D/L‐alanine and their water soluble Ru (II) organometallic catalysts ( 1 – 6 ) were designed from their reaction with [RuCl₂(η⁶‐p‐cymene)]₂. The analytical and spectral methods were used to confirm the structure of the ligands and complexes. The solid state structure of L1, 5 and 6 was confirmed by single crystal XRD. The organometallic compounds ( 1 – 6 ) catalyzed the asymmetric transfer hydrogenation of aromatic, heteroaromatic and bulky ketones to yield respective enantiopure secondary alcohols with admirable conversions (up to 99%) and attractive enantiomeric excesses (ee up to 98%), in presence of formic acid and triethylamine in water medium under non‐inert atmospheric conditions.     

Thermoregulated phase‐transfer catalysis via PEG‐armed Ru(II)‐bearing microgel core star polymers: Efficient and reusable Ru(II) catalysts for aqueous transfer hydrogenation of ketones

Thermoregulated phase‐transfer catalysis for the transfer hydrogenation of 2‐octanone in 2‐propanol/H₂O biphasic media was achieved with ruthenium‐bearing microgel‐core star polymers with amphiphilic, thermosensitive poly(ethylene glycol) (PEG) arms [Ru(II)‐PEG star], which were directly prepared by the ruthenium‐catalyzed living radical polymerization in conjunction with a phosphine ligand‐carrying styrene derivative. The star polymers were first placed in the aqueous (lower) layer at room temperature and immediately moved into the organic (upper) layer at 100 °C, and once again, moved down to the aqueous layer (lower) upon cooling the solution to room temperature. The Ru(II)‐PEG star catalyst was clearly superior to the original Ru(II) catalyst and related non‐microgel catalysts [Ru(II)‐PEG block] in terms of activity and recovery/recycle, due to the unique designer structure of the microgel‐core star polymers. Other substrates (less hydrophobic alkyl ketones and aromatic ketone) were also efficiently hydrogenated into the corresponding sec‐alcohols with the star catalyst in aqueous media. © 2009 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 48: 373–379, 2010     

Ruthenium(III) complexes of amine-bis(phenolate) ligands as catalysts for transfer hydrogenation of ketones

Twelve ruthenium(III) complexes bearing amine-bis(phenolate) tripodal ligands of general formula [Ru(L¹–L³)(X)(EPh₃)₂] (where L¹–L³ are dianionic tridentate chelator) have been synthesized by the reaction of ruthenium(III) precursors [RuX₃(EPh₃)₃] (where E = P, X = Cl; E = As, X = Cl or Br) and [RuBr₃(PPh₃)₂(CH₃OH)] with the tripodal tridentate ligands H₂L¹, H₂L² and H₂L³ in benzene in 1:1 molar ratio. The newly synthesized complexes have been characterized by analytical (elemental and magnetic susceptibility) and spectral methods. The complexes are one electron paramagnetic (low-spin, d⁵) in nature. The EPR spectra of the powdered samples at RT and the liquid samples at LNT shows the presence of three different ‘g’ values (g_x ≠ g_y ≠ g_z) indicate a rhombic distortion around the ruthenium ion. The redox potentials indicate that all the complexes undergo one electron transfer process. The catalytic activity of one of the complexes [Ru(pcr-chx)Br(AsPh₃)₂] was examined in the transfer hydrogenation of ketones and was found to be efficient with conversion up to 99% in the presence of isopropanol/KOH.     

Synthesis,characterization and catalytic,cytotoxic and antimicrobial activities of two novel cyclotriphosphazene‐based multisite ligands and their Ru(II) complexes

Two novel cyclotriphosphazene ligands ( 2 and 3 ) bearing 3‐oxypyridine groups and their corresponding Ru(II) complexes ( 4 and 5 ) were synthesized and their structures were characterized using Fourier transform infrared, ¹H NMR and ³¹P NMR spectroscopic data and elemental analysis. The Ru(II) complexes were used as catalysts for catalytic transfer hydrogenation of p‐substituted acetophenone derivatives in the presence of KOH. Additionally, the cytotoxic activities of compounds 2 , 3 , 4 , 5 were evaluated against PC3 (human prostate cancer), DLD‐1 (human colorectal cancer), HeLa (human cervical cancer) and PNT1A (normal human prostate) cell lines. Finally the antimicrobial activities of compounds 2 , 3 , 4 , 5 were evaluated against a panel of Gram‐positive and Gram‐negative bacteria and yeast cultures. The complexes showed efficient catalytic activity towards transfer hydrogenation of acetophenone derivatives, especially those bearing electron‐withdrawing substituents on the para‐position of the aryl ring. The compounds were found to have moderate to high cytotoxic and antimicrobial activities, and Ru(II) complexation enhanced both cytotoxic and antimicrobial activities in comparison with the parent compounds. Copyright © 2015 John Wiley & Sons, Ltd.     

Hydrogenation versus transfer hydrogenation of ketones: two established ruthenium systems catalyze both

The established standard ketone hydrogenation (abbreviated HY herein) precatalyst [Ru(Cl)(2)((S)-tolbinap)[(S,S)-dpen]] ((S),(S,S)-1) has turned out also to be a precatalyst for ketone transfer hydrogenation (abbreviated TRHY herein) as tested on the substrate acetophenone (3) in iPrOH under standard conditions (45 degrees C, 45 bar H(2) or Ar at atmospheric pressure). HY works at a substrate catalyst ratio (s:c) of up to 10(6) and TRHY at s:c<10(4). Both produce (R)-1-phenylethan-1-ol ((R)-4), but the ee in HY are much higher (78-83 %) than in TRHY (4-62 %). In both modes, iPrOK is needed to generate the active catalysts, and the more there is (1-4500 equiv), the faster the catalytic reactions. The ee is about constant in HY and diminishes in TRHY as more iPrOK is added. The ketone TRHY precatalyst [Ru(Cl)(2)((S,S)-cyP(2)(NH)(2))] ((S,S)-2), established at s:c=200, has also turned out to be a ketone HY precatalyst at up to s:c=10(6), again as tested on 3 in iPrOH under standard conditions. The enantioselectivity is opposite in the two modes and only high in TRHY: with (S,S)-2, one obtains (R)-4 in up to 98 % ee in TRHY as reported and (S)-4 in 20-25 % ee in HY. iPrOK is again required to generate the active catalysts in both modes, and again, the more there is, the faster the catalytic reactions. The ee in TRHY are only high when 0.5-1 equivalents iPrOK are used and diminish when more is added, while the (low) ee is again about constant in HY as more iPrOK is added (0-4500 equiv). The new [Ru(H)(Cl)((S,S)-cyP(2)(NH)(2))] isomers (S,S)-9 A and (S,S)-9 B (mixture, exact structures unknown) are also precatalysts for the TRHY and HY of 3 under the same conditions, and (R)-4 is again produced in TRHY and (S)-4 in HY, but the lower ee shows that in TRHY (S,S)-9 A/(S,S)-9 B do not lead to the same catalysts as (S,S)-2. In contrast, the ee are in accord with (S,S)-9 A/(S,S)-9 B leading to the same catalysts as (S,S)-2 in HY. The kinetic rate law for the HY of 3 in iPrOH and in benzene using (S,S)-9 A/(S,S)-9 B/iPrOK or (S,S)-9 A/(S,S)-9 B/tBuOK is consistent with a fast, reversible addition of 3 to a five-coordinate amidohydride (S,S)-11 to give an (S,S)-11-substrate complex, in competition with the rate-determining addition of H(2) to (S,S)-11 to give a dihydride [Ru(H)(2)((S,S)-cyP(2)(NH)(2))] (S,S)-10, which in turn reacts rapidly with 3 to generate (S)-4 and (S,S)-11. The established achiral ketone TRHY precatalyst [Ru(Cl)(2)(ethP(2)(NH)(2))] (12) has turned out to be also a powerful precatalyst for the HY of 3 in iPrOH at s:c=10(6) and of some other substrates. Response to the presence of iPrOK is as before, except that 12 already functions well without it at up to s:c=10(6).     

Ruthenium(II) complexes derived from 2‐phenylthiazoline‐4‐carboxylic acid: structure and catalytic activity for transfer hydrogenation reaction

Piano‐stool ([(p‐cymene)Ru(thz)Cl], 2 ) and six‐coordinated ([Ru(thz)₂(PPh₃)₂], 3 ) ruthenium complexes derived from 2‐phenylthiazoline‐4‐carboxylic acid (Hthz, 1 ) were synthesized for the first time, and fully characterized using conventional methods. Also, the molecular structure of complex 3 was determined using X‐ray analysis. These complexes were evaluated as catalysts for transfer hydrogenation of carbonyl compounds in the presence of isopropyl alcohol and KO^tBu. Complex 2 was found to be more active than 3 in transfer hydrogenation. Copyright © 2016 John Wiley & Sons, Ltd.