Synthesis, characterization and reactivity of polypyridyl ruthenium(II) carbonyl complexes with phosphine derivatives: Ruthenium-carbon bond labilization based on steric and electronic effects

Ruthenium phosphine complexes with a CO ligand [Ru(tpy)(PR₃)(CO)Cl]⁺ (tpy = 2,2′:6′,2″-terpyridine, R = Ph or p-tolyl), were prepared by introduction of CO gas to the corresponding dichloro complexes at room temperature. New carbonyl complexes were characterized by various methods including structural analyses. They were shown to release CO following the addition of several N-donors to form the corresponding substituted complexes. The kinetic data and structural results observed in this study indicated that the CO release reactions proceeded in an interchange mechanism. The molecular structures of [Ru(tpy)(PPh₃)(CO)Cl]PF₆, [Ru(tpy)(P(p-tolyl)₃)(CO)Cl]PF₆ and [Ru(tpy)(PPh₃)(CH₃CN)Cl]PF₆ were determined by X-ray crystallography.     

Interactions of arene-Ru(II)-chloroquine complexes of known antimalarial and antitumor activity with human serum albumin (HSA) and transferrin

The interactions of π-arene-Ru(II)-chloroquine complexes with human serum albumin (HSA), apotransferrin and holotransferrin have been studied by circular dichroism (CD) and UV-Visible spectroscopies, together with isothermal titration calorimetry (ITC). The data for [Ru(η⁶-p-cymene)(CQ)(H₂O)Cl]PF₆ (1), [Ru(η⁶-benzene)(CQ)(H₂O)Cl]PF₆ (2), [Ru(η⁶-p-cymene)(CQ)(H₂O)₂][PF₆]₂ (3), [Ru(η⁶-p-cymene)(CQ)(en)][PF₆]₂ (4), [Ru(η⁶-p-cymene)(η⁶-CQDP)][BF₄]₂ (5) (CQ: chloroquine; DP: diphosphate; en: ethylenediamine), in comparison with CQDP and [Ru(η⁶-p-cymene)(en)Cl][PF₆] (6) as controls demonstrate that 1, 2, 3, and 5, which contain exchangeable ligands, bind to HSA and to apotransferrin in a covalent manner. The interaction did not affect the α-helical content in apotransferrin but resulted in a loss of this type of structure in HSA. The binding was reversed in both cases by a decrease in pH and in the case of the Ru-HSA adducts, also by addition of chelating agents. A weaker interaction between complexes 4 and 6 and HSA was measured by ITC but was not detectable spectroscopically. No interactions were observed for complexes 4 and 6 with apotransferrin or for CQDP with either protein. The combined results suggest that the arene-Ru(II)-chloroquine complexes, known to be active against resistant malaria and several lines of cancer cells, also display a good transport behavior that makes them good candidates for drug development.     

Cytotoxicity of half sandwich ruthenium(II) complexes with strong hydrogen bond acceptor ligands and their mechanism of action

Neutral and cationic organometallic ruthenium(II) piano stool complexes of the type [(η⁶-cymene)RuCl(X)(Y)] (complexes R1-R8) has been synthesized and characterized. In cationic complexes, X, Y is either a η² phosphorus ligand such as 1,1-bis(diphenylphosphino)methane (DPPM) and 1,2-bis(diphenylphosphino)ethane (DPPE) or partially oxidized ligands such as 1,2-bis(diphenylphosphino)methane monooxide (DPPMO) and 1,2-bis(diphenylphosphino)ethane monooxide (DPPEO) which are strong hydrogen bond acceptors. In neutral complexes, X is chloride and Y is a monodentate phosphorous donor. Complexes with DPPM and DPPMO ligands ([(η⁶-cymene)Ru(η²-DPPM)Cl]PF₆ (R2), [(η⁶-cymene)Ru(η²-DPPMO)Cl]PF₆ (R3), [(η⁶-cymene)Ru(η¹-DPPM)Cl₂] (R5) and [(η⁶-cymene)Ru(η¹-DPPMO)Cl₂] (R6) show good cytotoxicity. Growth inhibition study of several human cancer cell lines by these complexes has been carried out. Mechanistic studies for R5 and R6 show that inhibition of cancer cell growth involves both cell cycle arrest and apoptosis induction. Using an apoptosis PCR array, we identified the sets of anti-apoptotic genes that were down regulated and pro-apoptotic genes that were up regulated. These complexes were also found to be potent metastasis inhibitors as they prevented cell invasion through matrigel. The complexes were shown to bind DNA in a non intercalative fashion and cause unwinding of plasmid DNA in cell-free medium by competitive ethidium bromide binding, viscosity measurements, thermal denaturation and gel mobility shift assays.     

Arene-Ru(II)-chloroquine complexes interact with DNA, induce apoptosis on human lymphoid cell lines and display low toxicity to normal mammalian cells

The complexes [Ru(η⁶-p-cymene)(CQ)Cl₂] (1), [Ru(η⁶-benzene)(CQ)Cl₂] (2), [Ru(η⁶-p-cymene)(CQ)(H₂O)₂][BF₄]₂ (3), [Ru(η⁶-p-cymene)(en)(CQ)][PF₆]₂ (4), [Ru(η⁶-p-cymene)(η⁶-CQDP)][BF₄]₂ (5) (CQ = chloroquine base; CQDP = chloroquine diphosphate; en = ethylenediamine) interact with DNA to a comparable extent to that of CQ and in analogous intercalative manner with no evidence for any direct contribution of the metal, as shown by spectrophotometric and fluorimetric titrations, thermal denaturation measurements, circular dichroism spectroscopy and electrophoresis mobility shift assays. Complexes 1-5 induced cytotoxicity in Jurkat and SUP-T1 cancer cells primarily via apoptosis. Despite the similarities in the DNA binding behavior of complexes 1-5 with those of CQ the antitumor properties of the metal drugs do not correlate with those of CQ, indicating that DNA is not the principal target in the mechanism of cytotoxicity of these compounds. Importantly, the Ru-CQ complexes are generally less toxic toward normal mouse splenocytes and human foreskin fibroblast cells than the standard antimalarial drug CQDP and therefore this type of compound shows promise for drug development.     

Syntheses and structures of vinyl and aryl derivatives of carbonyl halide iron complexes

cis,trans-Fe(CO)₂(PMe₃)₂(p-Y-C₆H₄)X [X=Br, Y=H (4a), MeO (4b), Cl (4c), F (4d), Me (4e); X=I, Y=H (5); X=Cl, Y=H (6)] and cis,trans-Fe(CO)₂(PMe₃)₂(σ-CHCH₂)X [X=Br (7); X=I (8); X=Cl (9)] are prepared by reacting dihalide complexes cis,trans,cis- Fe(CO)₂(PMe₃)₂X₂ [X=Br (1), X=I (2), X=Cl (3)] with Grignard reagents p-Y-C₆H₄-MgBr (Y=H, OMe, Cl, F, Me) or CH₂CH-MgBr and with lithium reagents PhLi, CH₂CH-Li. With both reagents, the reaction proceeds following two parallel pathways: one is the metallation reaction which yields alkyl derivatives, the other affords 17 electron complexes [Fe(CO)₂(PMe₃)₂X] via monoelectron reductive elimination. The influence of the halides and organometallic reagents on the yield of the metallation reaction is discussed. The solution structure of the complexes is assigned on the basis of IR and ¹H, ¹³C, ¹⁹F, ³¹P NMR spectra. The solid state structure of complexes 4a, 5 and 6 is determined by single crystal X-ray diffractometric methods.     

Synthesis and characterisation of ferrocene-containing β-diketonato complexes of rhodium(I) and rhodium(III)

The synthesis of new β-diketonato rhodium(I) complexes of the type [Rh(FcCOCHCOR)(CO)₂] and [Rh(FcCOCHCOR)(CO)(PPh₃)] with Fc=ferrocenyl and R=Fc, C₆H₅, CH₃ and CF₃ are described. ¹H, ¹³C and ³¹P NMR data showed that for each of the non-symmetric β-diketonato mono-carbonyl rhodium(I) complexes, two isomers exist in solution. The equilibrium constant, K_c, which relates these two isomers in an equilibrium reaction, are concentration independent but temperature and solvent dependent. Δ_rG, Δ_rH and Δ_rS values for this equilibrium have been determined and a linear relationship between solvent polarity on the Dimroth scale and K_c exists. The relationship between RhP bond lengths, d(RhP), and ³¹P NMR peak positions as well as coupling constants ¹J(³¹P¹⁰³Rh) has been quantified to allow calculation of approximate d(RhP) values. Variations in d(RhP) for [Rh(RCOCHCOR′)(CO)(PPh₃)] complexes have also been related to the group electronegativities (Gordy scale) of the terminal β-diketonato R groups trans to PPh₃. A measure of the electron density on the rhodium centre of [Rh(RCOCHCOR′)(CO)(PPh₃)] may be expressed in terms of the IR carbonyl stretching wave number, ν(CO), the sum of the group electronegativities of the R and R′ groups, (χ_R+χ_R′), or the observed pK_a^′ values of the free β-diketones RCOCH₂COR^′. An empirical relationship between ν(CO) and either pK_a^′ or (χ_R+χ_R′) has also been quantified.     

Novel [Ru(polypyridine)(CO)2Cl2] and [Ru(polypyridine)2(CO)Cl]-type complexes: Characterizing the effects of introducing azopyridyl ligands by electrochemical, spectroscopic and crystallographic measurements

The reaction of ruthenium carbonyl polymer ([Ru(CO)₂Cl₂]_n) with azopyridyl compounds (2,2′-azobispyridine; apy or 2-phenylazopyridine; pap) generated new complexes, [Ru(azo)(CO)₂Cl₂] (azo = apy, pap). [Ru(apy)(CO)₂Cl₂] underwent photodecarbonylation to give a chloro-bridged dimer complex, whereas the corresponding pap complex ([Ru(pap)(CO)₂Cl₂]) was not converted to a dimer. The reactions of the chloro-bridged dimer containing the bpy ligand (bpy = 2,2′-bipyridine) with either apy or pap resulted in the formation of mixed polypyridyl complexes, [Ru(azo)(bpy)(CO)Cl]⁺. The novel complexes containing azo ligands were characterized by various spectroscopic measurements including the determination of X-ray crystallographic structures. Both [Ru(azo)(CO)₂Cl₂] complexes have two CO groups in a cis position to each other and two chlorides in a trans position. The azo groups are situated cis to the CO ligand in [Ru(azo)(bpy)(CO)Cl]⁺. All complexes have azo N-N bond lengths of 1.26-1.29 Å. The complexes exhibited azo-based two-electron reduction processes in electrochemical measurements. The effects of introducing azopyridyl ligands to the ruthenium carbonyl complexes were examined by ligand-based redox potentials, stretching frequencies and force constants of CO groups and bond parameters around Ru-CO moieties.     

Rhodium(III) cis-dihydrido complexes with 3,6-bis(2′-pyridyl)pyridazine (dppn) and bidiazines. Crystal and molecular structure of [Rh(H)2(dppn)(PPh3)2]PF6· CH2Cl2

The acetone complex [Rh(H)₂(acetone)₂(PPh₃)₂]- PF₆ reacts with bidiazines and 3,6-bis(2′-pyridyl)- pyridazine (dppn) giving the air stable cis-dihydrido rhodium(III) [Rh(H)₂(L)(PPh₃)₂]PF₆ complexes. The structure of the dichloromethane solvate of [Rh(H)₂(dppn)(PPh₃)₂]PF₆ has been determined by X-ray crystal structure analysis. Crystals are monoclinic, space group P2₁/a, with a = 18.629(6), b = 15.339(5), c = 17.146(5) Å, β = 101.02(3)° and Z = 4. The structure has been solved from diffractometer data by Patterson and Fourier methods and refined by block-matrix least-squares to R = 0.076 for 6225 observed reflections. In the structure discrete [Rh(H)₂(dppn)(PPh₃)₂]⁺ cationic complexes, PF₆⁻ anions and dichloromethane solvent molecules are present. The Rh atom is octahedrally surrounded by two cis hydride ligands and by two cis nitrogen atoms from a dppn molecule acting as a bidentate chelating ligand through two neighbouring pyridyl and pyridazinyl nitrogen atoms. Two P atoms from PPh₃, ligands in trans apical positions complete to octahedral the coordination of Rh.     

Synthesis, structure, and characterization of some ruthenium arene complexes of N-(arylmethylene)-2-(methylthio)anilines and 2-(methylthio)aniline

A series of cationic, half-sandwich ruthenium complexes with the general formula [(η⁶-p-cymene)RuCl(MeSC₆H₄2-NCHAr)][PF₆] (3a-h), have been prepared from the reaction of [(η⁶-p-cymene)RuCl₂]₂ with various N,S-donor Schiff base ligands derived from 2-(methylthio)aniline and several substituted benzaldehydes. The related aniline complex [(η⁶-p-cymene)RuCl(MeS-C₆H₄-2-NH₂)][PF₆] (4) was synthesized from 2-(methylthio)aniline. All of the ruthenium complexes were characterized by IR, ¹H NMR, and UV/Vis spectroscopies. The molecular structure of complex 4 was determined by X-ray crystallography.     

Tetrazole and triazole carbene complexes of group 6 metal carbonyls

In order to study the relative stability of cis- and trans-isomers of bis(NHC)tetracarbonyl complexes of group 6 metals, we synthesized the corresponding complexes with triazolin- and tetrazolinylidene ligands. By reaction of the free carbene (L = 1,3,4-triphenyl-4,5-dihydro-1H-1,2,4-triazolin-5-ylidene) - first synthesized by Enders - with the hexacarbonyls of Cr, Mo and W the corresponding M(L)(CO)₅ complexes are generated. Depending on an excess of carbene also the cis-(L)₂Mo(CO)₄ complex was obtained. The latter can be photolytically converted to the trans-(L)₂Mo(CO)₄ complex. The corresponding complexes with the 1,4-dimethyltetrazolin-5-ylidene ligand (L′), Cr(L′)(CO)₅, cis-(L′)₂Cr(CO)₄ and trans-(L′)₂Cr(CO)₄ can be obtained by reaction of hexacarbonyl-μ-trihydroxy-dichromate with dimethyltetrazolium salt. In the cis-(L′)₂Cr(CO)₄ complex, one carbonyl ligand can be replaced by donor ligands such as pyridine or phenylisocyanide to form sym-mer-tricarbonyl complexes. All new complexes are fully characterized by spectroscopy and most by single-crystal X-ray analysis.     

Optically active iridium complexes with cyclopentadienyl-phosphine ligands: synthesis and oxidative addition of methyl iodide

The dimer [Ir(μ-Cl)(C₈H₁₄)₂]₂ reacts with the ligands (S)-(C₅H₄CH₂CH(Ph)PPh₂)Li and (R)-(C₅H₄CH(Cy)CH₂PPh₂)Li to give (S)-[Ir(η⁵-C₅H₄CH₂CH(Ph)PPh₂-κP)(C₈H₁₄)] and (R)-[Ir(η⁵-C₅H₄CH(Cy)CH₂PPh₂-κP)(C₈H₁₄)], which upon treatment with CH₃I at room temperature afford the cationic iridium(III) compounds (S,S_Ir)-[Ir(η⁵-C₅H₄CH₂CH(Ph)PPh₂-κP)(CH₃)(C₈H₁₄)][I] as a single diastereomer, and (R)-[Ir(η⁵-C₅H₄CH(Cy)CH₂PPh₂-κP)(CH₃)(C₈H₁₄)][I] as a 9:1 mixture of two diastereomers. If the oxidative addition reaction is performed at reflux in methylene chloride, the starting complexes convert to the neutral compounds (S)-[Ir(η⁵-C₅H₄CH₂CH(Ph)PPh₂-κP)(CH₃)(I)] and (R)-[Ir(η⁵-C₅H₄CH(Cy)CH₂PPh₂-κP)(CH₃)(I)] as 1.6:1 and 3.3:1 mixtures of diastereoisomers, respectively. Carbonyl iridium complexes are synthesized by reacting [IrCl(CO)(PPh₃)₂] with the ligands to afford (S)-[Ir(η⁵-C₅H₄CH₂CH(Ph)PPh₂-κP)(CO)] and (R)-[Ir(η⁵-C₅H₄CH(Cy)CH₂PPh₂-κP)(CO)]. They give upon treatment with CH₃I the cationic species (S)-[Ir(η⁵-C₅H₄CH₂CH(Ph)PPh₂-κP)(CH₃)(CO)][I] and (R)-[Ir(η⁵-C₅H₄CH(Cy)CH₂PPh₂-κP)(CH₃)(CO)][I] as 1.6:1 and 3:1 mixture of diastereomers, respectively. No migratory-insertion of the methyl group into the carbonyl-metal bond has been observed even after prolonged heating.     

Quantifying the electronic cis effect of phosphine, arsine and stibine ligands by use of rhodium(I) Vaska-type complexes

The cis effects of phosphine, arsine and stibine ligands have been evaluated by measuring the IR stretching frequency in dichloromethane of the carbonyl ligand in a series of Rh(I) Vaska-type complexes, trans-[RhCl(CO)(L)₂]. These data were correlated with those obtained by Tolman for the electronic trans influences in the [Ni(L)(CO)₃] complexes. The electronic contribution, χ_Fc, of ferrocenyl was determined as 0.8 from these plots by evaluating PPh₂Fc as ligand. In order to accommodate arsine and stibine ligands an additional correction term, to compensate for differences in the donor atom, was added to Tolman’s equation for calculation of the Tolman electronic parameter of phosphine ligands. In the resulting equation: ν(CO_Ni)=2056.1+∑_i=1³χ_i+C_L values for C_L of C_P=0, C_As=−1.5 and C_Sb=−3.1 are suggested for phosphine, arsine and stibine ligands, respectively. The crystal and molecular structures of trans-[RhCl(CO)(PPh₂Fc)₂] · 2C₆H₆, trans-[RhCl(CO){P(NMe₂)₃}₂] and trans-[RhCl(CO)(AsPh₃)₂] are reported. The Tolman cone angles for PPh₂Fc and P(NMe₂)₃ were determined as 169° and 166°, while the effective cone angles for PPh₂Fc, P(NMe₂)₃ and AsPh₃ were determined as 171°, 168° and 147°, respectively.     

A convenient synthesis of isocyclam and [16]aneN4 and the photophysics of their dicyanochromium(III) complexes

The syntheses of the tetraazamacrocyclic ligands 1,4,7,11-tetraazacyclotetradecane (isocyclam) and 1,5,9,13-tetraazacyclohexadecane ([16]aneN₄) in two steps starting from the corresponding tetraamine and diethylmalonate is reported. The trans-dicyanochromium(III) complexes, trans-[Cr(isocyclam)(CN)₂]PF₆ and trans-[Cr([16]aneN₄)(CN)₂]PF₆ have also been prepared. Both are ²E_g emitters with 0-0 band emission wavelengths at 721.2 and 704.8 nm, respectively. The isocyclam complex has a room temperature excited state lifetime of 147 μs in aqueous solution which increases to 215 μs upon macrocyclic N-H deuteration, whereas the corresponding lifetime of the [16]aneN₄ complex is 25 μs and is unaffected by macrocyclic N-H deuteration. The implications of the temperature dependence of the excited state lifetimes are also presented.     

Dithiolate and diselenolate complexes [Pt2(μ-ECH2CHCHCH2E)(PPh3)4] (E = S, Se): Synthesis, characterisation and mass spectrometric formation of the dichalcogenide species [Pt2(μ-E2)(PPh3)4]

The reactions of [Pt₂(μ-E)₂(PPh₃)₄] (E = S, Se) with cis-1,4-dichlorobut-2-ene (cis-ClCH₂CHCHCH₂Cl) give the dichalcogenolate complexes [Pt₂(μ-ECH₂CHCHCH₂E)(PPh₃)₄]²⁺; an X-ray structure determination on the thiolate complex was carried out. The complexes give the expected dications in ESI mass spectra recorded at very low cone voltages, but at moderate cone voltages undergo facile fragmentation via a retro-Diels-Alder reaction and loss of 1,3-butadiene, giving the dichalcogenide species [Pt₂(μ-E₂)(PPh₃)₄]²⁺. Analogous species containing bidentate phosphine or arsine ligands have been previously generated electrochemically, and studied theoretically.     

New pyridyl modified phosphines: Synthesis and late transition-metal coordination studies

Using a phosphorus based Mannich condensation reaction the new pyridylphosphines {5-Ph₂PCH₂N(H)}C₅H₃(2-Cl)N (1-Cl) and {2-Ph₂PCH₂N(H)}C₅H₃(5-Br)N (1-Br) have been synthesised in good yields (60% and 88%, respectively) from Ph₂PCH₂OH and the appropriate aminopyridine. The ligands 1-Cl and 1-Br display variable coordination modes depending on the choice of late transition-metal complex used. Hence P-monodentate coordination has been observed for the mononuclear complexes AuCl(1-Cl) (2), AuCl(1-Br) (3), RuCl₂(p-cymene)(1-Cl) (4), RuCl₂(p-cymene)(1-Br) (5), RhCl₂(Cp^∗)(1-Cl) (6), RhCl₂(Cp^∗)(1-Br) (7), IrCl₂(Cp^∗)(1-Cl) (8), IrCl₂(Cp^∗)(1′-Cl) (8′), IrCl₂(Cp^∗)(1-Br) (9), cis-/trans-PdCl₂(1-Cl)₂ (10), cis-/trans-PdCl₂(1-Br)₂ (11), cis-PtCl₂(1-Cl)₂ (12) and cis-PtCl₂(1-Br)₂ (13). Reaction of Pd(Me)Cl(cod) (cod = cycloocta-1,5-diene) with either 1 equiv. of 1-Br or the known pyridylphosphines 1′-Cl, 1-OH or 1-H gave the P/N-chelate complexes Pd(Me)Cl(1-Br-1-H) (14)-(17). All new compounds have been fully characterised by spectroscopic and analytical methods. Furthermore the structures of 4, 5, 10 and 16 · (CH₃)₂SO have been elucidated by single crystal X-ray crystallography. A crystal structure of the dinuclear metallocycle trans,trans-[PdCl₂{μ-P/N-{Ph₂PCH₂N(H)}C₅H₄N}]₂ · CHCl₃, 18 · CHCl₃, has also been determined. Here 1-H bridges, using both P and pyridyl N donors, two dichloropalladium centres affording a 12-membered ring with the PdCl₂ units adopting a head-to-tail arrangement.     

Synthetic and mechanistic studies on ruthenium dicarbonyl complexes containing PhP(CH2CH2CH2PCy2)2 (Cyttp) ligand

A synthetic and mechanistic study is reported on ligand substitution and other reactions of six-coordinate ruthenium(II) carbonyl complexes containing tridentate PhP(CH₂CH₂CH₂PCy₂)₂ (Cyttp). Carbonylation of cis-mer-Ru(OSO₂CF₃)₂(CO)(Cyttp) (1) affords [cis-mer-Ru(OSO₂CF₃)(CO)₂(Cyttp)]O₃SCF₃ (2(O₃SCF₃)) and, on longer reaction times, [cis-mer-Ru(solvent)(CO)₂(Cyttp)](O₃SCF₃)₂ (solvent = acetone, THF, methanol). 2(O₃SCF₃) reacts with each of NaF, LiCl, LiBr, NaI, and LiHBEt₃ to yield [cis-mer-RuX(CO)₂(Cyttp)]⁺ (X = F (3), Cl (4), Br (5), I (6), H (7)), isolated as 3-7(BPh₄). These conversions proceed with high stereospecificity to afford only a single isomer of the product that is assigned a structure in which the Ph group of Cyttp points toward the CO trans to X (anti when X = F, Cl, Br, or I; syn when X = H). Treatment of 2(O₃SCF₃) with NaOMe and CO generates the methoxycarbonyl complex [cis-mer-Ru(CO₂Me)(CO)₂(Cyttp)]⁺ (8), whereas addition of excess n-BuLi to 2(O₃SCF₃) in THF under CO affords mer-Ru(CO)₂(Cyttp) (9). The two ¹³C isotopomers [cis-mer-Ru(OSO₂CF₃)(CO)(¹³CO)(Cyttp)]O₃SCF₃ (2′(O₃SCF₃): ¹³CO trans to P_C; 2″(O₃SCF₃): ¹³CO cis to all P donors) were synthesized by appropriate adaptations of known transformations and used in mechanistic studies of reactions with each of LiHBEt₃, NaOMe/CO, and n-BuLi. Whereas LiHBEt₃ reacts with 2′(O₃SCF₃) and 2″(O₃SCF₃) to replace triflate by hydride without any scrambling of the carbonyl ligands, the corresponding reactions of NaOMe-CO are more complex. The methoxide combines with the CO cis to triflate in 2, and the resultant methoxycarbonyl ligand ends up positioned trans to the incoming CO in 8. A mechanism is proposed for this transformation. Finally, treatment of either 2′(O₃SCF₃) or 2″(O₃SCF₃) with an excess of n-BuLi leads to the formation of the same two ruthenium(0) isomers of mer-Ru(CO)(¹³CO)(Cyttp). These products represent, to our knowledge, the first example of a syn-anti pair of isomers of a five-coordinate metal complex.     

A kinetic study on pyridine exchange reactions at a bis(μ-acetato)(μ-oxo)diruthenium(III) center: effects of monodentate and bidentate N-heterocyclic ligands cis to the oxo bridge

A series of (μ-oxo)bis(μ-acetato)diruthenium(III) complexes containing two pyridine (py) ligands and varied N-heterocyclic ligands in the positions trans and cis to μ-O, respectively, have been prepared to study py/py-d₅ exchange reactions using ¹H NMR spectroscopy. The diruthenium(III) complexes under investigation are [Ru₂(μ-O)(μ-CH₃COO)₂(py)₆](PF₆)₂ (1), [Ru₂(μ-O)(μ-CH₃COO)₂(bpy)₂(py)₂](PF₆)₂ (2), [Ru₂(μ-O)(μ-CH₃COO)₂(acpy)₄(py)₂](FF₆)₂ (3), and [Ru₂(μ-O)(μ-CH₃COO)₂(dmbpy)₂(py)₂](PF₆)₂ (4), where bpy=2,2′-bipyridine, acpy=4-acetylpyridine, and dmbpy=4,4′-dimethyl-2,2′-bipyridine. Pseudo-first order rate constants for the ligand-exchange reactions are 10⁻⁶−10⁻⁵ s⁻¹ for 1-4 in CD₃CN at 298 K. It is found that the rate of the py/py-d₅ exchange reactions is controlled by the electronic nature of the cis-oriented ancillary ligands, while the exchange mechanisms are tuned principally by the ligand steric factors. The activation parameters (ΔH^‡ and ΔS^‡) indicate that exchange reactions proceed through the dissociative (D) or the interchange dissociative (I_d) mechanism for 1 and 3. Negative ΔS^‡ values observed for 2 and 4 suggest a significant contribution of incoming ligands to the exchange pathway. The kinetic and thermodynamic parameters for the diruthenium series and the corresponding data for Ru-based oxo bridged trinuclear complexes established previously are compared and discussed.     

Controlled nitric oxide photo-release from nitro ruthenium complexes: The vasodilator response produced by UV light irradiation

Preliminary pharmacological studies of various nitric oxide (NO) photo-releasing agents are reported based on the flash-photolysis studies of the nitro ruthenium complexes cis-[Ru^II(NO₂)L(bpy)₂]⁺ (bpy = 2,2′-bipyridine and L = pyridine, 4-picoline and pyrazine) and [Ru^II(NO₂)(bpy)(terpy)]⁺ (terpy = terpyridine) in physiological medium. The net photoreactions under these conditions are two primary photoproducts, in (I) there is Ru^II-NO₂ photoaquation, where the photoproducts are Ru^II-H₂O plus and (II) homolytic dissociation of NO from a coordinated nitrito to derive the Ru^II-OH₂ specie and NO. Based on photochemical processes, the nitro ruthenium complexes were incorporated in water in oil (W/O) microemulsion and used in the vasorelaxation induced experiment. Denuded rat aortas were contracted with KCl and nitro ruthenium complexes in microemulsion were added. Perfusion pressures were recorded while arteries were irradiated at 355 nm The time to reach maximum relaxation was longer for [Ru^II(NO₂)(bpy)(terpy)]⁺ complex (ca. 50 min, n = 6) than for cis-[Ru(NO₂)L(bpy)₂]⁺ with L = py and 4-pic complex (ca. 28 min, n = 6) and cis-[Ru(NO₂)(bpy)₂ (pz)]²⁺ complex (ca. 24 min, n = 5).     

Donor-substituted allenylidene(carbonyl)(XR3)chromium complexes (X=P, As, Sb) - synthesis and properties

Photolysis of the allenylidene pentacarbonyl chromium complexes [(CO)₅CrCCC(R¹)R²] (R¹=NMe₂, NPh₂; R²=NMe₂, OMe, Ph) in THF in the presence of equimolar amounts of XR₃ (XR₃=various phosphanes, P(OMe)₃, AsPh₃, SbPh₃) affords cis-allenylidene tetracarbonyl XR₃ complexes, cis-[(CO)₄(XR₃)CrCCC(R¹)R²]. When in the photolysis of [(CO)₅CrCCC(NMe₂)Ph], the phosphanes PR₃ (R=C₆H₄F-p, C₆H₄Cl-p, OMe) are used in excess (three equivalents) two carbonyl ligands are displaced and the mer-tricarbonyl complexes mer-[(CO)₃(PR₃)₂CrCCC(NMe₂)Ph] are formed both PR₃ ligands being mutually trans. The structure of the new complexes is established by IR, NMR, and UV-Vis spectroscopy, that of cis-[(CO)₄(PPh₃)CrCCC(NMe₂)Ph] additionally by an X-ray structural analysis. As indicated by the spectroscopic data of the compounds, these complexes are best described as hybrids of allenylidene and zwitterionic alkynyl complexes with delocalization of the electron pair at nitrogen bonded to the C_γ atom of the allenylidene ligand towards the metal center. The relative contribution of the allenylidene and zwitterionic alkynyl resonance forms is influenced by XR₃. Increasing the donor properties of XR₃ favors the allenylidene resonance form.     

Multinuclear NMR of cis-dicarbonylbis(dithiocarbamato)iron(II) complexes in chloroform solution

The ¹³C and ¹⁵SN NMR spectra of eleven cis-Fe(S₂CNRR′)₂(CO)₂ complexes, where R and R′ are organic substituents, have been measured at ambient temperature in CDCl₃ (0.08–0.16 M). The ¹³C absorptions for the carbonyl ligands correlate well with the force constants for the CO stretching vibrations in CHCl₃ solution. Each of the parameters (¹³CO absorption and k_cis for CO) correlate well with the aqueous solution pK_a for⁺H₂NRR′, corrected for the phenyl-containing substituents, high pK_a values corresponding to high ¹³CO absorptions and low k_cis CO force constants. [p ]Evidence was found in the ¹³C NMR spectra for hindered rotation about the CN bond in S₂CNC₂ in complexes with higher pK_a(corr) values and in the ¹³C spectra of the corresponding thiuram disulfides. [p ]The ¹⁵N (natural abundance) NMR spectra for each of the complexes was determined. Each revealed a single sharp absorption in a region of the ¹⁵N NMR spectrum which indicates substantial CN double bond character, as one would expect for coordinated dithiocarbamate ligands.