Preparation of silver nanoparticles from silver(I) nano-coordination polymer

Nanorods of two-dimensional organometallic coordination polymer, [Ag(μ₄-DPOAc)]_n (1) [DPOAc⁻ = diphenylacetate], has been synthesized by the reaction of potassium diphenylacetate (DPOAcK) and AgNO₃ by sonochemical process. Reaction conditions, such as the concentration of the initial reagents played important roles in the size and growth process of the final product. Silver nanoparticles were synthesized from nanorods of compound 1. These nano-coordination polymer and nanoparticles were characterized by X-ray powder diffraction (XRD) and scanning electron microscopy (SEM). Thermal stability of nano and crystal samples of compound 1 were studied and compared with each other.     

A zigzag chain coordination polymer consisting of silver(I) ion having square planar geometry

Silver(I) complexes of hexakis(tolylsulfanyl)benzene (htsb), [Ag(htsb)](PF₆) (1), have been prepared and their molecular structures were determined by X-ray crystallography. In 1, the silver ion prefers a square planar coordination geometry comprized of four S atoms from two different htsb molecules and producing a zigzag chain structure of AgS in the silver coordination polymer. Based on the thermo-gravimetry analysis results, two tolylsulfanyl groups were easily eliminated at approximately 211 °C. However, [Ag(htsb)(2-butanone)] (PF₆) (2), which were obtained by the reactions in different solvents, showed a different colors and thermal degradation behaviors.     

Macrocyclic dinuclear gold(I) and silver(I) NHCs complexes

The ligands bis-(imidazolium) hexafluorophosphate (Himy = -C₃N₂H₃-, imidazolium; R = 1-naphthylmethylene, 1a; 9-anthracenylmethylene, 1b) with an oxoether chain were easily prepared by the reaction of substituted imidazole with the diglycol diiodide, followed by exchange of anions with . 1a and 1b reacted with Ag₂O in DMSO or CH₃CN to yield [2 + 2] dinuclear Ag(I) NHCs macrocyclic complexes 2a and 2b, which showed much different conformation in solid corresponding to the R- substituent. Carbene transmetalation reactions of 2a-b with Au(SMe₂)Cl give dinuclear Au(I) analogs 3a and 3b. The new NHCs complexes were characterized by elemental analyses, ¹H NMR, ¹³C NMR and the structures of 2a-b and 3a were confirmed by X-ray diffraction determination.     

Interaction of metal ions with polynucleotides and related compounds. X. Studies on the reaction of silver (I) with the nucleosides and polynucleotides, and the effect of silver(I) on the zinc(II) degradation of polynucleotides

Potentiometric titration curves of the silver(I) complexes of cytidine, adenosine, and uridine show little uptake of base below pH 7, unlike the curve for silver(I)-guanosine, which shows extensive base uptake at neutral pH. This observation is correlated with spectrophotometric data showing little difference between the silver complex spectra of adenosine, cytidine, and uridine and the spectra of uncomplexed nucleosides, except at high pH, but showing a great difference between the silver complex spectra of guanosine and inosine and the corresponding uncomplexed nucleosides even at pH 6. Similar comparisons of the silver complexes of poly A, poly C, poly I, and poly U, both by potentiometric titration and by spectrophotometry, show that poly I behaves like guanosine and inosine as expected, differing from poly A and poly C. However, poly U behaves like poly I and thus does not resemble uridine in its complexing behavior. There is thus a dichotomy between poly A and poly C on the one hand in silver complexing phenomena, compared with poly U and poly I on the other. When silver(I) is added to systems containing zinc(II) and various polynucleotides, the same dichotomy is noted. Silver(I) inhibits the degradation by zinc(II) of all four polynucleotides, but the degradation of poly I and poly U is prevented virtually completely. Silver(I) alone has no degradative effect on RNA and inhibits, the zinc(II) degradation of RNA. Polynucleotide complexes in which silver(I) and zinc(II) are simultaneously bound to different positions on the macromolecules are postulated as intermediates in the inhibited degradation reactions.     

Syntheses and characterizations of six hydrogen-bonded silver(I) complexes from assembly of silver(I) nitrate and aminobenzoic acid

Six hydrogen-bonded silver(I) complexes, Ag(4-abaH)₂(NO₃) (1), [Ag(4-abaH)₂(NO₃)]_n (2), {[Ag(4-aba)(4-abaH)] · H₂O}_n (3), {[Ag(4,4^′-bipy)(H₂O)](4-aba)_0.5(NO₃)_0.5 · (H₂O)_0.5}_n (4), [Ag[(3-abaH_0.5)₂] (5), and {[Ag(3-aba)] · H₂O}_n (6) (4-abaH=4-aminobenzoic acid, 3-abaH=3-aminobenzoic acid), have been synthesized and characterized by single-crystal X-ray diffraction analyses. In 1, 4-abaH serves as a monodentate ligand coordinating to Ag(I) through its nitrogen atom, while uncoordinated carboxylic group links (4-abaH)-Ag-(4-abaH) into a one-dimensional metallic carboxylic synthon. 2 may be regarded as an extension of 1 into a two-dimensional carboxylic synthon through NO₃ ⁻ bridging two adjacent Ag(I) centers. In 3, 4-abaH in a monodentate mode and 4-aba in a μ-N,O bridging mode link three-coordinated Ag(I) to form a one-dimensional swallow-like chain, which is further extended into a two-dimensional layer structure through inter-chain hydrogen bonding interactions. The alternating Ag(I) and 4,4^′-bipy in 4 give rise to a slightly distorted linear chain, which is further extended into a two-dimensional layer through the completely overlapping and off-set stacking interactions. The hydrogen bonds involving in weakly coordinated aqueous molecules and 4-aba further extend it into a three-dimensional framework. In 5, the inter-molecular hydrogen bonding and π-π stacking interactions extend Ag[(3-abaH_0.5)₂] into a two-dimensional supramolecular architecture. In 6, 3-aba in a μ₃-N,O,O^′ coordination mode links three three-coordinated Ag(I) into a two-dimensional network. Uncoordinated aqueous molecules and the adjacent 3-aba oxygen atoms form intermolecular hydrogen bonds.     

Mono- and bimetallic gold(I) and silver(I) pentafluoropropionates and related compounds

A series of eight new carboxylate complexes of the general type (L)_nMOC(O)R (L=PMe₃; n=1; M=Ag, Au; R=C₂F₅. L=PPh₃; n=1-3; M=Ag; R=C₂F₅, t-Bu) have been prepared in high yields. Crystal and molecular structures have been determined for three representative examples. The crystal structure of (Ph₃P)AgOC(O)C₂F₅ contains dimers in which the silver atoms are bridged by the carboxylate oxygen atoms. This bridging resembles the structural motif found in silver carboxylates without ligand support. Usage of the smaller phosphine PMe₃ leads to the formation of a polymeric chain structure in (Me₃P)AgOC(O)C₂F₅ with bridging carboxylate anions and short Ag-Ag contacts holding the monomers together. The reaction of (4-Me₂N-C₆H₄)Ph₂ PAuCl with two equivalents of C₂F₅CO₂Ag leads to the formation of a mixed metal product containing both gold and silver. The crystal structure analysis of this compound revealed a tetranuclear complex containing a central dimeric silver pentafluoropropionate unit which is chelated by the (triarylphosphine)gold(I) pentafluoropropionate molecules via Ag-Au metallophilic contacts and Ag-O donor/acceptor interactions.     

Some features of hydrogen (ion) secretion by the frog skin

We have studied the movements of H⁺ from the in vitro frog skin into the outside solution because it has been suggested that the movement of sodium from the outside solution into the skin may result from the forced exchange of Na⁺ by H⁺.Our main observations can be summarized as follows: (a) Hydrogen moves from the skin into the outside solution at a rate of 0.04 μequiv · cm^?2 · h^?1 while Na⁺ influx had a value of 0.49 μequiv · cm^?2 · h^?1. (b) The rate of H⁺ secretion is not significantly affected by substituting the Na⁺ in the outside solution by K⁺ nor by inhibiting Na⁺ influx with amiloride (5 · 10^?5 M). (c) Acetazolamide (5 · 10^?3 M) blocked H⁺ secretion without altering the potential difference across the skin. (d) The rate of H⁺ production is not underestimated because it may have been neutralized by HCO₃^? secreted into the outside solution in exchange for Cl^?. Substituting all the Cl^? by SO₄^2? in the outside solutions does not result in an increase in the rate of H⁺ production. (e) The steady-state rate of H⁺ secretion is not affected by large changes in electrochemical potential gradients for H⁺. Neither abolishing the potential difference across the skin nor a 10-fold change in H⁺ concentration in the outside solution affected significantly the steady-state rate of H⁺ secretion. (f) The H⁺ secretion was abolished by the metabolic inhibitors dinitrophenol (1 · 10^?4 M) and Antimycin A (1.5 · 10^?6 M) which also markedly reduced the potential difference across the skin.Observations (a), (b), and (c) suggest that H⁺ and Na⁺ movements across the outer border of the isolated frog skin are not coupled. The ratio of Na⁺ to H⁺ movements is very different from unity and Na⁺ movements can be abolished without any effects on H⁺ secretion and conversely H⁺ movements can be abolished without interruption of Na⁺ uptake.A second conclusion suggested by these results is that the H⁺ secretion does not result from movement of H⁺ following its electrochemical potential gradient since that rate of secretion is not affected by marked changes in either potential or [H⁺]. Furthermore, the effects of metabolic inhibitors suggest that H⁺ secretion requires the expenditure of energy by the cell.     

Nucleic acid-metal interactions: V. The effect of silver(I) on the structures of A- and B-DNA forms

The interaction of silver(I) with DNA has been studied with uv LD in aqueous solution and in a humid anisotropic poly(vinyl alcohol) host (B-DNA) and also in 80% ethanolic solution (A-DNA). Addition of silver ions has a pronounced effect on the dichroic spectra of DNA, indicating that the DNA structure is significantly altered. By correlation with calculated reduced LD spectra, using intensities and moments of the corresponding electronic transitions of the DNA bases, the experimental spectra of DNA at high silver content may be interpreted in terms of tilt and roll angles of the bases in the double helix. In ethanolic A-DNA solution there is a pronounced decrease in the orientation by flow of DNA, suggesting that the complexation of DNA to silver may be accompanied by the formation of compact tertiary structures.     

Antimicrobial properties of highly fluorinated silver(I) tris(pyrazolyl)borates

Highly fluorinated tris(pyrazolyl)borate ligand [HB(3,5-(CF3)2Pz)3]- has been used in the isolation of air- and light-stable silver complex, [HB(3,5-(CF3)2Pz)3]Ag(OSMe2). It is a monomeric tetrahedral silver complex with an O-bonded dimethylsulfoxide ligand. The silver adduct [HB(3,5-(CF3)2Pz)3]Ag(OSMe2) and the related [HB(3,5-(CF3)2Pz)3] Ag(THF) (where OSMe2 = dimethyl sulfoxide; THF = tetrahydrofuran) show good antibacterial activity, and their antimicrobial efficacy against Staphylococcus aureus is greater than those of AgNO3 and silver sulfadiazine.     

Ligand-dependent aggregation of chicken hemoglobin AI

The hemoglobin A_I component of the white leghorn chicken may potentially provide an animal model for the $\text{in vitro}$ aggregation behavior of human hemoglobin S. In solutions of low ionic strength, it has been found to undergo a striking loss of solubility upon deoxygenation, leading to the formation of macromolecular aggregates. This property is not shared by the other major chicken hemoglobin component, designated A_II. Compositional and NH₂-terminal sequence analysis indicate that extensive primary structural differences reside in the alpha chains of these two hemoglobins. The beta chains appear to be identical. Examination by electron microscopy suggests that the deoxyhemoglobin A_I forms microcrystalline arrays. The A_I component shows diminished reactivity with ¹³CO₂, as judged from ¹³C NMR measurements.     

The effect of pressure on the photochemistry of tris(bipyridyl)chromium(III) ion

The quantum yield for the photoaquation of Cr(bpy)₃³⁺ in basic medium decreases with increasing pressure, with an apparent volume of activation of 3.8 ± 1.0 ml mol⁻¹. From this value and that associated with the phosphorescence lifetime, the volumes of activation for non-radiative decay to the ground state and for formation of photoproduct are derived as −1.6 and +2.9 ml mol⁻¹, respectively. The latter value is consistent with either an associative process with water entering from pockets between the ligands or a dissociative process involving one or both bonds to a bipyridyl ligand.     

Interaction of amino acids with silver(I) ions.

The reactivity of silver(I) ions towards twenty amino acids has been studied in aqueous unbuffered solutions using an ion-selective electrode as a highly sensitive monitor. Contrary to general belief, silver ions are not completely specific for cysteine, but also react with lysine, arginine, methionine and, to a minor extent, cystine. Nevertheless the interaction with all of these species except cysteine is too weak to affect significantly the determination of thiol in proteins by the customary argentometric titration method. The possible origin of errors arising in such titrations is discussed.     

Effect of FS (alpha 2 gamma beta s) hybrid hemoglobin on Hb S nucleation and aggregation

Asymmetrical cross-linked FS (alpha 2 gamma beta s) hybrid hemoglobin (Hb FS-fumarate) was prepared by reacting mixtures of hemoglobins F and S with double-headed aspirin, bis(3,5-dibromosalicyl) fumarate. When the molar ratio of hemoglobin to the cross-linking agent was 1 to 2 in a 1:1 FS mixture, the relative ratio of the products, cross-linked hemoglobins F (Hb F-fumarate), FS (HB FS-fumarate), and S (Hb S-fumarate), was 1.0:2.6:2.0, in contrast to a 1:2:1 ratio of cross-linked hemoglobins A, AS, and S in a 1:1 AS mixture. These results suggest that the fumaryl group reacts differently with Hb F, Hb FS and Hb S, and that the difference could be attributed to the difference in the structure in the vicinity of the EF6 Lys of non alpha-chains. The oxygen-binding properties of Hb F-fumarate, Hb FS-fumarate, and Hb S-fumarate were similar, except that the n-value of Hb F-fumarate was slightly lower than n-values of Hb S-fumarate and Hb FS-fumarate. Kinetic studies on aggregation showed that the addition of Hb FS-fumarate to unmodified Hb S did not affect the delay time prior to aggregation, but did increase the total turbidity. Electrophoretic and densitometric scanning analysis of the aggregate phase of this mixture showed the fraction of Hb FS-fumarate to be 19%. Hb F-fumarate's effect on the delay time is concentration-dependent; the greater the concentration of Hb F-fumarate, the longer the delay time. The turbidity after aggregation of the mixture of Hb S and Hb F-fumarate was much less than that of Hb S and Hb FS-fumarate. However, the fraction of Hb F-fumarate in the aggregate phase was 19%, which is similar to that of Hb FS-fumarate. These data suggest that Hb F and FS hybrid hemoglobin cannot participate in nuclei formation, but can participate in aggregation after sufficient amounts of nuclei are formed from Hb S, and that increased levels of Hb F do not have an inhibitory effect on the formation of nuclei but on the growth of aggregates.     

Peculiar features of kink dynamics in inhomogeneous DNA

A mathematical model was constructed for studies of the peculiar features of the dynamics of local conformational distortions (kinks) in inhomogeneous DNA. General formulas were obtained that determine the dependence of the main dynamic characteristics of kinks: size, energy, energy density and velocity, on DNA composition. Quantitative estimates were made for the characteristics of kinks activated in polynucleotide chains analogous to promoter sequences A₁, A₂, and A₃ of bacteriophage T7.     

Inhibitory effect of copper(II) on zinc(II)-induced aggregation of amyloid beta-peptide

Aggregation of amyloid beta-peptide (Abeta), a key pathological event in Alzheimer's disease, has been shown in vitro to be profoundly promoted by Zn(II). This fact suggests that some factors in the normal brain protect Abeta from the Zn(II)-induced aggregation. We demonstrate for the first time that Cu(II) effectively inhibits the Abeta aggregation by competing with Zn(II) for histidine residues. The Raman spectrum of a metal-Abeta complex in the presence of both Zn(II) and Cu(II) shows that the cross-linking of Abeta through binding of Zn(II) to the N(tau) atom of histidine is prevented by chelation of Cu(II) by the N(pi) atom of histidine and nearby amide nitrogens. The inhibitory effect is strongest at a Cu/Abeta molar ratio of around 4. Above this ratio, Cu(II) itself promotes the Abeta aggregation by binding to the phenolate oxygen of Tyr10. These results emphasize the importance of regulation of Cu(II) levels to inhibit Abeta aggregation, and are consistent with an altered metal homeostasis in Alzheimer's disease.     

Carnivora: the primary structure of the hemoglobin from the silver fox (Vulpes vulpes var., Canidae)

The primary structure determination of the hemoglobin alpha- and beta-chains from the silver fox (Vulpes vulpes var., Canidae) is described. The separation of the chains could be achieved directly from the hemoglobin by RP-HPLC as well as by column chromatography of the globin using carboxymethyl-cellulose. Following tryptic digestion of the chains, the peptides were isolated by RP-HPLC. Amino-acid sequences were determined by Edman degradation in liquid and gas phase sequencers. The peptides could be aligned by homology with human and other Carnivora hemoglobins. Compared to human hemoglobin the alpha- and beta-chains of the silver fox exhibit 24 and 13 amino-acid exchanges, respectively. They differ by one alpha- and two beta-chain replacements from the domestic dog and the coyote. The substitutions affecting contact positions are discussed.     

Synthesis and structural characterization of silver(I), aluminium(III) and cobalt(II) complexes with 4-isopropyltropolone (hinokitiol) showing noteworthy biological activities. Action of silver(I)-oxygen bonding complexes on the antimicrobial activities

Through two unequivalent oxygen donor atoms of the hinokitiol (Hhino; C10H12O2; 4-isopropyltropolone) ligand that showed noteworthy biological activities, the dimeric, silver(I)-oxygen bonding complex [Ag(hino)]2 1, the monomeric aluminium(III) complex [Al(hino)3].0.5H2O 4 and the cobalt(II) complex "[Co(hino)2]2.H2O" 6 were synthesized and characterized with elemental analysis, thermogravimetric and differential thermal analysis (TG/DTA), FTIR and solution (1H and 13C) NMR spectroscopy. The crystal structure of 1 was determined by Rietveld analysis based on X-ray powder diffraction (XPD) data and those of [Al(hino)3].MeOH 4a and [Co(hino)2(EtOH)]2 6a, being obtained as yellow block crystals and red platelet crystals, respectively, by crystallization of 4 and 6, were determined by single-crystal X-ray analysis. The antimicrobial activities of 1, 4 and 6, evaluated with minimum inhibitory concentration (MIC; microg ml(-1)), were compared with those of other metal complexes (M=Na, Li, Cs, Ca, V, Zn) with the hino- ligand. The antimicrobial activities observed in the alkali-metal salts strongly suggested that they were attributed to the effect of the anionic hino- species. The antimicrobial activities of 1 were significantly enhanced, whereas those of other metal complexes were suppressed, compared with those of the neutral Hhino and anionic hino- molecules. The antimicrobial activities observed in 1 were comparable with those of other recently found silver(I)-oxygen bonding complexes, the ligands of which had no activity. Thus, it is proposed that the antimicrobial activities of the silver(I)-oxygen bonding complexes are due to a direct interaction or complexation of the silver(I) ion with biological ligands such as protein, enzyme and membrane, and the coordinating ligands of the silver(I) complexes play the role of a carrier of the silver(I) ion to the biological system.     

Oxygen binding and aggregation of bullfrog hemoglobin

The hemoglobin of the bullfrog, Rana catesbeiana, forms aggregates larger than tetramers in two ways. The first, which results from intermolecular disulfide bonds, can be prevented by treatment with iodoacetamide. The second way results from the association of the deoxygenated forms of the two major components, B and C, to form reversibly an aggregate which is believed to be a trimer, BC2. The sedimentation velocity data show that the stoichiometry of the aggregate cannot be 1:1. The electrophoretic pattern of the deoxygenated B/C mixture suggests that the association is not indefinite. No significant aggregation of the separate deoxygenated tetramers of the components nor of the oxygenated components or mixture occurs. Gel chromatography of the oxygenated forms of components B and C and of mixtures indicates that the B and C tetramers both form dimers upon dilution with a dissociation constant of 2-3 micron. The oxygen-binding data indicate that the B/C aggregate has a much lower oxygen affinity than its constituent tetramers. Dissociation of the low affinity B/C aggregate to higher affinity B and C tetramers with increasing oxygenation gives rise to enhanced cooperativity as measured by the Hill coefficient which is maximal near 75-80% oxygenation and is as high as 4.1 at a heme concentration of 15 mM.     

Apoptosis-inducing ability of silver(I) cyanide-phosphines useful for anti-cancer studies

Metal-based drugs have shown early promise as anticancer agents suggesting the potential application of silver(I) complexes as apoptosis-inducing agents. The ability of a silver(I) cyanide containing phosphine complex to induce cell death was evaluated in both a malignant (SNO esophageal cancer) and non-malignant (HDF-a skin and HEK293 kidney) cell lines. A dose-dependent decrease in cell viability was observed in the SNO cells. Light microscopy revealed morphological features indicative of apoptotic cell death. The mode of cell death was confirmed as apoptosis by phosphatidylserine externalization, DNA fragmentation and nuclear condensation. Furthermore, both the non-malignant cell lines showed morphological features indicative of apoptosis when exposed to complex 1. We propose the use of this silver(I) cyanide phosphine complex as an highly effective positive apoptosis control for use in anticancer studies of phosphine complexes.