Quantitative softness parameters and their application in elucidation of Structure of Bimetallic Tetrathiocyanate Complexes

〉₂M(NCS)₂M′(SCN)₂〈 and [ML₆][M′(SCN)₄], (M = Co(II) and Ni(II), M′ = Zn(II), Cd(II) and Hg(II) and L = aniline(ani), p-toluidine(tol), pyridine(py), nicotinamide(nia), 2,2′-bipyridine(bipy) and 4-aminopyridine (apy)) have been prepared and characterized. Their structure have been proposed on the basis of molar conductance, magnetic moment, group theoretical calculations, ligand field parameters, infrared and electronic spectral studies. The proposed structures have also been supported by quantitative values of softness ?\documentclass{article}\pagestyle{empty}\begin{document}$ {\rm E}_{\rm n}^{_ + ^ +},{\rm E}_{\rm m}^{_{\rm +}^{\rm +}} $\end{document}”?,. Total softness of M and M′ and their difference \documentclass{article}\pagestyle{empty}\begin{document}$ \Delta {\rm TE}_{\rm n}^{_ + ^ +} \left({{\rm M} - {\rm M}'} \right) $\end{document} have also been derived by the following equations and related to the structure of the complexes. .     

Superconductivity and resistance behaviour of σ-phase alloys: Nb−Rh and Ta−Rh

Superconductivity, structure and electrical resistance behaviour of -phase alloys of Nb–Rh and Ta–Rh are investigated. The Ta–Rh alloys do not become superconducting above 1.2 K. The andH _c2 (0) values of a homogeneous alloy with the composition Nb_65.2Rh_34.8 are 2.95 K, 13.9 kG/K and 23 kG, respectively, whereas for an inhomogeneous alloy with the composition Nb_63.7Rh_36.3 these values are 4.24 K, 5.5 kG/K and 14 kG, respectively. Splat quenching results in a substantial increase in the andH _c2 (0) values of the Rh-rich sample. Annealing (900°C, 100 h) of the Rh-rich sample leads only to small changes in the superconducting properties but a small amount of Nb–Rh solid solution has been formed. The electrical resistance of Nb_65.2Rh_34.8 decreases with decreasing temperature and varies asT ^0.5 between 150 and 240 K and asT between 60 and 140 K. For Ta_70.0Rh_30.0 the temperature coefficient changes to negative values below 170K. values are calculated for Nb–Rh using McMillan's formula. An estimatedT _c value of Ta–Rh is 0.2 K. TheH _c2 (0) values of Nb–Rh are in good agreement with the theoreticalH _c ^2** (0) values.Dedicated to Prof. Dr. W. Buckel on the occasion of his 60th birthday     

Theβ-decay of100Y: Discovery of a very low lying 0+ state in100Zr

Theβ-decay of¹⁰⁰Y has been investigated at the gas filled recoil separator JOSEF by means ofγ-ray and conversion electron spectroscopy. Twoβ-decay modes, of half lives 0.94±0.03 s and 0.55±0.15 s, have been observed. Using Xγ-, Xce-, γγ- andγce-coincidences the level scheme of¹⁰⁰Zr has been constructed. An excited 0 ₂ ⁺ state at 331.3 keV has been discovered in this nucleus. Theβ-decay from the 0.55 s decay mode in¹⁰⁰Y shows a strong preference for the ground state compared to the 0 ₂ ⁺ state in¹⁰⁰Zr. The structure of¹⁰⁰Zr and the nature of the 0 ₂ ⁺ level is discussed in the light of the present results.     

Monomer dependence of radiation graft polymerization. V. Poly(ethylene-g-4-vinylpyridine)

The radiation-initiated graft polymerization of 4-vinylpyridine to high-density polyethylene has been studied under diffusion-free conditions by the mutual irradiation technique. The reaction rate is 1/2 order in radiation intensity over the range 0.00076–0.011 Mrad/hr. The reaction rate is first order in monomer at 0.00076 Mrad/hr, over the complete range of monomer concentrations; at 0.021 Mrad/hr, up to 60 vol % monomer; and at 0.21 Mrad/hr, up to 50 vol % monomer.     

Effect of diffusion on rates and molecular weights in graft polymerization

A theoretical analysis has been made of the graft polymerization process in terms of the quantitative interrelationship between the initiation rate R_i, the k_p/k_t^1/ ratio of the monomer, the equilibrium solubility M of the monomer in the polymer, the polymer film thickness L, and the diffusivity D of the monomer in the polymer. It is shown how the values of these parameters in any grafting system interact to lead to diffusion-controlled graft polymerization. Whether graft polymerization is diffusion-free or diffusion-controlled depends on the values of K_p, d, k_p/k_p^1/2, and L as gathered in the parameter A = [(K_p/k_t^1/2)R_i, D,/^1/2] L/2. When the values of the various terms are such that A is less than 0.1 (i.e., D is large while R_i, k_p, and L are small), the reaction is diffusion-free. When A is greater than 3 (i.e., D is small while R_i, k_p, and L are large), the reaction is diffusion-controlled. The derived equations showing the relationship between kinetic and diffusional parameters are theoretically applicable to all grafting systems, i.e., for all monomer-polymer combinations under all conditions of reaction temperature, radiation intensity and polymer film thickness. The theoretical analysis has been verified for the rate and degree of polymerization for the radiation-induced graft polymerization of styrene to polyethylene.     

Ruthenium(II) complexes with mono and ditertiary arsines and phosphines and their reaction with small molecules

Dichlorotetrakis(dimethylsulphoxide)ruthenium(II) reacts with AsPh₃ AsMePh₂, AsMe₂Ph and SbPh₃ in ethanolic hydrochloric acid solution to yield the complexes RuCl₂(DMSO)₂(AsPh₃)₂, RuCl₂(DMSO) L₂ (L = AsMePh₂, AsMe₂Ph, SbPh₃) respectively. The treatment of ruthenium(II) blue solution with AsMePh₂, AsMe₂Ph and SbPh₃ in alcohol resulted in the formation of the complexes; RuCl₂L₃ (L = AsMePh₂, AsMe₂Ph and SbPh₂), respectively. The reaction of RuCl₂(DMSO)₄ with the bidentate ligands 1,2 bis (diphenylarsino)methane (DPAM), 1,2 bis(diphenylarsino)ethane (DPAE) and 1,2 bis (diphenylphosphino)methane (DPPM). 1,2 bis(diphenylphosphino)ethane (DPPE), in ethanol gave the complexes RuCl₂(DPAM)₂, RuCl₂(DPAE)₂, RuCl₂ (DPPM)₂ RuCl₂(DPPE)₂, respectively. The complexes thus obtained undergo reaction with carbon monoxide, hydrogen, molecular nitrogen and nitric oxide to yield a variety of mixed ligand complexes.     

Production and Purification of Pectinase from Bacillus subtilis 15A-B92 and Its Biotechnological Applications

Enzymes that degrade pectin are called pectinases. Pectinases of microbial origin are used in juice clarification as the process is cost-effective. This study screened a pectinase-producing bacterium isolated from soil and identified as Bacillus subtilis 15A B-92 based on the 16S rRNA molecular technique. The purified pectinase from the isolate showed 99.6 U/mg specific activity and 11.6-fold purity. The molecular weight of the purified bacterial pectinase was 14.41 ± 1 kD. Optimum pectinase activity was found at pH 4.5 and 50 °C, and the enzyme was 100% stable for 3.5 h in these conditions. No enzymatic inhibition or activation effect was seen with Fe²⁺, Ca²⁺, or Mg²⁺. However, a slight inhibition was seen with Cu²⁺, Mn²⁺, and Zn²⁺. Tween 20 and 80 slightly inhibited the pectinase, whereas iodoacetic acid (IAA), ethylenediaminetetraacetate (EDTA), urea, and sodium dodecyl sulfate (SDS) showed potent inhibition. The bacterial pectinase degraded citrus pectin (100%); however, it was inactive in the presence of galactose. With citrus pectin as the substrate, the Km and Vmax were calculated as 1.72 mg/mL and 1609 U/g, respectively. The high affinity of pectinase for its substrate makes the process cost-effective when utilized in food industries. The obtained pectinase was able to clarify orange and apple juices, justifying its application in the food industry.     

Three New Acrylic Acid Derivatives from Achillea mellifolium as Potential Inhibitors of Urease from Jack Bean and α-Glucosidase from Saccharomyces cerevisiae

(1) Background: Achillea mellifolium belongs to a highly reputed family of medicinal plants, with plant extract being used as medicine in indigenous system. However, limited data is available regarding the exploitation of the medicinal potential of isolated pure compounds from this family; (2) Methods: A whole plant extract was partitioned into fractions and on the basis of biological activity, an ethyl acetate fraction was selected for isolation of pure compounds. Isolated compounds were characterized using different spectroscopic techniques. The compounds isolated from this study were tested for their medicinal potential using in-vitro enzyme assay, coupled with in-silico studies; (3) Results: Three new acrylic acid derivatives (1–3) have been isolated from the ethyl acetate fraction of Achillea mellifolium. The characterization of these compounds (1–3) was carried out using UV/Vis, FT-IR, 1D and 2D-NMR spectroscopy (¹H-NMR, ¹³C-NMR, HMBC, NOESY) and mass spectrometry. These acrylic acid derivatives were further evaluated for their enzyme inhibition potential against urease from jack bean and α glucosidase from Saccharomyces cerevisiae, using both in-silico and in-vitro approaches. In-vitro studies showed that compound 3 has the highest inhibition against urease enzyme (IC₅₀ =10.46 ± 0.03 μΜ), followed by compound 1 and compound 2 with percent inhibition and IC₅₀ value of 16.87 ± 0.02 c and 13.71 ± 0.07 μΜ, respectively, compared to the standard (thiourea-IC₅₀ = 21.5 ± 0.01 μΜ). The investigated IC₅₀ value of compound 3 against the urease enzyme is two times lower compared to thiourea, suggesting that this compound is twice as active compared to the standard drug. On the other hand, all three compounds (1–3) revealed mild inhibition potential against α-glucosidase. In-silico molecular docking studies, in combination with MD simulations and free energy, calculations were also performed to rationalize their time evolved mode of interaction inside the active pocket. Binding energies were computed using a MMPBSA approach, and the role of individual residues to overall binding of the inhibitors inside the active pockets were also computed; (4) Conclusions: Together, these studies confirm the inhibitory potential of isolated acrylic acid derivatives against both urease and α-glucosidase enzymes; however, their inhibition potential is better for urease enzyme even when compared to the standard.     

Microscale Thermophoresis and Molecular Modelling to Explore the Chelating Drug Transportation in the Milk to Infant

The microscale thermophoresis (MST) technique was utilized to investigate lactoferrin–drug interaction with the iron chelator, deferiprone, using label-free system. MST depends on the intrinsic fluorescence of one interacting partner. The results indicated a significant interaction between lactoferrin and deferiprone. The estimated binding constant for the lactoferrin–deferiprone interaction was 8.9 × 10⁻⁶ ± 1.6, SD, which is to be reported for the first time. Such significant binding between lactoferrin and deferiprone may indicate the potentiation of the drug secretion into a lactating mother’s milk. The technique showed a fast and simple approach to study protein–drug interaction while avoiding complicated labeling procedures. Moreover, the binding behavior of deferiprone within the binding sites of lactoferrin was investigated through molecular docking which reflected that deferiprone mediates strong hydrogen bonding with ARG121 and ASP297 in pocket 1 and forms H-bond and ionic interaction with ASN640 and ASP395, respectively, in pocket 2 of lactoferrin. Meanwhile, iron ions provide ionic interaction with deferiprone in both of the pockets. The molecular dynamic simulation further confirmed that the binding of deferiprone with lactoferrin brings conformational changes in lactoferrin that is more energetically stable. It also confirmed that deferiprone causes positive correlation motion in the interacting residues of both pockets, with strong negative correlation motion in the loop regions, and thus changes the dynamics of lactoferrin. The MM-GBSA based binding free energy calculation revealed that deferiprone exhibits ∆G TOTAL of −63,163 kcal/mol in pocket 1 and −63,073 kcal/mol in pocket 2 with complex receptor–ligand difference in pocket 1 and pocket 2 of −117.38 kcal/mol and −111.54 kcal/mol, respectively, which in turn suggests that deferiprone binds more strongly in the pocket 1. The free energy landscape of the lactoferrin–deferiprone complex also showed that this complex remains in a high energy state that confirms the strong binding of deferiprone with the lactoferrin. The current research concluded that iron-chelating drugs (deferiprone) can be transported from the mother to the infant in the milk because of the strong attachment with the lactoferrin active pockets.