N,N-Dibromobenzenesulfonamide as an analytical reagent: Determination of thiocyanate and cyanide ions in metal complexes and salts and thiosemicarbazide alone and in its metal complexes

Simple, rapid, and reproducible analytical procedures, for determining thiocyanate and cyanide ions in metal salts and complexes and thiosemicarbazide (TSC) in the free state and in its metal complexes, with the new oxidant, dibromamine-B (DBB), have been proposed. These procedures are also useful for computing the number of ligands present in the complexes. With DBB, CN⁻, and NCS⁻ ions and TSC undergo stoichiometric oxidations with 2-, 8-, and 12-electron changes per ion or molecule, respectively, in water-acetic acid medium. The reagent DBB has been prepared and characterized by elemental analyses and ir and FT-NMR-¹H and -¹³C spectral data.     

Activation of p300 histone acetyltransferase by small molecules altering enzyme structure: probed by surface-enhanced Raman spectroscopy

Reversible acetylation of nucleosomal histones and nonhistone proteins play pivotal roles in the regulation of all the DNA templated phenomenon. Dysfunction of the enzymes involved in the acetylation/deacetylation leads to several diseases. Therefore, these enzymes are the targets for new generation therapeutics. Here, we report the synthesis of trifluoromethyl phenyl benzamides and their effect on histone acetyltransferase (HAT) activity of p300. One of these benzamides, CTPB (N-(4-chloro-3-trifluoromethyl-phenyl)-2-ethoxy-6-pentadecyl-benzamide), was discovered as a potent activator of the p300 HAT activity. We have found that pentadecyl hydrocarbon chain of CTPB is required to activate the HAT only under certain context. Furthermore, our results show that the relative position of -CF3 and -Cl in CTB (N-(4-chloro-3-trifluoromethyl-phenyl)-2-ethoxy-benzamide) is also very critical for the activation. Surface-enhanced Raman spectroscopy (SERS) of p300 and the HAT activator complexes evidently suggest that the activation of HAT activity is achieved by the alteration of p300 structure. Therefore, apart from elucidating the chemical basis for small molecule mediated activation of p300, this report also describes, for the first time, Raman spectroscopic analysis of the complexes of histone-modifying enzymes and their modulators, which may be highly useful for therapeutic applications.     

Structural studies of 2,5-disubstituted 1,3,4-thiadiazole derivatives from dithioesters under the mild condition: Studies on antioxidant,antimicrobial activities,and molecular docking

Abstract

A series of 2,5-disubstituted 1,3,4-thiadiazole was synthesized and evaluated for their antioxidant and molecular docking studies. These molecules were efficiently synthesized under mild and inexpensive starting material. Construction of these molecules developed using substituted aldehydes and substituted dithioesters in presence of NCS (N-Chorosuccinimide). The compounds 4a, 4b, 4c, 4f, and 4k showed good antibacterial and antioxidant activity among which, 4k possess excellent antibacterial and antioxidant activity. The results of antioxidant activity studies revealed that compound 4k manifested profound antioxidant potential. The molecular docking study was performed with respective newly synthesized compounds to ascertain the binding mode of 4k with respect to the critical proteins involved in biosynthesis and metabolic pathways.     

Kinetic and mechanistic studies on the oxidation of arginine and histidine by chloramine-T in hydrochloric acid medium

The oxidation of amino acids by chloramine-T (CAT) in HCl medium at 30°C indicates simultaneous catalysis by H⁺ and Cl^– ions in the HCl concentration range of 0.04–0.12 M. The reaction is first order with respect to concentrations [CAT], [H⁺] and [arginine], but zero order with respect to [histidine]. The rate depends also on Cl^– concentration following 0.7th order. At HCl concentrations >0.12 M, the rate equation is:w=k[CAT] [amino acid]^0.6 and is independent of the [Cl^–]. A suitable mechanism has been suggested.

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-T (CAT) HCl (30°C) H⁺, Cl^– [HCl]=0,04–0,12M. [CAT], [H⁺] [] []. [Cl^–]^0,7. [HCl]>0,12M =k · [CAT][]^0,6 [Cl^–]. .

     

Analysis of a shielded TE011 mode composite dielectric resonator for stable frequency reference

Analysis of a TE₀₁₁ mode composite sapphire-rutile dielectric resonator has been carried out to study the temperature variation of resonance frequency, close to the Cs atomic clock hyperfine frequency of 9.192 GHz. The complementary behavior of dielectric permittivity with temperature of the composite has been exploited to obtain the desired turning point in the resonant frequency. The frequency of the composite structure is found to be independent of the shield diameter beyond four times the puck diameter.     

Controlled synthesis of nanocrystalline Li2MnSiO4 particles for high capacity cathode application in lithium-ion batteries

Monodispersed Li(2)MnSiO(4) nanoparticles are synthesized via a supercritical solvothermal method at 300 °C for 5 min reaction time. The as-synthesized nanoparticles are free from impurities and have 15-20 nm diameter. After coating with conductive polymer, a discharge capacity of 313 mA h g(-1) is obtained for the first time because of nearly 2Li(+) reaction.     

Anti-cancer activity of novel dibenzo[b,f]azepine tethered isoxazoline derivatives

Background  

Nef is an HIV-1 accessory protein essential for viral replication and AIDS progression. Nef interacts with a multitude of host cell signaling partners, including members of the Src kinase family. Nef preferentially activates Hck, a Src-family kinase (SFK) strongly expressed in macrophages and other HIV target cells, by binding to its regulatory SH3 domain. Recently, we identified a series of kinase inhibitors that preferentially inhibit Hck in the presence of Nef. These compounds also block Nef-dependent HIV replication, validating the Nef-SFK signaling pathway as an antiretroviral drug target. Our findings also suggested that by binding to the Hck SH3 domain, Nef indirectly affects the conformation of the kinase active site to favor inhibitor association.     

Manganese(III) oxidation of L‐serine in aqueous sulfuric acid medium: Kinetics and mechanism

Kinetics and mechanism of oxidation of L‐serine by manganese(III) ions have been studied in aqueous sulfuric acid medium at 323 K. Manganese(III) sulfate was prepared by an electrolytic oxidation of manganous sulfate in aqueous sulfuric acid. The dependencies of the reaction rate are: an unusual one and a half‐order on [Mn(III)], first‐order on [ser], an inverse first‐order on [H⁺], and an inverse fractional‐order on [Mn(II)]. Effects of complexing agents and varying solvent composition were studied. Solvent isotope studies in D₂O medium were made. The dependence of the reaction rate on temperature was studied and activation parameters were computed from Arrhenius‐Eyring plots. A mechanism consistent with the observed kinetic data has been proposed and discussed. © 1999 John Wiley & Sons, Inc. Int J Chem Kinet 31: 525–530, 1999