Cooperative B–H bond activation: dual site borane activation by redox active κ2-N,S-chelated complexes

Cooperative dual site activation of boranes by redox-active 1,3-N,S-chelated ruthenium species, mer-[PR₃{κ²-N,S-(L)}₂Ru{κ¹-S-(L)}], (mer-2a: R = Cy, mer-2b: R = Ph; L = NC₇H₄S₂), generated from the aerial oxidation of borate complexes, [PR₃{κ²-N,S-(L)}Ru{κ³-H,S,S′-BH₂(L)₂}] (trans–mer-1a: R = Cy, trans–mer-1b: R = Ph; L = NC₇H₄S₂), has been investigated. Utilizing the rich electronic behaviour of these 1,3-N,S-chelated ruthenium species, we have established that a combination of redox-active ligands and metal–ligand cooperativity has a big influence on the multisite borane activation. For example, treatment of mer-2a–b with BH₃·THF led to the isolation of fac-[PR₃Ru{κ³-H,S,S′-(NH₂BSBH₂N)(S₂C₇H₄)₂}] (fac-3a: R = Cy and fac-3b: R = Ph) that captured boranes at both sites of the κ²-N,S-chelated ruthenacycles. The core structure of fac-3a and fac-3b consists of two five-membered ruthenacycles [RuBNCS] which are fused by one butterfly moiety [RuB₂S]. Analogous fac-3c, [PPh₃Ru{κ³-H,S,S′-(NH₂BSBH₂N)(SC₅H₄)₂}], can also be synthesized from the reaction of BH₃·THF with [PPh₃{κ²-N,S-(SNC₅H₄)}{κ³-H,S,S′-BH₂(SNH₄C₅)₂}Ru], cis–fac-1c. In stark contrast, when mer-2b was treated with BH₂Mes (Mes = 2,4,6-trimethyl phenyl) it led to the formation of trans- and cis-bis(dihydroborate) complexes [{κ³-S,H,H-(NH₂BMes)Ru(S₂C₇H₄)}₂], (trans-4 and cis-4). Both the complexes have two five-membered [Ru–(H)₂–B–NCS] ruthenacycles with κ²-H–H coordination modes. Density functional theory (DFT) calculations suggest that the activation of boranes across the dual Ru–N site is more facile than the Ru–S one.

Redox-active ruthenium complexes supported by hemilabile κ²-N,S-chelated ruthenacycles undergo unusual dual site B–H bond activation through metal–ligand cooperation with free and bulky boranes.     

Detection of σ-alkane complexes of manganese by NMR and IR spectroscopy in solution: (η5-C5H5)Mn(CO)2(ethane) and (η5-C5H5)Mn(CO)2(isopentane)

Irradiation of CpMn(CO)₃ in liquid ethane at 135 K at 355 nm yields a photoproduct that exhibits ν(CO) bands in the IR spectrum shifted to low wavenumber with respect to CpMn(CO)₃ that are indicative of a Mn(i) dicarbonyl. Parallel experiments employing in situ irradiation within an NMR probe (133 K, 355 nm photolysis) reveal the ¹H NMR signals of this product and confirm its formulation as the σ-ethane complex CpMn(CO)₂(η²-C1–H-ethane). The resonance of its coordinated C–H group is observed at δ –5.84 and decays with lifetime of ca. 360 s. Analogous photolysis experiments in isopentane solution with IR detection produce CpMn(CO)₂(η²-C–H-isopentane) with similar IR bands to those of CpMn(CO)₂(η²-C–H-ethane). ¹H NMR spectra of the same species were obtained by irradiation of CpMn(CO)₃ in a 60 : 40 mixture of propane and isopentane; three isomers of CpMn(CO)₂(η²-C–H-isopentane) were detected with coordination of manganese at the two inequivalent methyl positions and at the methylene group, respectively. The lifetimes of these isomers are ca. 380 ± 20 s at 135 K and do not vary significantly from each other. These σ-complexes of manganese are far more reactive than those of related CpRe(CO)₂(alkane) complexes which are stable in solution at 170–180 K. The room temperature lifetimes of CpMn(CO)₂(η²-C–H-ethane) and CpMn(CO)₂(η²-C–H-isopentane), as determined by TRIR spectroscopy, are 2.0 ± 0.1 and 28 ± 1 μs, respectively.     

Arene ruthenium oxinato complexes: Synthesis, molecular structure and catalytic activity for the hydrogenation of carbon dioxide in aqueous solution

Two families of arene ruthenium oxinato complexes of the types [(η⁶-arene)Ru(η²-N,O-L)Cl] and [(η⁶-arene)Ru(η²-N,O-L)(OH₂)]⁺ have been synthesized from the dinuclear precursors [(η⁶-arene)RuCl₂]₂ (arene = para-cymeme or hexamethylbenzene) and the corresponding oxine LH (LH = 8-hydroxyquinoline, 5-chloro-8-hydroxyquinoline, 5,7-dichloro-8-hydroxyquinoline, 5-nitro-8-hydroxyquinoline, 5,7-dimethyl-8-hydroxyquinoline, 5,7-dichloro-2-methyl-8-hydroxyquinoline). The molecular structures of the neutral chloro complexes [(η⁶-C₆Me₆)Ru(η²-N,O-L)Cl] (LH = 8-hydroxyquinoline, 5,7-dichloro-2-methyl-8-hydroxyquinoline) and [(η⁶-MeC₆H₄Prⁱ)Ru(η²-N,O-L)Cl] (LH = 5,7-dichloro-2-methyl-8-hydroxyquinoline) as well as those of the cationic aqua derivatives [(η⁶-MeC₆H₄Prⁱ)Ru(η²-N,O-L)(OH₂)]⁺ (LH = 8-hydroxyquinoline, 5,7-dimethyl-8-hydroxyquinoline), isolated as the tetrafluoroborate salts, show in all cases a piano-stool arrangement with the arene ligand, the chelating oxinato ligand and the chloro or the aqua ligand surrounding the ruthenium center in a pseudo-tetrahedral fashion. The analogous reaction of [(η⁶-MeC₆H₄Prⁱ)RuCl₂]₂ with other N,O-chelating ligands such as 2-pyridinemethanol or tetrahydrofurfurylamine did not give the expected analogs but resulted in the formation of the complexes [(η⁶-MeC₆H₄Prⁱ)Ru(η²-NC₅H₄CH₂OH)Cl]⁺ and [(η⁶-MeC₆H₄Prⁱ)Ru(η¹-NHCH₂C₄H₃O)Cl₂]. The neutral and cationic complexes of the types [(η⁶-arene)Ru(η²-N,O-L)Cl] and [(η⁶-arene)Ru(η²-N,O-L)(OH₂)]⁺ have been found to catalyze the hydrogenation of carbon dioxide to give formate in alkaline aqueous solution with catalytic turnovers up to 400.     

Syntheses,characterization, and crystal structures of ruthenium(II)/(III) complexes with tridentate salicylaldiminato ligands

Treatment of [Ru(PPh₃)₃Cl₂] with one equivalent of tridentate Schiff base 2-[(2-dimethylamino-ethylimino)-methyl]-phenol (HL) in the presence of triethylamine afforded a ruthenium(III) complex [RuCl₃(κ²-N,N-NH₂CH₂CH₂NMe₂)(PPh₃)] as a result of decomposition of HL. Interaction of HL and one equivalent of [RuHCl(CO)(PPh₃)₃], [Ru(CO)₂Cl₂] or [Ru(tht)₄Cl₂] (tht = tetrahydrothiophene) under different conditions led to isolation of the corresponding ruthenium(II) complexes [RuCl(κ³-N,N,O-L)(CO)(PPh₃)] (2), [RuCl(κ³-N,N,O-L)(CO)₂] (3), and a ruthenium(III) complex [RuCl₂(κ³-N,N,O-L)(tht)] (4), respectively. Molecular structures of 1·CH₂Cl₂, 2·CH₂Cl₂, 3 and 4 have been determined by single-crystal X-ray diffraction.     

Unexpected effect of catalyst concentration on photochemical CO2 reduction by trans(Cl)–Ru(bpy)(CO)2Cl2: new mechanistic insight into the CO/HCOO– selectivity

Photochemical CO₂ reduction catalysed by trans(Cl)–Ru(bpy)(CO)₂Cl₂ (bpy = 2,2′-bipyridine) efficiently produces carbon monoxide (CO) and formate (HCOO^–) in N,N-dimethylacetamide (DMA)/water containing [Ru(bpy)₃]²⁺ as a photosensitizer and 1-benzyl-1,4-dihydronicotinamide (BNAH) as an electron donor. We have unexpectedly found catalyst concentration dependence of the product ratio (CO/HCOO^–) in the photochemical CO₂ reduction: the ratio of CO/HCOO^– decreases with increasing catalyst concentration. The result has led us to propose a new mechanism in which HCOO^– is selectively produced by the formation of a Ru(i)–Ru(i) dimer as the catalyst intermediate. This reaction mechanism predicts that the Ru–Ru bond dissociates in the reaction of the dimer with CO₂, and that the insufficient electron supply to the catalyst results in the dominant formation of HCOO^–. The proposed mechanism is supported by the result that the time-course profiles of CO and HCOO^– in the photochemical CO₂ reduction catalysed by [Ru(bpy)(CO)₂Cl]₂ (0.05 mM) are very similar to those of the reduction catalysed by trans(Cl)–Ru(bpy)(CO)₂Cl₂ (0.10 mM), and that HCOO^– formation becomes dominant under low-intensity light. The kinetic analyses based on the proposed mechanism could excellently reproduce the unusual catalyst concentration effect on the product ratio. The catalyst concentration effect observed in the photochemical CO₂ reduction using [Ru(4dmbpy)₃]²⁺ (4dmbpy = 4,4′-dimethyl-2,2′-bipyridine) instead of [Ru(bpy)₃]²⁺ as the photosensitizer is also explained with the kinetic analyses, reflecting the smaller quenching rate constant of excited [Ru(4dmbpy)₃]²⁺ by BNAH than that of excited [Ru(bpy)₃]²⁺. We have further synthesized trans(Cl)–Ru(6Mes-bpy)(CO)₂Cl₂ (6Mes-bpy = 6,6′-dimesityl-2,2′-bipyridine), which bears bulky substituents at the 6,6′-positions in the 2,2′-bipyridyl ligand, so that the ruthenium complex cannot form the dimer due to the steric hindrance. We have found that this ruthenium complex selectively produces CO, which strongly supports the catalytic mechanism proposed in this work.     

Arene Ruthenium(II) Complexes Bearing the κ-P or κ-P,κ-S Ph2P(CH2)3SPh Ligand

Neutral [Ru(η⁶-arene)Cl₂{Ph₂P(CH₂)₃SPh-κP}] (arene = benzene, indane, 1,2,3,4-tetrahydronaphthalene: 2a, 2c and 2d) and cationic [Ru(η⁶-arene)Cl(Ph₂P(CH₂)₃SPh-κP,κS)]X complexes (arene = mesitylene, 1,4-dihydronaphthalene; X = Cl: 3b, 3e; arene = benzene, mesitylene, indane, 1,2,3,4-tetrahydronaphthalene, and 1,4-dihydronaphthalene; X = PF₆: 4a–4e) complexes were prepared and characterized by elemental analysis, IR, ¹H, ¹³C and ³¹P NMR spectroscopy and also by single-crystal X-ray diffraction analyses. The stability of the complexes has been investigated in DMSO. Complexes have been assessed for their cytotoxic activity against 518A2, 8505C, A253, MCF-7 and SW480 cell lines. Generally, complexes exhibited activity in the lower micromolar range; moreover, they are found to be more active than cisplatin. For the most active ruthenium(II) complex, 4b, bearing mesitylene as ligand, the mechanism of action against 8505C cisplatin resistant cell line was determined. Complex 4b induced apoptosis accompanied by caspase activation.     

Regulation of electron donating ability to metal center: isolation and characterization of ruthenium carbonyl complexes with N,N- and/or N,O-donor polypyridyl ligands

Polypyridyl ruthenium(II) dicarbonyl complexes with an N,O- and/or N,N-donor ligand, [Ru(pic)(CO)₂Cl₂]⁻ (1), [Ru(bpy)(pic)(CO)₂]⁺ (2), [Ru(pic)₂(CO)₂] (3), and [Ru(bpy)₂(CO)₂]²⁺ (4) (pic=2-pyridylcarboxylato, bpy=2,2′-bipyridine) were prepared for comparison of the electron donor ability of these ligands to the ruthenium center. A carbonyl group of [Ru(L1)(L2)(CO)₂]ⁿ (L1, L2=bpy, pic) successively reacted with one and two equivalents of OH⁻ to form [Ru(L1)(L2)(CO)(C(O)OH)]ⁿ⁻¹ and [Ru(L1)(L2)(CO)(CO₂)]ⁿ⁻². These three complexes exist as equilbrium mixtures in aqueous solutions and the equilibrium constants were determined potentiometrically. Electrochemical reduction of 2 in CO₂-saturated CH₃CN–H₂O at −1.5 V selectively produced CO.     

Syntheses and Characterization of the First Cycloheptatrienyl Transition-Metal Complexes with a M-CF3 Bond

The organometallic chemistry of metal complexes with organocyclic ligands of higher than five hapticity is much more lacking than the chemistry of metal complexes with η⁵-cyclopentadienyl ligands, which has been explored in considerable depth, resulting in novel advances. The main reason for this is stability. In particular, reports indicate that (η⁷-C₇H₇)ML_n complexes are considerably less stable than analogous (η⁵-C₅H₅)ML_n. In perfluoroalkyl metal chemistry, there is currently no reported (η⁷-C₇H₇)ML_n derivative, whereas a number of alkylated ones are known and important conclusions have been drawn about their stability. Responding to this void, and using Morrison’s trifluoromethylating reagent, the present study reports the synthesis and characterization of the first cycloheptatrienyl molybdenum complexes bearing the trifluoromethyl moiety; (η⁷-C₇H₇)Mo(CO)₂CF₃ (I), and (η⁷-C₇H₇)Mo(CO)(PMe₃)CF₃ (II) and discusses their low thermal instability.     

Bifunctional activation of amine-boranes by the W/Pd bimetallic analogs of “frustrated Lewis pairs”

The reaction between basic [(PCP)Pd(H)] (PCP = 2,6-(CH₂P(t-C₄H₉)₂)₂C₆H₄) and acidic [LWH(CO)₃] (L = Cp (1a), Tp (1b); Cp = η⁵-cyclopentadienyl, Tp = κ³-hydridotris(pyrazolyl)borate) leads to the formation of bimolecular complexes [LW(CO)₂(μ-CO)⋯Pd(PCP)] (4a, 4b), which catalyze amine-borane (Me₂NHBH₃, ^tBuNH₂BH₃) dehydrogenation. The combination of variable-temperature (¹H, ³¹P{¹H}, ¹¹B NMR and IR) spectroscopies and computational (ωB97XD/def2-TZVP) studies reveal the formation of an η¹-borane complex [(PCP)Pd(Me₂NHBH₃)]⁺[LW(CO₃)]⁻ (5) in the first step, where a BH bond strongly binds palladium and an amine group is hydrogen-bonded to tungsten. The subsequent intracomplex proton transfer is the rate-determining step, followed by an almost barrierless hydride transfer. Bimetallic species 4 are easily regenerated through hydrogen evolution in the reaction between two hydrides.

Bimetallic complexes [LW(CO)₂(μ-CO)⋯Pd(PCP)] cooperatively activate amine-boranes for their dehydrogenation via N–H proton tunneling at RDS and H₂ evolution from two neutral hydrides.     

Donor Atom Preference of Organoruthenium and Organorhodium Cations on the Interaction with Novel Ambidentate (N,N) and (O,O) Chelating Ligands in Aqueous Solution

Two novel, pyridinone-based chelating ligands containing separated (O,O) and (N_amino,N_het) chelating sets (N_amino = secondary amine; N_het = pyrrole N for H(L3) (1-(3-(((1H-pyrrole-2-yl)methyl)-amino)propyl)-3-hydroxy-2-methylpyridin-4(1H)-one) or pyridine N for H(L5) (3-hydroxy-2-methyl-1-(3-((pyridin-2-ylmethyl)amino)propyl)pyridin-4(1H)-one)) were synthesized via reduction of the appropriate imines. Their proton dissociation processes were explored, and the molecular structures of two synthons were assessed by X-ray crystallography. These ambidentate chelating ligands are intended to develop Co(III)/PGM (PGM = platinum group metal) heterobimetallic multitargeted complexes with anticancer potential. To explore their metal ion binding ability, the interaction with Pd(II), [(η⁶-p-cym)Ru]²⁺ and [(η⁵-Cp*)Rh]²⁺ (p-cym = 1-methyl-4-isopropylbenzene, Cp* = pentamethyl-cyclopentadienyl anion) cations was studied in aqueous solution with the combined use of pH-potentiometry, NMR and HR ESI-MS. In general, organorhodium was found to form more labile complexes over ruthenium, while complexation of the (N,N) chelating set was slower than the processes of the pyridinone unit with (O,O) coordination. Formation of the organoruthenium complexes starts at lower pH (higher thermodynamic stabilities of the corresponding complexes) than for [(η⁵-Cp*)Rh]²⁺ but, due to the higher affinity of [η⁶-p-cym)Ru]²⁺ towards hydrolysis, the complexed ligands are capable of competing with hydroxide ion in a lesser extent than for the rhodium systems. As a result, under biologically relevant conditions, the rhodium binding effectivity of the ligands becomes comparable or even slightly higher than their effectivity towards ruthenium. Our results indicate that H(L3) is a less efficient (N,N) chelator for these metal ions than H(L5). Similarly, due to the relative effectivity of the (O,O) and (N,N) chelates at a 1:1 metal-ion-to-ligand ratio, H(L5) coordinates in a (N,N) manner to both cations in the whole pH range studied while, for H(L3), the complexation starts with (O,O) coordination. At a 2:1 metal-ion-to-ligand ratio, H(L3) cannot hinder the intensive hydrolysis of the second metal ion, although a small amount of 2:1 complex with [(η⁵-Cp*)Rh]²⁺ can also be detected.     

MM quadruply bonded complexes supported by vinylbenzoate ligands: synthesis,characterization, photophysical properties and application as synthons

From the reactions between M₂(TⁱPB)₄ compounds and meta and para-vinylbenzoic acids (2 equiv.) in toluene at room temperature the compounds trans-M₂(TⁱPB)₂L₂, where L = m-vinylbenzoate 1A (M = Mo) and 1B (M = W) and TⁱPB = 2,4,6-triisopropylbenzoate, and where L = p-vinylbenzoate 2A (M = Mo) and 2B (M = W) have been isolated. Compounds 1A and 2A have been shown to undergo Heck carbon–carbon coupling reactions with phenyliodide to produce trans-Mo₂(TⁱPB)₂(O₂CC₆H₄-m-CHCH–C₆H₅)₂, 3A and trans-Mo₂(TⁱPB)₂(O₂CC₆H₄-p-CHCH–C₆H₅)₂, 4A. The molybdenum compounds 1A and 2A have been structurally characterized by single crystal X-ray crystallography. All the new compounds have been characterized by ¹H NMR, IR, UV-visible absorption and emission spectroscopy, high resolution MALDI-TOF MS, fs- and ns-transient absorption spectroscopy and fs-time-resolved IR spectroscopy. Electronic structure calculations employing density functional theory, DFT, and time-dependent DFT have been employed to aid in the interpretation of spectral data. All compounds show intense absorptions in the visible region corresponding to M₂δ to Lπ* charge transfer transitions. The lifetimes of the ¹MLCT state fall in the range of 1–10 ps and for the molybdenum complexes the T₁ states are ³δδ* with lifetimes ∼50 μs while for the tungsten complexes the T₁ are ³MLCT with lifetimes in the range of 3–10 ns.     

Ferro- and Antiferromagnetic Interactions in Oxalato-Centered Inverse Hexanuclear and Chain Copper(II) Complexes with Pyrazole Derivatives

Two novel copper(II) complexes of formulas {[Cu(4-Hmpz)₄][Cu(4-Hmpz)₂(µ₃-ox-κ²O¹,O²:κO^2′:κO^1′)(ClO₄)₂]}_n (1) and {[Cu(3,4,5-Htmpz)₄]₂[Cu(3,4,5-Htmpz)₂(µ₃-ox-κ²O¹,O²:κO^2′:κO^1′)(H₂O)(ClO₄)]₂[Cu₂(3,4,5-Htmpz)₄(µ-ox-κ²O¹,O²:κ²O^2′,O^1′)]}(ClO₄)₄·6H₂O (2) have been obtained by using 4-methyl-1H-pyrazole (4-Hmpz) and 3,4,5-trimethyl-1H-pyrazole (3,4,5-Htmpz) as terminal ligands and oxalate (ox) as the polyatomic inverse coordination center. The crystal structure of 1 consists of perchlorate counteranions and cationic copper(II) chains with alternating bis(pyrazole)(µ₃-κ²O¹,O²:κO^2′:κO^1′-oxalato)copper(II) and tetrakis(pyrazole)copper(II) fragments. The crystal structure of 2 is made up of perchlorate counteranions and cationic centrosymmetric hexanuclear complexes where an inner tetrakis(pyrazole)(µ-κ²O¹,O²:κ²O^2′,O^1′-oxalato)dicopper(II) entity and two outer mononuclear tetrakis(pyrazole)copper(II) units are linked through two mononuclear aquabis(pyrazole)(µ₃-κ²O¹,O²:κO^2′:κO^1′-oxalato)copper(II) units. The magnetic properties of 1 and 2 were investigated in the temperature range 2.0–300 K. Very weak intrachain antiferromagnetic interactions between the copper(II) ions through the µ₃-ox-κ²O¹,O²:κO^2′:κO^1′ center occur in 1 [J = −0.42(1) cm⁻¹, the spin Hamiltonian being defined as H = −J∑S_1,i · S_2,i+1], whereas very weak intramolecular ferromagnetic [J = +0.28(2) cm⁻¹] and strong antiferromagnetic [J’ = −348(2) cm⁻¹] couplings coexist in 2 which are mediated by the µ₃-ox-κ²O¹,O²:κO^2′:κO^1′ and µ-ox-κ²O¹,O²:κ²O^2′,O^1′ centers, respectively. The variation in the nature and magnitude of the magnetic coupling for this pair of oxalato-centered inverse copper(II) complexes is discussed in the light of their different structural features, and a comparison with related oxalato-centered inverse copper(II)-pyrazole systems from the literature is carried out.     

IR-Spectroscopic Study of Complex Formation of Nitrogen Oxides (NO,N2O) with Cationic Forms of Zeolites and the Reactivity of Adsorbed Species in CO and CH4 Oxidation

The formation of complexes and disproportionation of nitrogen oxides (NO, N₂O) on cationic forms of LTA, FAU, and MOR zeolites was investigated by diffuse-reflectance IR spectroscopy. N₂O is adsorbed on the samples under study in the molecular form and the frequencies of the first overtone of the stretching vibrations ν¹_0–2 and the combination bands of the stretching vibrations with other vibrational modes for N₂O complexes with cationic sites in zeolites (ν³_0–1 + ν¹_0–1, ν¹_0–1 + δ_0–2) are more significantly influenced by the nature of the zeolite. The presence of several IR bands in the region of 2400–2600 cm⁻¹ (the ν¹_0–1 + δ_0–2 transitions) for different zeolite types was explained by the availability of different localization sites for cations in these zeolites. The frequencies in this region also depend on the nature of the cation (its charge and radius). The data can be explained by the specific geometry of the N₂O complex formed, presumably two-point adsorption of N₂O on a cation and a neighboring oxygen atom of the framework. Adsorption of CO or CH₄ on the samples with preliminarily adsorbed N₂O at 20–180 °C does not result in any oxidation of these molecules. NO⁺ and N₂O₃ species formed by disproportionation of NO are capable of oxidizing CO and CH₄ molecules to CO₂, whereas NO_x is reduced simultaneously to N₂ or N₂O. The peculiarities in the behavior of cationic forms of different zeolites with respect to adsorbed nitrogen oxides determined by different density and localization of cations have been established.     

Synthesis and structural characterization of a coordinatively unsaturated ruthenium complex,CpRu(Ph2nacnac), and its CO adduct

Two new half sandwich ruthenium complexes with 2-N-phenylamino-4-N-phenylimino-2-pentene (Ph₂nacnac) ligands have been synthesized and characterized. Single crystal X-ray diffraction analysis reveals the monomeric, highly air sensitive complex Cp^∗Ru(Ph₂nacnac) (4) has a coordinatively unsaturated structure and the coordination environment around Ru(II) is effectively a triangle made up of Ct(Cp^∗)–N(1)–N(2). An air stable complex Cp^∗Ru(Ph₂nacnac)(CO) (5) is prepared by reaction of 4 with CO, and has a pseudo-tetrahedral geometry around the Ru(II) center, made up of Ct(Cp^∗)–N(1)–N(2)–C(28).     

Reactions of 2-(arylazo)aniline with ruthenium substrates: Isolation, characterizations and reactivities of delocalized diazoketiminato and orthometallated Ru(II) chelates

Reactions of 2-(arylazo)aniline, HL-NH₂ [H represents the dissociable protons upon complexation and HL-NH₂ is p-RC₆H₄NNC₆H₄-NH₂; R = H for HL¹-NH₂; CH₃ for HL²-NH₂ and Cl for HL³-NH₂] with Ru(H)(CO)(PPh₃)₃Cl and Ru(CO)₃(PPh₃)₂ afforded products of compositions [(HL-NH)Ru(CO)Cl(PPh₃)₂] and [(L-NH)Ru(PPh₃)₂(CO)], respectively. All the complexes were characterized unequivocally. The X-ray structures of the complexes 4c and 5c have been determined. The cyclic volatammograms exhibited one reversible oxidative response in the range of 0.56–0.16 V versus SCE for [(L-NH)Ru(PPh₃)₂(CO)] and a quasi reversible oxidative response within 0.56–0.70 V versus SCE for [(HL-NH)Ru(CO)Cl(PPh₃)₂]. The conversion of ketones to corresponding alcohols has been studied in presence of newly synthesized ruthenium complexes.     

Synthesis, characterization and photophysics of bimetallic manganese(I) and ruthenium(II) complexes

A series of new manganese(I) and ruthenium(II) monometallic and bimetallic complexes made of 2,2′-bipyridine and 1,10-phenanthroline ligands, [Mn(CO)₃(NN)(4,4′-bpy)]⁺, [{(CO)₃(NN)Mn}₂(4,4′-bpy)]²⁺ and [(CO)₃(NN)Mn(4,4′-bpy)Ru(NN)₂Cl]²⁺ (NN = 2,2′-bipyridine, 1,10-phenanthroline; 4,4′-bpy = 4,4′-bipyridine) are synthesized and characterized, in addition to already known ruthenium(II) complexes [Ru(NN)₂Cl(4,4′-bpy)]⁺ and [Cl(NN)₂Ru(4,4′-bpy)Ru(NN)₂Cl]²⁺. The electrochemical properties show that there is a weak interaction between two metal centers in Mn–Ru heterobimetallic complexes. The photophysical behavior of all the complexes is studied. The Mn(I) monometallic and homobimetallic complexes have no detectable emission. In Mn–Ru heterobimetallic complexes, the attachment of Mn(I) with Ru(II) provides interesting photophysical properties.     

Ruthenafuran Complexes Supported by the Bipyridine-Bis(diphenylphosphino)methane Ligand Set: Synthesis and Cytotoxicity Studies

Mononuclear and dinuclear Ru(II) complexes cis-[Ru(κ²-dppm)(bpy)Cl₂] (1), cis-[Ru(κ²-dppe)(bpy)Cl₂] (2) and [Ru₂(bpy)₂(μ-dpam)₂(μ-Cl)₂](Cl)₂ ([3](Cl)₂) were prepared from the reactions between cis(Cl), cis(S)-[Ru(bpy)(dmso-S)₂Cl₂] and diphosphine/diarsine ligands (bpy = 2,2′-bipyridine; dppm = 1,1-bis(diphenylphosphino)methane; dppe = 1,2-bis(diphenylphosphino)ethane; dpam = 1,1-bis(diphenylarsino)methane). While methoxy-substituted ruthenafuran [Ru(bpy)(κ²-dppe)(C^O)]⁺ ([7]⁺; C^O = anionic bidentate [C(OMe)CHC(Ph)O]⁻ chelate) was obtained as the only product in the reaction between 2 and phenyl ynone HC≡C(C=O)Ph in MeOH, replacing 2 with 1 led to the formation of both methoxy-substituted ruthenafuran [Ru(bpy)(κ²-dppm)(C^O)]⁺ ([4]⁺) and phosphonium-ring-fused bicyclic ruthenafuran [Ru(bpy)(P^C^O)Cl]⁺ ([5]⁺; P^C^O = neutral tridentate [(Ph)₂PCH₂P(Ph)₂CCHC(Ph)O] chelate). All of these aforementioned metallafuran complexes were derived from Ru(II)–vinylidene intermediates. The potential applications of these metallafuran complexes as anticancer agents were evaluated by in vitro cytotoxicity studies against cervical carcinoma (HeLa) cancer cell line. All the ruthenafuran complexes were found to be one order of magnitude more cytotoxic than cisplatin, which is one of the metal-based anticancer agents being widely used currently.     

Modification of amyloid-beta peptide aggregation via photoactivation of strained Ru(ii) polypyridyl complexes

Alzheimer''s disease (AD) is a chronic neurodegenerative disorder characterized by progressive and irreversible damage to the brain. One of the hallmarks of the disease is the presence of both soluble and insoluble aggregates of the amyloid beta (Aβ) peptide in the brain, and these aggregates are considered central to disease progression. Thus, the development of small molecules capable of modulating Aβ peptide aggregation may provide critical insight into the pathophysiology of AD. In this work we investigate how photoactivation of three distorted Ru(ii) polypyridyl complexes (Ru1–3) alters the aggregation profile of the Aβ peptide. Photoactivation of Ru1–3 results in the loss of a 6,6′-dimethyl-2,2′-bipyridyl (6,6′-dmb) ligand, affording cis-exchangeable coordination sites for binding to the Aβ peptide. Both Ru1 and Ru2 contain an extended planar imidazo[4,5-f][1,10]phenanthroline ligand, as compared to a 2,2′-bipyridine ligand for Ru3, and we show that the presence of the phenanthroline ligand promotes covalent binding to Aβ peptide His residues, and in addition, leads to a pronounced effect on peptide aggregation immediately after photoactivation. Interestingly, all three complexes resulted in a similar aggregate size distribution at 24 h, forming insoluble amorphous aggregates as compared to significant fibril formation for peptide alone. Photoactivation of Ru1–3 in the presence of pre-formed Aβ_1–42 fibrils results in a change to amorphous aggregate morphology, with Ru1 and Ru2 forming large amorphous aggregates immediately after activation. Our results show that photoactivation of Ru1–3 in the presence of either monomeric or fibrillar Aβ_1–42 results in the formation of large amorphous aggregates as a common endpoint, with Ru complexes incorporating the extended phenanthroline ligand accelerating this process and thereby limiting the formation of oligomeric species in the initial stages of the aggregation process that are reported to show considerable toxicity.

Photoactivation of a series of Ru(ii) polypyridyl complexes leads to ligand exchange and modulation of amyloid-beta peptide aggregation of relevance to Alzheimer''s disease.     

Optically active transition metal complexes. Part 117:Synthesis,crystal structure and properties of chiral (η6-arene)ruthenium complexes with N,O- and N,N-ligands

The complexes [(η⁶-p-ⁱPrC₆H₄Me)Ru(NO₂pesa)Cl] 2, [(η⁶-p-ⁱPrC₆H₄Me)Ru(oxazsa)Cl] 3 and [(η⁶-p-ⁱPrC₆H₄Me)Ru(pepy)Cl] 4, chiral in the chelate ligand and chiral at the ruthenium atom, have been prepared by reaction of [(η⁶-p-ⁱPrC₆H₄Me)RuCl₂]₂ with the anions of the (S)-configured bidentate N,O- and N,N-ligands. [(η⁶-p-ⁱPrC₆H₄Me)Ru(pesa)I] 5 was synthesized by halide exchange. The diastereomer ratios of compounds 2–4 with respect to the stereogenic ruthenium atom are in CDCl₃ 2a:2b=81:19, 3a:3b=77:23 and 4a:4b=61:39. Compound 5 is obtained diastereomerically pure. An X-ray structure analysis of 3 shows (R_Ru,S_C)-configuration