Copper(II) cations coordinated with PMDTA (pentamethyldiethylenetriamine) and TMEDA (tetramethylethylenediamine) possess a high synthetic potential. The synthesis of these cations was carried out by metathesis reactions with silver salts. The cationic copper(II) complexes, [Cu(PMDTA)(Me2CO)Cl]+, [Cu(PMDTA)(H2O)Cl]+, [Cu(PMDTA)(DMF)]+, [Cu(PMDTA)Cl]+, [Cu(PMDTA)OAc]+, [Cu(PMDTA)(MeCN)2]2+, [Cu2(TMEDA)2Cl3]+ and [Cu(TMEDA)(MeCN)3]2+ were synthesised as PF6 salts, crystallised and characterised by single-crystal X-ray diffraction. 相似文献
The stability constants of mixed ligand complexes of the type M(Phen)(ACA)+, where M = Cu2+ or Zn2+, Phen = 1,10-phenanthroline and ACA? = propionate, valerate and 2-cyclohexylacetate, were determined by potentiometric pH titration in 50% (v/v) dioxanewater and were compared with the stabilities of the corresponding ternary complexes formed with formate and acetate. The ternary complexes containing the alkanecar?ylates (ACA?) are significantly more stable, due to intramolecular hydrophobic interactions between the alkyl residue of the ACAt¯ligands and the 1,10-phenanthroline molecule. For Zn(Phen)(valerate)+ this intramolecular ligand-ligand interaction was confirmed by1H NMR shift measurements. The formation degree of the intramolecular adducts in the ternary Cu2+ and Zn2+ complexes was calculated and the position of the intramolecular equilibrium between the opened and closed isomer was determined: the closed isomer occurs between about 10 to 35 percent. Comparisons with related data show that the extent of this interaction is about the same in water and in 50% aqueous dioxane; this contrasts with the experience made with simple unbridged adducts, which are destabilized by the addition of dioxane (or other organic solvents). Furthermore, evaluation of the available stability data for the Cu2+/leucinate (Leu?) system shows that addition of some dioxane to an aqueous solution (in which of the closed isomer exists to about 20%) favors the intramolecular interaction between the two isopropyl residues in Cu(Leu)2 considerably: in 40 to 50% aqueous dioxane the formation degree of the closed isomer reaches about 80%. Higher concentrations of the organic solvent destabilize the hydrophobic interaction. The overall stability of Cu(Leu)+ and Cu(Leu)2, as well of Cu(alaninate)+ and Cu(alaninate)2, is governed by the polarity of the solvent while the extent of the intramolecular ligand-ligand interaction is influenced by the hydrophobic properties of the solvent molecules. Based on the stability data it is shown that intramolecular ligandligand interactions are quite a common feature for many binary and ternary amino acid complexes: e.g., M(norvalinate)2, M(phenyl-alaninate)2, M(tyrosinate)2 [M = Co2+, Ni2+, Cu2+, Zn2+] or Cu(tyrptophanate)2 and M(phenylalaninate)(norvalinate) or M(phenylalaninate)(tyrosinate) [M = Co2+, Ni2+, Cu2+]. In addition, evidence is presented that direct M2+-aromatic interactions are of no significance in these amino acid complexes in solution. The relevance of the present results with regard to biological systems is indicated. 相似文献
Two new mixed ligand complexes of copper(II) with N,N,N′,N″,N″-pentamethyldiethylenetriamine and polypyridine ligands have been prepared and characterized by means of spectroscopic, magnetic and single-crystal X-ray diffraction methods. These two complexes are isomorph and isostructure in which the coordination polyhedron about the copper(II) ion is distorted square pyramidal. [Cu(PMDT)(bipy)]2+ and [Cu(PMDT)(phen)]2+ show an absorption wavelength maximum at 625 and 678 nm, respectively, assigned to the d-d transition. Antibacterial, antifungal and superoxide dismutase activities of these complexes have also been measured. It was observed that [Cu(PMDT)(bipy)](ClO4)2 was more effective against P. Pyocyanea and Klebsiella sp. than S. aureus. Similarly, Fusarium sp. was highly susceptible against [Cu(PMDT)(bipy)](ClO4)2 but less susceptible against [Cu(PMDT)(phen)](ClO4)2. 相似文献
Complexes of the formula cis-[Pt(H~N)(L)Cl2], where (H~N) are the protonated diamines including 3-aminoquinuclidine, N-aminopiperidine, piperazine, N-methylpiperazine, 1,1,4-trimethylpiperazine, and N-methyl-1,4-diazabicyclo [2,2,2] octane (N-methyl-dabco) and L = SCN?, NO2?, Br?, and F?, were synthesized from the protonated diamine complexes, [Pt(H~N)Cl3]. The antitumor activities of the complexes were evaluated in vitro against L1210 murine leukemia cells, and ID50 values for the L-substituted complexes were compared to values of the parent complexes. In each case it was found that replacement of a chloride ion by SCN?, NO2?, Br?, or F?, either reduced or completely eliminated antitumor activity. This effect is explained in terms of the trans-directing ability of the ligand, L, compared to chloride. The NO2-substituted complex of 3- aminoquinuclidine was tested in vivo and found to exhibit little or no antitumor activity. 相似文献
The interaction of the Cu(II) drugs CuL(NO3) and CuL′(NO3) (HL is pyridine-2-carbaldehyde thiosemicarbazone and HL′ is pyridine-2-carbaldehyde 4N-methylthiosemicarbazone, in water named [CuL]+ and [CuL′]+) with [poly(dA–dT)]2, [poly(dG–dC)]2, and calf thymus (CT) DNA has been probed in aqueous solution at pH 6.0, I = 0.1 M, and T = 25 °C by absorbance, fluorescence, circular dichroism, and viscosity measurements. The results reveal that these drugs act as groove binders with [poly(dA–dT)]2, with a site size n = 6–7, whereas they act as external binders with [poly(dG–dC)]2 and/or CT-DNA, thus establishing overall electrostatic interaction with n = 1. The binding constants with [CuL′]+ were slightly larger than with [CuL]+. The title compounds display some cleavage activity in the presence of thiols, bringing about the rupture of the DNA strands by the reactive oxygen species formed by reoxidation of Cu(I) to Cu(II); this feature was not observed in the absence of thiols. Mutagenic assays performed both in the presence and in the absence of S9 mix, probed by the Ames test on TA 98, TA 100, and TA 102, were negative. Weak genotoxic activity was detected for [CuL]+ and [CuL′]+, with a significative dose–response effect for [CuL′]+, which was shown to be more cytotoxic in the Ames test and 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide cell proliferation assays. Methylation of the terminal NH2 group enhances the antiproliferative activity of the pyridine-2-carbaldehyde thiosemicarbazones. 相似文献
The stoichiometry and kinetics of the reaction between [Cu(dien)(OH)]+ and [Fe(CN)6]3− in aqueous alkaline medium are described. The rate equation − (d[Fe(III)]/dt = {k1[OH−]2[[Cu(dien)(OH)]+] + k2[OH−] × [[Cu(dien)(OH)]+]2}([Fe(III)]/[Fe(II)]) (Fe(III) = [Fe(CN)6]3−; Fe(II) = [Fe(CN)6]4−, the 4:4:1 OH−/Fe(III)/[Cu(dien)(OH)]+ stoichiometric ratio and the nature of the ultimate products identified in the reaction solution suggest the fast formation of a doubly deprotonated Cu(III)-diamido complex which slowly undergoes an internal redox process where the ligand is oxidised to the Schiff base H2NCH2CH2NCHCHNH.The [[Cu(dien)(OH)]+]2 term in the rate equation is explained with the formation of a transient μ-hydroxo mixed-valence Cu dimer. A two-electron internal reduction of the Cu(III) complex yielding a Cu(I) intermediate is suggested to account for the presence of monovalent copper in a precipitate which forms at relatively high reactant concentrations and in the absence of dioxygen. 相似文献
Three new thiodiacetato-Cu(II) chelates have been synthesized and studied by X-ray crystallography and by thermal, spectral and magnetic methods. [Cu(tda)]n (1) is a 3D-polymer with a pentadentate tda, which acts with a fac-O2 + S(apical)-tridentate chelating conformation and as a twofold anti, syn-μ-η1:η1 carboxylate bridge. In its square pyramidal Cu(II) coordination (type 4 + 1) four O(carboxylate) donors define a close regular square base, but the Cu-S(apical) bond deviates 27.4° from the perpendicular to the mean basal plane. Each anti,syn-bridging carboxylate group exhibits two C-O (average 1.26(1) Å) and two Cu-O bonds (average 1.958(7) Å), which are very similar in length to each other. In contrast, the mixed-ligand complexes of [Cu(tda)(Him)2(H2O)] (compound 2, distorted octahedral, type 4 + 1 + 1) and [Cu(tda)(5Mphen)] · 2H2O (compound 3, distorted square pyramidal, type 4 + 1) have molecular structures and the tda ligand displays only a fac-O2 + S(apical)-tridentate conformation. The Cu-S(apical) bond lengths (2.570(1), 2.623(1) or 2.573(1) Å for 1, 2 or 3, respectively) are shorter than those previously reported for closely related Cu(II)-tda derivatives. The different tda ligand roles in their Cu(II) derivatives are rationalized on the basis of crystal packing forces driving in the absence or presence of auxiliary ligands (with two or three N-donor atoms). 相似文献
We have studied the kinetics of the complex formation of gold(III) complexes, [AuCl2(en)]+ (dichlorido(ethylenediamine)aurate(III)-ion) and [AuCl2(SMC)] (dichlorido (S-methyl-l-cysteine)aurate(III)) with four biologically N-donor nucleophiles. It was shown that studied ligands have a high affinity for gold(III) complex, which may have important biological implications, since the interactions of Au(III) with DNA is thought to be responsible for the anti-tumour activity. The [AuCl2(SMC)] complex is more reactive than [AuCl2(en)]+. L-His reacts faster than the other N-donor nucleophiles in the reaction with [AuCl2(en)]+, but in the reaction with [AuCl2(SMC)] 5′-GMP is the best nucleophile. Gold(III) complexes are much more reactive than Pt(II) complexes with the same nucleophiles. The activation parameters for all studied reactions suggest an associative substitution mechanism. The cytotoxicity of gold(III) complexes, [AuCl2(en)]+, [AuCl2(SMC)] and [AuCl2(DMSO)2]+ was evaluated in vitro against chronic lymphocytic leukemia cells, obtained from blood of patients with chronic lymphocytic leukemia (CLL). The [AuCl2(en)]+ complex show comparable cytotoxicity profiles compared to cisplatin. 相似文献
Reaction of Cu(ClO4)2·6H2O, SRaaiNR′ (1-alkyl-2-[(o-thioalkyl)phenylazo]imidazole) and NH4SCN (1:1:2 mol ratio) affords distorted square pyramidal, [CuII(SRaaiNR′)(SCN)2] (3) compound while identical reaction with [Cu(MeCN)4](ClO4) yields -SCN- bridged coordination polymer, [CuI(SRaaiNR′)(SCN)]n (4). These two redox states [CuII and CuI] are interconvertible; reduction of [CuII(SRaaiNR′)(SCN)2] by ascorbic acid yields [CuI(SRaaiNR′)(SCN)]n while the oxidation of [CuI(SRaaiNR′)(SCN)]n by H2O2 in presence of excess NH4SCN affords [CuII(SRaaiNR′)(SCN)2]. They are structurally confirmed by single crystal X-ray diffraction study. Cyclic voltammogram of the complexes show Cu(II)/Cu(I) redox couple at ∼0.4 V and azo reductions at negative to SCE. UV light irradiation in MeCN solution of [CuI(SRaaiNR′)(SCN)]n (4) show trans-to-cis isomerisation of coordinated azoimidazole. The reverse transformation, cis-to-trans, is very slow with visible light irradiation while the process is thermally accessible. Quantum yields (?t→c) of trans-to-cis isomerisation are calculated and free ligands show higher ? than their Cu(I) complexes. The activation energy (Ea) of cis-to-trans isomerisation is calculated by controlled temperature experiment. Copper(II) complexes, 3, do not show photochromism. DFT and TDDFT calculation of representative complexes have been used to determine the composition and energy of molecular levels and results have been used to explain the solution spectra, photochromism and redox properties of the complexes. 相似文献
A series of silver and copper coordination complexes has been studied using secondary ion mass spectrometry (SIMS). Results are presented for the monomeric silver(I) complexes [Ag(CNR)4]X, where R = cyclohexyl for X ClO4−, and R = methyl or t-butyl for X PF6−. Likewise, Cu(I) complexes [Cu(CNR)4]PF6, where R =methyl, t-butyl, or cyclohexyl, were examined. The presence of AgL2+ (L represents the intact RNC ligand) and the absence of AgL3+ and AgL4+ species attests to the gas phase stability of two-coordinate silver(I). Similar results to these were obtained for the Cu(I) complexes, with the exception of [Cu(CNCH3)4]PF6 whose spectrum contains CuL4+, CuL3+, CuL2+, CuL+, and Cu+ ions. The latter result reflects the enhanced stability of the tetrahedral Cu(I) geometry compared to Ag(I) in the gas phase. Cross labeling experiments and isotopic labeling studies have provided insights into fragmentation mechanisms. Ligand exchange occurs when mixtures are examined. These exchange reactions provide evidence for extensive molecular mixing which can accompany SIMS even under low primary ion dose conditions. Cluster ion formation as well as the observation of α-cleavage of the NC bonds of RNC ligands have been observed and these results are discussed. Granulated graphite and ammonium chloride were employed to study matrix effects. Granulated graphite enhanced NC cleavage for the silver complexes but had little effect on the relative abundance of silver cluster ions. On the other hand, copper cluster ions were more sensitive to matrix effects. 相似文献
Short-chain dehydrogenase/reductase homologues from Escherichia coli (YdfG) and Saccharomyces cerevisiae (YMR226C) show high sequence similarity to serine dehydrogenase from Agrobacterium tumefaciens. We cloned each gene encoding YdfG and YMR226C into E. coli JM109 and purified them to homogeneity from the E. coli clones. YdfG and YMR226C consist of four identical subunits with a molecular mass of 27 and 29 kDa, respectively. Both enzymes require NADP+ as a coenzyme and use l-serine as a substrate. Both enzymes show maximum activity at about pH 8.5 for the oxidation of l-serine. They also catalyze the oxidation of d-serine, l-allo-threonine, d-threonine, 3-hydroxyisobutyrate, and 3-hydroxybutyrate. The kcat/Km values of YdfG for l-serine, d-serine, l-allo-threonine, d-threonine, l-3-hydroxyisobutyrate, and d-3-hydroxyisobutyrate are 105, 29, 199, 109, 67, and 62 M?1 s?1, and those of YMR226C are 116, 110, 14600, 7540, 558, and 151 M?1 s?1, respectively. Thus, YdfG and YMR226C are NADP+-dependent dehydrogenases acting on 3-hydroxy acids with a three- or four-carbon chain, and l-allo-threonine is the best substrate for both enzymes. 相似文献
His-Val-His and His-Val-Gly-Asp are two naturally occurring peptide sequences, present at the active site
of Cu,Zn-superoxide dismutase (Cu,Zn-SOD). We have already studied the interaction of His-Val-His=A
(copper binding site) with Cu(II) and of His-Val-Gly-Asp=B (zinc binding site) with Zn(II). As a
continuation of this work and for comparison purposes we have also studied the interaction of Zn(II) with
His-Val-His and Cu(II) with His-Val-Gly-Asp using both potentiometric and spectroscopic methods (visible,
EPR, NMR). The stoichiometry, stability constants and solution structure of the complexes formed have been
determined. Histamine type of coordination is observed for/ZnAH/2+, /ZnA/+, /ZnA2H/+ and/ZnA2/ in acidic pH while deprotonation of coordinated water molecules is observed at higher pH. /CUB/ species is
characterized by the formation of a macrochelate and histamine type coordination. Its stability results in the
suppression of amide deprotonation which occurs at high pH resulting in the formation of the highly distorted
from square planar geometry 4N complex/CuBH-3/3. 相似文献
α-Amino-acid esters (EH+) interact with [Cu(IMDA)]° to give mixed ligand complexes according to the equilibrium, where EH+ represents the protonated ester +NH3CH(R)CO2R′ and IMDA2? is HN(CH2CO2?)2. The mixed ligand complexes are only formed over a rather narrow pH range (ca. pH 5.8–6.5). At higher pH there is kinetic evidence for the competing equilibrium, Rate constants kOH have been obtained by pH-stat for the hydrolyses [where A? = NH2CH(R)CO2?] The complexed α-amino-acid esters undergo base hydrolysis ca. 104 times faster than the free esters E. Values of kOH show little dependence on the nature of the alkyl substituent R but the normal leaving group effect of methyl esters hydrolyzing at ca. twice the rate of ethyl esters is observed. Activation parameters have been determined for base hydrolysis of [Cu(IMDA)(glyOMe)]°, and possible mechanisms for the reaction are considered. 相似文献
Mixed ligand complexes: [Co(L)(bipy)] · 3H2O (1), [Ni(L)(phen)] · H2O (2), [Cu(L)(phen)] · 3H2O (3) and [Zn(L)(bipy)] · 3H2O (4), where L2− = two -COOH deprotonated dianion of N-(2-benzimidazolyl)methyliminodiacetic acid (H2bzimida, hereafter, H2L), bipy = 2,2′ bipyridine and phen = 1,10-phenanthroline have been isolated and characterized by elemental analysis, spectral and magnetic measurements and thermal studies. Single crystal X-ray diffraction studies show octahedral geometry for 1, 2 and 4 and square pyramidal geometry for 3. Equilibrium studies in aqueous solution (ionic strength I = 10−1 mol dm−3 (NaNO3), at 25 ± 1 °C) using different molar proportions of M(II):H2L:B, where M = Co, Ni, Cu and Zn and B = phen, bipy and en (ethylene diamine), however, provides evidence of formation of mononuclear and binuclear binary and mixed ligand complexes: M(L), M(H−1L)−, M(B)2+, M(L)(B), M(H−1L)(B)−, M2(H−1L)(OH), (B)M(H−1L)M(B)+, where H−1L3− represents two -COOH and the benzimidazole N1-H deprotonated quadridentate (O−, N, O−, N), or, quinquedentate (O−, N, O−, N, N−) function of the coordinated ligand H2L. Binuclear mixed ligand complex formation equilibria: M(L)(B) + M(B)2+ ? (B)M(H−1L)M(B)+ + H+ is favoured with higher π-acidity of the B ligands. For Co(II), Ni(II) and Cu(II), these equilibria are accompanied by blue shift of the electronic absorption maxima of M(II) ions, as a negatively charged bridging benzimidazolate moiety provides stronger ligand field than a neutral one. Solution stability of the mixed ligand complexes are in the expected order: Co(II) < Ni(II) < Cu(II) > Zn(II). The Δ log KM values are less negetive than their statistical values, indicating favoured formation of the mixed ligand complexes over the binary ones. 相似文献
The aim of this work was to investigate the influence of [PdCl4]2 ? , [PdCl(dien)]+ and [PdCl(Me4dien)]+ complexes on Na+/K+-ATPase activity. The dose-dependent inhibition curves were obtained in all cases. IC50 values determined by Hill analysis were 2.25 × 10? 5 M, 1.21 × 10? 4 M and 2.36 × 10? 4 M, respectively. Na+/K+-ATPase exhibited typical Michelis-Menten kinetics in the presence of Pd(II) complexes. Kinetic parameters (Vmax, Km) derived using Eadie–Hofstee transformation indicated a noncompetitive type of Na+/K+-ATPase inhibition. The inhibitor constants (Ki) were determined from Dixon plots. The order of complex affinity for binding with Na+/K+-ATPase, deducted from Ki values, was [PdCl4]2 ? >[PdCl(dien)]+>[PdCl(Me4dien)]+. The results indicated that the potency of Pd(II) complexes to inhibit Na+/K+-ATPase activity depended strongly on ligands of the related compound. Furthermore, the ability of SH-donor ligands, l-cysteine and glutathione, to prevent and recover the Pd(II) complexes-induced inhibition of Na+/K+-ATPase was examined. The addition of 1 mM l-cysteine or glutathione to the reaction mixture before exposure to Pd(II) complexes prevented the inhibition by increasing the IC50 values by one order of magnitude. Moreover, the inhibited enzymatic activity was recovered by addition of SH-donor ligands in a concentration-dependent manner. 相似文献
Potentiometric, visible, and infrared studies of the complexation of N-(2-acetamido)-2-aminoethanesulfonic acid (ACESH) by Ca(II), Mg(II), Mn(II), Co(II), Zn(II), Ni(II), and Cu(II) are reported. Ca(II), Mg(II), and Mn(II) were found not to complex with ACES?, while Co(II), Zn(II), Ni(II), and Cu(II) were found to form 2:1, ACES? to M2+, complexes, and [Cu(ACES)2] was found to undergo stepwise deprotonation of the amide groups to form [Cu(H?1ACES)22?]. Formation (affinity) constants for the various metal complexes are reported, and the probable structures of the various metal chelates in solution are discussed. 相似文献
This report describes synthesis and evaluation of cationic complexes, [99mTc(CO)3(L)]+ (L = N-methoxyethyl-N,N-bis[2-(bis(3-ethoxypropyl)phosphino)ethyl]amine (L1), N-[(15-crown-5)-2-yl]-N,N-bis[2-(bis(3-ethoxypropyl)phosphino)ethyl]amine (L2) and N-[(18-crown-6)-2-yl]-N,N-bis[2-(bis(3-ethoxypropyl)phosphino)ethyl]amine (L3)) as potential radiotracers for heart imaging. Preliminary results from biodistribution studies in female adult BALB-c mice indicated that the cationic 99mTc(I)-tricarbonyl complex, [99mTc(CO)3(L2)]+, has a significant localization in the heart at 60 min post-injection. To understand the coordination chemistry of these bisphosphine ligands with the 99mTc(I)-tricarbonyl core, we prepared [Re(CO)3(L4)]Br (L4: N,N-bis[(2-diphenylphosphino)ethyl]methoxyethylamine) as a model compound. [Re(CO)3(L4)]Br has been characterized by elemental analysis, IR, ESI-MS, NMR (1H, 13C, 1H-1H COSY, and 1H-13C HMQC) methods, and X-ray crystallography. In solid state, [Re(CO)3(L4)]+ has a distorted octahedron coordination geometry with PNP occupying one facial plane. The chelator backbone adopts a “chair” conformation with phosphine-P atoms at equatorial positions and the amine-N at the apical site. In solution, [Re(CO)3(L4)]+ is able to maintain its cationic nature with no dissociation of carbonyl ligands or any of the three PNP donors. 相似文献
Abstract The cytotoxicity of several Co(II), Ni(II), Cu(II) and Zn(II) complexes with various molecular structures and geometries, has been tested on LoVo and 2008 cells at 1–100 μM concentration for 24 h exposure. On the basis of 24 h results, the exposure time was prolonged to 48 and to 72 hours. The most potent complexes result [Cu(tren)(H2O)]2+ 2Cl?, E, [CoCl3(H2Meppz)], G, and [CoCl3(HMe2ppz)], H, (tren=tris(2-aminoethyl)amine, H2Meppz=1-methylpiperazin-1-ium, HMe2ppz=1,4-dimethylpiperazin-1-ium cations). Nevertheless, these complexes are able to induce cell growth reduction of about 50% at highest doses tested (1-100 μM) and after 72 h exposure. 相似文献
The biomimetic dioximatoiron complexes [Fe(Hdmed)]+ and [Fe(H2dmdt)]2+ act as catecholase models but the latter also catalyzes the intradiol cleavage of 3,5-ditert-butylcatechol. This remarkable selectivity was ascribed to the stable, hydrogen-bonded, macrocyclic coordination sphere of [Fe(Hdmed)]+, precluding bidentate catechol binding, as opposed to the less stable, mobile structure of [Fe(H2dmdt)]2+. This hypothesis is supported by the structures of [Fe(Hdmed)]+ and [Fe(H2dmdt)]2+ determined by X-ray diffraction in 1 M methanol solution. This study is a demonstrative example for the capabilities of the X-ray diffraction technique applied for complexes in the solution phase. The characteristic bond lengths of the complex and the number of solvent molecules in the solvation shell have been determined. To examine the structure of the complexes, gas phase density functional geometry optimizations were performed by using the adf-2004.01 and gaussian-98 packages. The PCM methodology was applied to estimate the effect of solvent on the relative energetics of the low-spin and high-spin electronic states of the complexes. The calculations confirmed that the electronic ground state corresponds to the triplet state for both complexes. 相似文献
