Assembly of diverse structural types of organotellurium compounds in the reactions of (4-MeO-C6H4)2TeO with pyridine carboxylic acids

The reactions of Ar₂TeO (Ar = 4-MeO-C₆H₄) with 2-, 3- and 4-pyridine carboxylic acids (LH) afforded different organotelluroxane structural types depending on the stoichiometry of the reactants and the conditions of the reaction. Ar₂Te(L)OH (1a-1c) are formed in a 1:1 reaction of Ar₂TeO with LH in the presence of water. On the other hand a 1:2 reaction under anhydrous conditions leads to the formation of Ar₂TeL₂ (2a-2c). A 2:2 reaction under anhydrous conditions affords the ditelluroxanes Ar₂Te(L)OTe(L)Ar₂ (3a-3c) while tritelluroxanes Ar₂Te(L)OTeAr₂OTe(L)Ar₂ (4a-4c) are formed in 3:2 reactions. Interestingly, 3a-3c are formed in the reaction of 2a-2c with Ar₂TeO. The former can be hydrolyzed to 1a-1c while the latter upon reaction with Ar₂TeO lead to the formation of the tritelluroxanes 4a-4c. Attempts to metalate 2a with PdCl₂(MeCN)₂ leads to a transfer of the carboxylate ligand to palladium affording Ar₂TeCl₂ and PdL₂. X-ray crystal structures of representative examples of the family of 1, 2 and 3 reveal interesting supramolecular structures and the formation of a novel [TeO]₂ structural unit. The latter results from intermolecular secondary Te?O interactions.     

6-[3-(4-Fluorophenyl)-1H-pyrazol-4-yl]-3-[(2-naphthyloxy)methyl][1,2,4]triazolo[3,4-b][1,3,4]thiadiazole as a potent antioxidant and an anticancer agent induces growth inhibition followed by apoptosis in HepG2 cells

In this paper we have investigated the in vitro antioxidant property of two triazolo-thiadiazoles, 6-[3-(4-fluorophenyl)-1H-pyrazol-4-yl]-3-[(2-naphthyloxy)methyl][1,2,4]triazolo[3,4-b][1,3,4]thiadiazole (FPNT) and 6-[3-(4-chlororophenyl)-1H-pyrazol-4-yl]-3-[(phenyloxy)methyl][1,2,4]triazolo[3,4-b][1,3,4]thiadiazole (CPPT) by spectrophotometric DPPH and ABTS radical scavenging methods as well as by lipid peroxide assay. The anticancer activity along with possible mechanism of action of triazolo-thiadiazoles in Hep G2 cells was explored using MTT assay, [³H] thymidine assay, flow cytometry and chromatin condensation studies. Both FPNT and CPPT exhibited a dose dependent cytotoxic effect on hepatocellular carcinoma cell line, HepG2. The IC₅₀ value was very low for both the compounds when compared to standard drug, doxorubicin. Incorporation of [³H] thymidine in conjunction with cell cycle analysis suggested that FPNT inhibited the growth of HepG2 cells. Flow cytometric studies revealed more percentage of cells in sub-G1 phase, indicating apoptosis, which was further confirmed through chromatin condensation studies by Hoechst staining. FPNT was found to be a potent antioxidant when compared to the standard in DPPH, ABTS radical scavenging assays and lipid peroxidation studies.     

Structural Feature Ions for Distinguishing N- and O-Linked Glycan Isomers by LC-ESI-IT MS/MS

Glycomics is the comprehensive study of glycan expression in an organism, cell, or tissue that relies on effective analytical technologies to understand glycan structure–function relationships. Owing to the macro- and micro-heterogeneity of oligosaccharides, detailed structure characterization has required an orthogonal approach, such as a combination of specific exoglycosidase digestions, LC-MS/MS, and the development of bioinformatic resources to comprehensively profile a complex biological sample. Liquid chromatography-electrospray ionization-mass spectrometry (LC-ESI-MS/MS) has emerged as a key tool in the structural analysis of oligosaccharides because of its high sensitivity, resolution, and robustness. Here, we present a strategy that uses LC-ESI-MS/MS to characterize over 200 N- and O-glycans from human saliva glycoproteins, complemented by sequential exoglycosidase treatment, to further verify the annotated glycan structures. Fragment-specific substructure diagnostic ions were collated from an extensive screen of the literature available on the detailed structural characterization of oligosaccharides and, together with other specific glycan structure feature ions derived from cross-ring and glycosidic-linkage fragmentation, were used to characterize the glycans and differentiate isomers. The availability of such annotated mass spectrometric fragmentation spectral libraries of glycan structures, together with such substructure diagnostic ions, will be key inputs for the future development of the automated elucidation of oligosaccharide structures from MS/MS data.

Stereoselective synthesis of (-)-1-epi-ventiloquinone L and (+)-ventiloquinone L, the monomeric unit of cardinalin 3

A stereoselective synthesis of (-)-1-epi-ventiloquinone L and (+)-ventiloquinone L, the monomeric unit of cardinalin 3 has been described. The synthesis is completed in 7 steps with 10.5% and 13% overall yields for (-)-1-epi-ventiloquinone L and (+)-ventiloquinone L respectively. The key steps involve D?tz benzannulation of carbene 5 with alkyne 6 to give a substituted naphthalene moiety and oxa-Pictet-Spengler reaction to install the 1,3-dimethylpyran moiety.     

Study of size-dependent glass transition and Kauzmann temperatures of tin dioxide nanoparticles

The size and shape effects on melting, glass transition, and Kauzmann temperatures of SnO₂ nanoparticles using Lindemann??s criterion have been studied. The melting temperature of SnO₂ nanoparticles decreases as the size of the particle decreases. As the particle size increases, melting temperature increases and approaches to the melting temperature 1,903?K of bulk irrespective of the shape. The glass transition and Kauzmann temperatures are analyzed through the size effect on the melting temperature. The glass transition and Kauzmann temperatures decrease with the decrease in size of SnO₂ nanoparticles.     

Laser Raman and conductivity studies of plasticized polymer electrolyte P(ECH-EO):propylenecarbonate:<Emphasis Type="Italic">γ</Emphasis>-butyrolactone:LiClO<Subscript>4</Subscript>

The plasticized polymer electrolytes composed of poly(epichlorohydrin-ethyleneoxide) (P(ECH-EO)) as host polymer, lithium perchlorate (LiClO₄) as salt, γ-butyrolactone (γ-BL), and propylene carbonate (PC) as plasticizer have been prepared by simple solution casting technique. The effect of mixture of plasticizers γ-BL and PC on conductivity of the polymer electrolyte P(ECH-EO):LiClO₄ has been studied. The band at 457 cm⁻¹ in the Raman spectra of plasticized polymer electrolyte is attributed to both the ring twisting mode of PC and the perchlorate ν ₂(ClO₄⁻) bending. The maximum conductivity value is observed to be 4.5 × 10⁻⁴ S cm⁻¹ at 303 K for 60P(ECH-EO):15PC:10γ-BL:15LiClO₄ electrolyte system. In the present investigation, an attempt has been made to correlate the Raman and conductivity data.     

Three-component self-assembly of a series of triply interlocked Pd12 coordination prisms and their non-interlocked Pd6 analogues

Template-assisted formation of multicomponent Pd(6) coordination prisms and formation of their self-templated triply interlocked Pd(12) analogues in the absence of an external template have been established in a single step through Pd-N/Pd-O coordination. Treatment of cis-[Pd(en)(NO(3))(2)] with K(3) tma and linear pillar 4,4'-bpy (en=ethylenediamine, H(3) tma=benzene-1,3,5-tricarboxylic acid, 4,4'-bpy=4,4'-bipyridine) gave intercalated coordination cage [{Pd(en)}(6)(bpy)(3)(tma)(2)](2)[NO(3)](12) (1) exclusively, whereas the same reaction in the presence of H(3) tma as an aromatic guest gave a H(3) tma-encapsulating non-interlocked discrete Pd(6) molecular prism [{Pd(en)}(6)(bpy)(3)(tma)(2)(H(3)tma)(2)][NO(3)](6) (2). Though the same reaction using cis-[Pd(NO(3))(2)(pn)] (pn=propane-1,2-diamine) instead of cis-[Pd(en)(NO(3))(2)] gave triply interlocked coordination cage [{Pd(pn)}(6)(bpy)(3)(tma)(2)](2)[NO(3)](12) (3) along with non-interlocked Pd(6) analogue [{Pd(pn)}(6)(bpy)(3) (tma)(2)](NO(3))(6) (3'), and the presence of H(3) tma as a guest gave H(3) tma-encapsulating molecular prism [{Pd(pn)}(6)(bpy)(3)(tma)(2)(H(3) tma)(2)][NO(3)](6) (4) exclusively. In solution, the amount of 3' decreases as the temperature is decreased, and in the solid state 3 is the sole product. Notably, an analogous reaction using the relatively short pillar pz (pz=pyrazine) instead of 4,4'-bpy gave triply interlocked coordination cage [{Pd(pn)}(6) (pz)(3)(tma)(2)](2)[NO(3)](12) (5) as the single product. Interestingly, the same reaction using slightly more bulky cis-[Pd(NO(3))(2)(tmen)] (tmen=N,N,N',N'-tetramethylethylene diamine) instead of cis-[Pd(NO(3))(2)(pn)] gave non-interlocked [{Pd(tmen)}(6)(pz)(3)(tma)(2)][NO(3)](6) (6) exclusively. Complexes 1, 3, and 5 represent the first examples of template-free triply interlocked molecular prisms obtained through multicomponent self-assembly. Formation of the complexes was supported by IR and multinuclear NMR ((1)H and (13)C) spectroscopy. Formation of guest-encapsulating complexes (2 and 4) was confirmed by 2D DOSY and ROESY NMR spectroscopic analyses, whereas for complexes 1, 3, 5, and 6 single-crystal X-ray diffraction techniques unambiguously confirmed their formation. The gross geometries of H(3) tma-encapsulating complexes 2 and 4 were obtained by universal force field (UFF) simulations.     

Cytotoxic Effect of Microbial Biosurfactants Against Human Embryonic Kidney Cancerous Cell: HEK-293 and Their Possible Role in Apoptosis

Two different microbial biosurfactants S9BS and CHBS were isolated from Lysinibacillus fusiformis S9 and Bacillus tequilensis CH. Cytotoxicity effect of these biosurfactants on human embryonic kidney cancerous cell (HEK-293) were studied with the help of 3-(4,5-dimethylthiazol-2yl-)-2, 5-diphenyl tetrazolium bromide (MTT) assay and morphological changes were observed under inverted microscope. The biosurfactants exhibited positive cytotoxic effect on HEK-293 cell line. It was found that LC₅₀ of S9BS and CHBS were 75 and 100 μg ml^?1, respectively. Further cell cycle and apoptosis analysis of biosurfactant-treated HEK-293 cell line were done by FACS. In this study, cytotoxic effect of glycolipid biosurfactant against HEK-293 cell lines is reported for the first time. Mechanism towards increased membrane permeability of biosurfactant-treated cancer cell may be the incorporation of its lipid moiety into the plasma membrane leading to formation of pores and membrane disruption. Hence, these microbial biosurfactants can prove to be significant biomolecule for cancer treatment.