Decavanadate-Bearing Guanidine Derivatives Developed as Antimicrobial and Antitumor Species.

To obtain biologically active species, a series of decavanadates (Hpbg)4[H2V10O28]·6H2O (1) (Htbg)4[H2V10O28]·6H2O; (2) (Hgnd)2(Hgnu)4[V10O28]; (3) (Hgnu)6[V10O28]·2H2O; and (4) (pbg = 1-phenyl biguanide, tbg = 1-(o-tolyl)biguanide, gnd = guanidine, and gnu = guanylurea) were synthesized and characterized by several spectroscopic techniques (IR, UV-Vis, and EPR) as well as by single crystal X-ray diffraction. Compound (1) crystallizes in space group P-1 while (3) and (4) adopt the same centrosymmetric space group P21/n. The unusual signal identified by EPR spectroscopy was assigned to a charge-transfer π(O)→d(V) process. Both stability in solution and reactivity towards reactive oxygen species (O2- and OH·) were screened through EPR signal modification. All compounds inhibited the development of Escherichia coli, Pseudomonas aeruginosa, Staphylococcus aureus, and Enterococcus faecalis bacterial strains in a planktonic state at a micromolar level, the most active being compound (3). However, the experiments conducted at a minimal inhibitory concentration (MIC) indicated that the compounds do not disrupt the biofilm produced by these bacterial strains. The cytotoxicity assayed against A375 human melanoma cells and BJ human fibroblasts by testing the viability, lactate dehydrogenase, and nitric oxide levels indicated compound (1) as the most active in tumor cells.

Zinc(II) Carboxylate Coordination Polymers with Versatile Applications.

This review considers the applications of Zn(II) carboxylate-based coordination polymers (Zn-CBCPs), such as sensors, catalysts, species with potential in infections and cancers treatment, as well as storage and drug-carrier materials. The nature of organic luminophores, especially both the rigid carboxylate and the ancillary N-donor bridging ligand, together with the alignment in Zn-CBCPs and their intermolecular interaction modulate the luminescence properties and allow the sensing of a variety of inorganic and organic pollutants. The ability of Zn(II) to act as a good Lewis acid allowed the involvement of Zn-CBCPs either in dye elimination from wastewater through photocatalysis or in pathogenic microorganism or tumor inhibition. In addition, the pores developed inside of the network provided the possibility for some species to store gaseous or liquid molecules, as well as to deliver some drugs for improved treatment.

Insights into Structure and Biological Activity of Copper(II) and Zinc(II) Complexes with Triazolopyrimidine Ligands.

In an attempt to increase the biological activity of the 1,2,4-triazolo[1,5-a]pyrimidine scaffold through complexation with essential metal ions, the complexes trans-[Cu(mptp)2Cl2] (1), [Zn(mptp)Cl2(DMSO)] (2) (mptp: 5-methyl-7-phenyl-1,2,4-triazolo[1,5-a]pyrimidine), [Cu2(dmtp)4Cl4]·2H2O (3) and [Zn(dmtp)2Cl2] (4) (dmtp: 5,7-dimethyl-1,2,4-triazolo[1,5-a]pyrimidine), were synthesized and characterized as new antiproliferative and antimicrobial species. Both complexes (1) and (2) crystallize in the P21/n monoclinic space group, with the tetrahedral surroundings generating a square-planar stereochemistry in the Cu(II) complex and a tetrahedral stereochemistry in the Zn(II) species. The mononuclear units are interconnected in a supramolecular network through π-π interactions between the pyrimidine moiety and the phenyl ring in (1) while supramolecular chains resulting from C-H∙∙∙π interactions were observed in (2). All complexes exhibit an antiproliferative effect against B16 tumor cells and improved antibacterial and antifungal activities compared to the free ligands. Complex (3) displays the best antimicrobial activity against all four tested strains, both in the planktonic and biofilm-embedded states, which can be correlated to its stronger DNA-binding and nuclease-activity traits.

New Cobalt (II) Complexes with Imidazole Derivatives: Antimicrobial Efficiency against Planktonic and Adherent Microbes and In Vitro Cytotoxicity Features.

Three novel Co(II) complexes of the type [Co(C4H5O2)2L2] (where C4H5O2 is methacrylate anion; L = C3H4N2 (imidazole; HIm) (1), C4H6N2 (2-methylimidazole; 2-MeIm) (2), C5H8N2 (2-ethylimidazole; 2-EtIm) (3)) have been synthesized and characterized by elemental analysis, IR and UV-Vis spectroscopic techniques, thermal analysis and single crystal X-ray diffraction. X-ray crystallography revealed for complexes (1) and (2) distorted trigonal bipyramid stereochemistry for Co(II), meanwhile for complex (3) evidenced that the unit cell comprises three molecular units with interesting structural features. In each unit, both stereochemistry adopted by metallic ion and coordination modes of carboxylate anions are different. The screening of antimicrobial activity revealed that Candida albicans planktonic cells were the most susceptible, with minimal inhibitory concentration (MIC) values of 7.8 µg/mL for complexes (1) and (2) and 15.6 µg/mL for complex (3). Complexes (1) and (2) proved to be more active than complex (3) against the tested bacterial strains, both in planktonic and biofilm growth state, with MIC and minimal biofilm eradication concentration (MBEC) values ranging from 15.6 to 62.5 µg/mL, the best antibacterial effects being noticed against Staphylococcus aureus and Pseudomonas aeruginosa. Remarkably, the MBEC values obtained for the four tested bacterial strains were either identical or even lower than the MIC ones. The cytotoxicity assay indicated that the tested complexes affected the cellular cycle of HeLa, HCT-8, and MG63 cells, probably by inhibiting the expression of vimentin and transient receptor potential canonical 1 (TRPC1). The obtained biological results recommend these complexes as potential candidates for the development of novel anti-biofilm agents.

Copper(II) Complexes with Mixed Heterocycle Ligands as Promising Antibacterial and Antitumor Species.

Complexes with mixed ligands [Cu(N-N)2(pmtp)](ClO4)2 ((1) N-N: 2,2'-bipyridine; (2) L: 1,10-phenanthroline and pmpt: 5-phenyl-7-methyl-1,2,4-triazolo[1,5-a]pyrimidine) were synthesized and structurally and biologically characterized. Compound (1) crystallizes into space group Pa and (2) in P-1. Both complexes display an intermediate stereochemistry between the two five-coordinated ones. The biological tests indicated that the two compounds exhibited superoxide scavenging capacity, intercalative DNA properties, and metallonuclease activity. Tests on various cell systems indicated that the two complexes neither interfere with the proliferation of Saccharomyces cerevisiae or BJ healthy skin cells, nor cause hemolysis in the active concentration range. Nevertheless, the compounds showed antibacterial potential, with complex (2) being significantly more active than complex (1) against all tested bacterial strains, both in planktonic and biofilm growth state. Both complexes exhibited a very good activity against B16 melanoma cells, with a higher specificity being displayed by compound (1). Taken together, the results indicate that complexes (1) and (2) have specific biological relevance, with potential for the development of antitumor or antimicrobial drugs.

On the role played by the chirality of ligands on the aggregation of heterometallic CuII -HgII complexes.

Copper(II) complexes constructed from enantiopure Schiff-base ligands derived from o-vanillin and methionine or from their racemic mixture have been employed as metalloligands towards mercury(II) ions. The nature of the heterometallic CuII -HgII complexes (coordination polymers or oligonucler species), resulted from the reactions of the copper(II) complexes with HgCl2 or HgI2 , is different. The enantiopure metalloligands lead to chiral coordination polymers, 1∞ [{Cu(R-/S-valmet)(H2 O)}2 HgCl2 ]·5H2 O·CH3 OH and 2∞ [{Cu2 (R-/S-valmet)2 (µ-H2 O)(H2 O)2 }HgI2 ]·4H2 O. The reaction of the racemic mixture of the metalloligands with HgX2 affords discrete complexes: [{Cu(R,S-valmet)(H2 O)2 }2 HgCl2 ]·2H2 O and [{Cu(R,S-valmet)(H2 O)(CH3 OH)}2 Hg2 I4 ].

Enantiopure versus Racemic Mixture in Reversible, Two-Step, Single-Crystal-to-Single-Crystal Transformations of Copper(II) Complexes.

The reaction of chiral sodium complexes, 1∞ [Na(S-valmetH)]⋅H2 O (1-S) and 1∞ [Na(R-valmetH)]⋅H2 O (1-R), with copper(II) acetate affords chiral one-dimensional coordination polymers with the formulas 1∞ [Cu(S-valmet)(H2 O)]⋅H2 O (2-S) and 1∞ [Cu(R-valmet)(H2 O)]⋅H2 O (2-R) (R/S-valmetH2 are Schiff base proligands resulting from the condensation reactions between o-vanillin and R/S-methionine). The copper ions are connected by the carboxylato groups belonging to the amino-acid moieties, resulting in infinite chains showing syn-anti out-of-plane bridging mode. The circular dichroism spectra of 1-S, 1-R, 2-S, and 2-R confirm their enantiomeric nature. Compounds 2-S and 2-R undergo a two-step single-crystal-to-single-crystal transformation, with the elimination of the lattice and coordinated water molecules: 1∞ [Cu(S-valmet)(H2 O)]⋅H2 O (2-S)→1∞ [Cu(S-valmet)]⋅H2 O (3-S⋅H2 O)→1∞ [Cu(S-valmet)] (3-S) and 1∞ [Cu(R-valmet)(H2 O)]⋅H2 O (2-R)→1∞ [Cu(R-valmet)]⋅H2 O (3-R⋅H2 O)→1∞ [Cu(R-valmet)] (3-R), respectively. During these transformations, every pair of face-to-face chains present in 2-S (or 2-R) has been "zipped up" into a chiral double chain through the removal of the aqua ligands and their replacement by the carboxylato oxygen atoms from the neighboring chain. Consequently, each carboxylato group now bridges three copper ions. The conversion of the single chains, 2-S and 2-R, into the double chains, 3-S and 3-R, is accompanied by a change of the strength of the exchange interactions between the copper ions: weak antiferromagnetic couplings are observed in compound 2-S (J/kB =-1.23(5) K, H=-2J ΣSi Si+1 ) and relatively strong in compound 3-S (J/kB =-76.0(8) K). When the racemic mixture of the ligands, R,S-valmetH2 , is employed, in the same experimental conditions, a racemic mixture of mononuclear compounds, [Cu(R,S-valmet)(H2 O)2 ]⋅H2 O (4-RS), is obtained. Compound 4-RS also undergoes a SCSC transformation with the elimination of the lattice and one of the coordinated water molecules, resulting in a racemic mixture of chiral chains, 1∞ [Cu(R-valmet)(H2 O)]⋅1∞ [Cu(S-valmet)(H2 O)] (5-RS). In this compound, the coupling of the copper(II) ions within the chains is weak and ferromagnetic (J/kB =+0.10(2) K). These results prove that the chirality of the valmetH2 ligands (optically pure or racemic mixture) plays a key role in the self-assembly process of the copper(II) complexes.

Synthesis, Structural Characterization, Antimicrobial Activity, and In Vitro Biocompatibility of New Unsaturated Carboxylate Complexes with 2,2'-Bipyridine.

The synthesis, structural characterization, cytotoxicity, and antimicrobial properties of four new complexes formed by employing acrylate anion and 2,2'-bipyridine are reported herein. X-ray crystallography revealed the trinuclear nature of [Mn3(2,2'-bipy)2(C3H3O2)6] (1), meanwhile complexes with general formula [M(2,2'-bipy)(C3H3O2)2(H2O)x]∙yH2O ((2) M: Ni, x = 1, y = 0; (3) M: Cu, x = 1, y = 0; (4) M: Zn, x = 0, y = 1; 2,2'-bipy: 2,2'-bipyridine; C3H3O2: acrylate anion) were shown to be mononuclear. The lowest minimum inhibitory concentration (MIC) of 128 µg mL-1 was recorded for all four tested complexes against Candida albicans, for complex (3) against Escherichia coli, and for complex (4) against Staphylocococcus aureus. Compounds (3) and (4) were also potent efflux pumps activity inhibitors (EPI), proving their potential for use in synergistic combinations with antibiotics. Complexes (1)-(4) revealed that they were not cytotoxic to HCT-8 cells. They also proved to interfere with the cellular cycle of tumour HCT-8 cells by increasing the number of cells found in the S and G2/M phases. Taken together, these results demonstrate the potential of zinc and copper complexes for use in the development of novel antimicrobial and anti-proliferative agents.

Cobalt(II) Ions Connecting [CoII4] Helicates into a 2-D Coordination Polymer Showing Slow Relaxation of the Magnetization.

The reactions of cobalt(II) perchlorate with a diazine tetratopic helicand, H4L, in the presence of sodium carbonate afford two coordination polymers constructed from tetranuclear anionic helicates as building blocks: ∞3[Co4L3Na4(H2O)4]·4H2O (1) and ∞2[Co5L3Na2(H2O)9]·2.7H2O·DMF (2). The tetranuclear triple-stranded helicates, {CoII4L3}4-, are connected in 1 by sodium(I) ions and in 2 by sodium(I) and cobalt(II) ions (H4L results from the condensation reaction between 3-formylsalicylic acid and hydrazine). The crystal structures of the two compounds have been solved. In both compounds the anionic helicates interact with the assembling cations through the carboxylato oxygen atoms. Compound 2 features chains resulting from connecting the tetranuclear helicates through cobalt(II) ions. The analysis of the magnetic properties of compounds 1 and 2 evidenced a dominant antiferromagnetic coupling for 1, resulting in a diamagnetic ground state. In contrast, the magnetic behavior of 2 is dominated at low temperature by the CoII ion which connects the antiferromagnetically coupled {CoII4} helical moieties. The ac magnetic measurements for 2 reveal the occurrence of slow relaxation of the magnetization that is due to the single, uncorrelated cobalt(II) ions, which are diluted in an essentially diamagnetic matrix of {CoII4} moieties (ΔEeff = 26.7 ± 0.3 cm-1 with τ0 = (2.3 ± 0.2) × 10-6 s).

[Ru(III)(valen)(CN)2](-): a New Building Block To Design 4d-4f Heterometallic Complexes.

New 4d-4f heterometallic complexes with a one-dimensional structure, (1)∞[{Ru(valen)(CN)2KRu(valen)(CN)2}{Ln(O2NO)2(CH3OH)3}]·2CH3OH (Ln = Gd, Tb, Dy), have been assembled from the reaction of [K(H2O)2Ru(III)(valen)(CN)2]·H2O with lanthanide nitrates. The exchange interaction between Ru(III) and Gd(III) mediated by the cyanido ligand was determined for the first time and found to be weak and of antiferromagnetic nature.

Cyanomethylene-bis(phosphonate)-based lanthanide complexes: structural, photophysical, and magnetic investigations.

The syntheses, structural investigations, magnetic and photophysical properties of a series of 10 lanthanide mononuclear complexes, containing the heteroditopic ligand cyanomethylene-bis(5,5-dimethyl-2-oxo-1,3,2λ(5)-dioxa-phosphorinane) (L), are described. The crystallographic analyses indicate two structural types: in the first one, [Ln(III)(L)3(H2O)2]·H2O (Ln = La, Pr, Nd), the metal ions are eight-coordinated within a square antiprism geometry, while the second one, [Ln(III)(L)3(H2O)]·8H2O (Ln = Sm, Eu, Gd, Tb, Dy, Ho, Er), contains seven-coordinated Ln(III) ions within distorted monocapped trigonal prisms. Intermolecular hydrogen bonding between nitrogen atoms of the cyano groups, crystallization, and coordination water molecules leads to the formation of extended supramolecular networks. Solid-state photophysical investigations demonstrate that Eu(III) and Tb(III) complexes possess intense luminescence with relatively long excited-state lifetimes of 530 and 1370 µs, respectively, while Pr(III), Dy(III), and Ho(III) complexes have weak intensity luminescence characterized by short lifetimes ranging between a few nanoseconds to microseconds. The magnetic properties for Pr(III), Gd(III), Tb(III), Dy(III), and Ho(III) complexes are in agreement with isolated Ln(III) ions in the solid state, as suggested by the single-crystal X-ray analyses. Alternating current (ac) susceptibility measurements up to 10 kHz reveal that only the Ho(III) complex shows a frequency-dependent ac response, with a relaxation mode clearly observed at 1.85 K around 4500 Hz.

Magnetic and luminescent binuclear double-stranded helicates.

Three new binuclear helicates, [M2L2]·3DMF (M = Co(II), 1, Zn(II), 3) and [Cu2L2]·DMF·0.4H2O (2), have been assembled using the helicand H2L that results from the 2:1 condensation reaction between o-vanillin and 4,4'-diaminodiphenyl ether. The metal ions within the binuclear helicates are tetracoordinated with a distorted tetrahedral geometry. Direct current magnetic characterization and EPR spectroscopy of the Co(II) derivative point to an easy axis type anisotropy for both Co(II) centers, with a separation of at least 55 K between the two doublets. Dynamic susceptibility measurements evidence slow relaxation of the magnetization in an applied dc field. Since the distance between the cobalt ions is quite large (11.59 Å), this is attributed in a first instance to the intrinsic properties of each Co(II) center (single-ion magnet behavior). However, the temperature dependence of the relaxation rate and the absence of slow dynamics in the Zn(II)-doped sample suggest that neither the simple Orbach mechanism nor Raman or direct processes can account for the relaxation, and collective phenomena have to be invoked for the observed behavior. Finally, due to the rigidization of the two organic ligands upon coordination, the pure zinc derivative exhibits fluorescence emission in solution, which was analyzed in terms of fluorescence quantum yields and lifetimes.

New families of hetero-tri-spin 2p-3d-4f complexes: synthesis, crystal structures, and magnetic properties.

In this work we report the synthesis, crystal structures, and magnetic behavior of 2p-3d-4f heterospin systems containing the nitroxide radical 4-azido-2,2,6,6-tetramethylpiperidine-1-oxyl radical (N3tempo). These compounds were synthesized through a one-pot reaction by using [Cu(hfac)2], [Ln(hfac)3] (hfac = hexafluoroacetylacetonate, Ln = Dy(III), Tb(III) or Gd(III)), and the N3tempo radical. Depending on the stoichiometric ratio used, the synthesis leads to penta- or trimetallic compounds, with molecular formulas [Cu3Ln2(hfac)8(OH)4(N3tempo)] (Ln = Gd, Tb, Dy) and [CuLn2(hfac)8(N3tempo)2(H2O)2] (Ln = Gd, Dy). The magnetic properties of all compounds were investigated by direct current (dc) and alternating current (ac) measurements. The ac magnetic susceptibility measurements of Tb(III)- and Dy(III)-containing compounds of both families revealed slow relaxation of the magnetization, with magnetic quantum tunneling in zero field.

Unexpected formation of N-(1-(2-aryl-hydrazono)isoindolin-2-yl)benzamides and their conversion into 1,2-(bis-1,3,4-oxadiazol-2-yl)benzenes.

Reaction between ortho-phthalaldehyde and various aroylhydrazines unexpectedly yields N-(1-(2-aryl-hydrazono)isoindolin-2-yl)benzamides as major products along with the predictable 1,2-bis-aroylhydrazones. NMR investigation of the major reaction products indicate the presence of a mixture of geometrical isomers, in various ratios. Single crystal X-ray diffraction confirms the proposed structure and indicates a Z configuration of the C═N double bond substitutents. Optimization of the condensation reaction conditions enabled quantitative isolation of the cyclic isomer. Oxidation of the isomers with bis(trifluoroacetoxy)iodobenzene (PIFA) leads to rapid formation of new highly fluorescent 1,2-bis(5-aryl-1,3,4-oxadiazol-2-yl)benzenes.

Enantiomeric pairs of copper(II) complexes with tridentate Schiff bases derived from R- and S-methionine: the role of decorating organic groups of the ligand in crystal packing and biological activity.

Three enantiomeric pairs consisting of copper(II) complexes with tridentate Schiff bases have been synthesized for employing in biological assessments: 1∞[Cu2(R/S-salmet)2(H2O)] (1-R/S·H2O), 1∞[Cu(R/S-3-HOMe-5-Me-salmet)] (2-R/S), and 1∞[Cu(R/S-3-MeO-salmet)] (3-R/S) (where R/S-salmetH2, R/S-3-HOMe-5-Me-salmetH2, and R/S-3-MeO-salmetH2 result from the condensation of R/S-methionine with salicylaldehyde, 2-hydroxy-3-(hydroxymethyl)-5-methylbenzaldehyde, and 3-methoxy-salicylaldehyde, respectively, in a 1 : 1 molar ratio). The crystal structures of 1-R·H2O and 2-R/S are reported. Moreover, the 1-R/S·H2O enantiomers have been subjected to a single-crystal-to-single-crystal (SC-SC) transformation by heating at 160 °C to afford their dehydrated forms, 1∞[Cu2(R/S-salmet)2] (1-R/S), whose structures have also been crystallographically determined. The coordination polyhedra of the metal centers, the binding modes of the ligands, and the 1-D double chain assemblies generated by the chiral mononuclear units are comparatively described. The diffuse reflectance UV-Vis and circular dichroism (CD) spectra of compounds 1-R/S·H2O, 1-R/S, and 2-R/S are analysed with respect to their structural peculiarities and compared to those of 3-R/S. The UV-Vis and CD spectra of solutions of 1-R/S, 2-R/S, and 3-R/S point to the collapse of the double chains via dissolution. Biological tests performed on the model eukaryote Saccharomyces cerevisiae indicated low toxicity for 1-R/S, 2-R/S, and 3-R, and moderate toxicity for 3-S. The S-type complexes were accumulated by cells in higher quantity compared to their R-type counterparts due to selective transport via the high-affinity S-methionine transporter, Mup1. A chemogenomic analysis of 3-S toxicity performed on a collection of yeast knockout mutants revealed that most of the deleted genes identified in the screen were involved in the cell response to oxidative stress, calcium-mediated response, or metal homeostasis. Altogether, it was concluded that 3-S accumulation may perturb the redox state of the cell, also interfering with the calcium-mediated response to oxidative stress or metal-related oxidative stress.

Antiproliferative Copper(II) Complexes Bearing Mixed Chelating Ligands: Structural Characterization, ROS Scavenging, In Silico Studies, and Anti-Melanoma Activity.

Melanoma is a skin cancer characterized by rapid growth and spread for which current therapies produce both resistance and increased risk of infection. To develop new anti-melanoma biocompatible species, the series of complexes Cu(N-N)(bzac)(X)⋅nH2O (N-N: 1,10-phenanthroline/2,2'-bipyridine, Hbzac: 1-phenyl-1,3-butanedione, X: NO3/ClO4, and n = 0, 1) was studied. Single-crystal X-ray diffraction revealed a mononuclear structure for all complexes. The ability of the complexes to scavenge or trap reactive oxygen species such as O2⋅- and HO⋅ was proved by EPR spectroscopy experiments. All complexes inhibited B16 murine melanoma cells in a dose-dependent and nanomolar range, but the complexes with 1,10-phenanthroline were more active. Moreover, comparative activity on B16 and healthy BJ cells revealed a therapeutic index of 1.27-2.24. Bioinformatic methods were used to calculate the drug-likeness, pharmacokinetic, pharmacogenomic, and pharmacodynamic profiles of the compounds. The results showed that all compounds exhibit drug-likeness features, as well as promising absorption, distribution, metabolism, and excretion (ADME) properties, and no toxicity. The pharmacodynamics results showed that the neutral species appear to be good candidates for antitumor molecular targets (Tyrosyl-DNA phosphodiesterase 1, DNA-(apurinic or apyrimidinic site) lyase or Kruppel-like factor 5). Furthermore, the pharmacogenomic results showed a good affinity of the copper(II) complexes for the human cytochrome. These results recommend complexes bearing 1,10-phenanthroline as good candidates for developing drugs to melanoma alternative treatment.

Luminescence thermometry based on one-dimensional benzoato-bridged coordination polymers containing lanthanide ions.

Three 1D coordination polymers with benzoate bridges have been assembled in the presence of 18-crown-6-ether (18C6): 1∞[Tb(PhCOO)3(H2O)(EtOH)]·0.5(18C6) 1, 1∞[Eu(PhCOO)3(H2O)2]·0.5(18C6) 2, 1∞[Nd(PhCOO)3(H2O)2]·0.5(18C6) 3. Compounds 2 and 3 are isomorphous. The crown ether molecules co-crystallize with the resulting 1D coordination polymers and play an important role in the supramolecular architecture of the crystals. A molecular alloy was prepared in a similar way to compound 1 using TbCl3·6H2O and EuCl3·6H2O in a molar ratio of 95 : 5. The EuIII ions have statistically substituted the TbIII ions in the host lattice The luminescence thermometry performance of the Tb0.95Eu0.05 system was investigated using pulsed excitation into TbIII absorption at 352 nm. The maximum Sr value is 1.88% K-1 at 80 K which is slightly reduced at 1.60% K-1 at 313 K. Time-gated emission spectroscopy, employed here for the first time, allows us to reduce the spectral overlap of Tb and Eu emissions in the 610 to 625 nm range by 100% at 80 K, from 18 to 9%. Compound 1 as well as the molecular alloy, Tb0.95Eu0.05, show X-ray induced luminescence.

Synthesis, Characterization, and In Vitro Insulin-Mimetic Activity Evaluation of Valine Schiff Base Coordination Compounds of Oxidovanadium(V).

Type 2 diabetes became an alarming global health issue since the existing drugs do not prevent its progression. Herein, we aimed to synthesize and characterize a family of oxidovanadium(V) complexes with Schiff base ligands derived from L-/D-valine (val) and salicylaldehyde (sal) or o-vanillin (van) as insulin-mimetic agents and to assess their potential anti-diabetic properties. Two new oxidovanadium(V) complexes, [{VVO(R-salval)(H2O)}(µ2-O){VVO(R-salval)}] and [{VVO(R-vanval)(CH3OH)}2(µ2-O)], and their S-enantiomers were synthesized and characterized. The compounds exhibit optical activity as shown by crystallographic and spectroscopic data. The stability, the capacity to bind bovine serum albumin (BSA), the cytotoxicity against human hepatoma cell line, as well as the potential anti-diabetic activity of the four compounds are investigated. The synthesized compounds are stable for up to three hours in physiological conditions and exhibit a high capacity of binding to BSA. Furthermore, the synthesized compounds display cytocompatibility at biologically relevant concentrations, exert anti-diabetic potential and insulin-mimetic activities by inhibiting the α-amylase and protein tyrosine phosphatase activity, and a long-term increase of insulin receptor phosphorylation compared to the insulin hormone. Thus, the in vitro anti-diabetic potential and insulin-mimetic properties of the newly synthesized oxidovanadium(V) compounds, correlated with their cytocompatibility, make them promising candidates for further investigation as anti-diabetic drugs.

Anti-biofilm Fe3O4@C18-[1,3,4]thiadiazolo[3,2-a]pyrimidin-4-ium-2-thiolate Derivative Core-shell Nanocoatings.

The derivatives 5,7-dimethyl[1,3,4]thiadiazolo[3,2-a]pyrimidin-4-ium-2-thiolate (1) and 7-methyl-5-phenyl[1,3,4]thiadiazolo[3,2-a]pyrimidin-4-ium-2-thiolate (2) were fully characterized by single-crystal X-ray diffraction. Their supramolecular structure is built through both π-π stacking and C=S-π interactions for both compounds. The embedment of the tested compounds into Fe3O4@C18 core-shell nanocoatings increased the protection degree against Candida albicans biofilms on the catheter surface, suggesting that these bioactive nanocoatings could be further developed as non-cytotoxic strategies for fighting biofilm-associated fungal infections.

Constructing robust channel structures by packing metallacalixarenes: reversible single-crystal-to-single-crystal dehydration.

The self-assembly process involving the dianion of trimesic acid (Htrim(2-)) and {Cu(tmen)}(2+) templating cations (tmen = N,N,N',N'-tetramethylethylenediamine) affords a new metallacalixarene, [Cu(4)(tmen)(4)(Htrim)(4)] x n H(2)O. The packing of the cyclic molecules in the crystal generates channels that are filled by water molecules. The dehydration-rehydration process of the crystals was found to be reversible.