Synthesis of novel structurally simplified estrogen analogues

A library of 17 novel estrogen analogues 3 and 4 containing different substituents at rings A and D (steroid nomenclature) was prepared in a five- to seven-step synthesis. The key transformation is a Sonogashira-coupling of cyclic vinyl iodides of type 7 or 8 with phenylacetylenes of type 9. Reduction of the keto function in 3 led to the estradiol analogue 5.     

Identification of potential inhibitory analogs of metastasis tumor antigens (MTAs) using bioactive compounds: revealing therapeutic option to prevent malignancy

The deeper understanding of metastasis phenomenon and detection of drug targets could be a potential approach to minimize cancer mortality. In this study, attempts were taken to unmask novel therapeutics to prevent metastasis and cancer progression. Initially, we explored the physiochemical, structural and functional insights of three metastasis tumor antigens (MTAs) and evaluated some plant-based bioactive compounds as potent MTA inhibitors. From 50 plant metabolites screened, isoflavone, gingerol, citronellal and asiatic acid showed maximum binding affinity with all three MTA proteins. The ADME analysis detected no undesirable toxicity that could reduce the drug likeness properties of top plant metabolites. Moreover, molecular dynamics studies revealed that the complexes were stable and showed minimum fluctuation at molecular level. We further performed ligand-based virtual screening to identify similar drug molecules using a large collection of 376,342 compounds from DrugBank. The results suggested that several structural analogs (e.g., tramadol, nabumetone, DGLA and hydrocortisone) may act as agonist to block the MTA proteins and inhibit cancer progression at early stage. The study could be useful to develop effective medications against cancer metastasis in future. Due to encouraging results, we highly recommend further in vitro and in vivo trials for the experimental validation of the findings.

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Rational Enzyme Design without Structural Knowledge: A Sequence-Based Approach for Efficient Generation of Transglycosylases

Glycobiology is dogged by the relative scarcity of synthetic, defined oligosaccharides. Enzyme-catalysed glycosylation using glycoside hydrolases is feasible but is hampered by the innate hydrolytic activity of these enzymes. Protein engineering is useful to remedy this, but it usually requires prior structural knowledge of the target enzyme, and/or relies on extensive, time-consuming screening and analysis. Here, a straightforward strategy that involves rational rapid in silico analysis of protein sequences is described. The method pinpoints 6–12 single-mutant candidates to improve transglycosylation yields. Requiring very little prior knowledge of the target enzyme other than its sequence, the method is generic and procures catalysts for the formation of glycosidic bonds involving various d /l -, α/β-pyranosides or furanosides, and exo or endo action. Moreover, mutations validated in one enzyme can be transposed to others, even distantly related enzymes.     

Synthesis of Novel Spiro-Oxazino-Quinoline Derivatives and Study of Their Photophysical Properties

A convenient route was successfully developed for the synthesis of novel heterocycles such as spiro-oxazino-quinoline derivatives from 2-aminoquinoline-3-carbonitrile (4) in good yield. The Spiro-quinoline derivatives (6, 8 and 10) were synthesized and further studied for their photophysical properties. Semiempirical molecular orbital calculation (PM3/PM6 for structure) proves to be a suitable tool for the prediction of absorption and fluorescence properties of these compounds.     

Nonlinear direct inverse method: a shortcut method for simultaneous calibration and isotherm determination

This work addresses a way to combine isotherm determination and nonlinear calibration. In this method, like the classical inverse method, experimental elution profiles are compared with the results of a detailed model that accounts for nonlinearity in equilibrium, axial dispersion, and mass transfer kinetics. However, unlike the classical inverse method, the calibration of detector is carried out simultaneously with isotherm determination thereby reducing cost and saving time. In this study no limitation is imposed on the linearity of the detector signal or on the overlapping of elution profiles for the separation of enantiomers. The method has been experimentally validated for the separation of a mixture of guaifenesin enantiomers over a wide range of concentration.     

Zinc and iron determination in serum and urine samples of thyroid patients using cloud point extraction

A simple and rapid cloud point extraction method was applied for preconcentration of trace quantities of zinc (Zn) and iron (Fe) in biological samples (serum and urine) of thyroid patients prior to determination by flame atomic absorption spectrometry. The metals in serum and urine samples were complexed with 1-(2-thiazolylazo)-2-naphthol and entrapped in the surfactant octylphenoxypolyethoxyethanol (Triton X-114). After centrifugation, the surfactant-rich phase was diluted with 0.1 M HNO3 in methanol. For optimum recovery of analytes, the influences of the analytical parameters, including pH and amounts of complexing and surfactant reagents, were investigated. Enrichment factors of 66.4 and 70.2 were obtained for the preconcentration of Zn(II) and Fe(III), respectively. The obtained results showed sufficient recoveries (>98%) for Zn(II) and Fe(III) in certified reference materials (CRMs). The proposed method was applied to the determination of Zn(II) and Fe(III) in biological (serum and urine) samples and CRMs.     

Synthesis,structure determination and chemoselective catalytic studies of amino acids complexes of osmium(II)

The two new half sandwich amino acids complexes of osmium, i.e. [Os(η6‐p‐cymene)(κ1‐N‐(rac)‐phenylglycine methylester)Cl₂] ( A ) and [Os(η6‐p‐cymene)(κ1‐N,N′‐(S)‐phenylalanineamido)Cl] ( B ) have been synthesized and employed for chemoselective reduction of ketones (nine α,β‐unsaturated ketones and three saturated ketones). The complexes were characterized by spectroscopic as well as analytical methods; their solid structures were confirmed by single‐crystal X‐ray analysis. Both of the osmium complexes catalyze the reduction of α,β‐unsaturated ketones to saturated ketones via isomerization of the initially produced allylic alcohols. The reducible substrates were studied to obtain information on the steric and electronic factors which may affect the interaction of the substrate with the metal center and, thus, control the selectivity of the hydrogen‐transfer reductions. Copyright © 2008 John Wiley & Sons, Ltd.     

Plasma activated water: the next generation eco-friendly stimulant for enhancing plant seed germination,vigor and increased enzyme activity,a study on black gram (Vigna mungo L.)

Plasma Chemistry and Plasma Processing - Chemical fertilization in agriculture is threatening to the ecosystem. Therefore, the use of eco-friendly stimulant for crop revolution is highly desirable....     

Synthesis of some novel D-ring-fused dioxa- and oxazaphosphorinanes in the estrone series

New types of P-heterocyclic-fused steroids, such as dioxa- and oxazaphosphorinane derivatives, were synthetized from estrone-1,3-dihydroxy and 1,3-aminoalcohol precursors by cyclization with phenylphosphonic dichloride.