Heterocyclo-Substituted Sulfa Drugs: Part XII. Mercapto-S-Azo-Benzothiazol Dyes and Their Metal Complexes

New azo sulfadrugs of 2-mercapto-S-azo ( p '-heterocyclo-substituted benzene-sulfonyl) benzothiazole derivatives (L 1 and L 2 ) were synthesized by coupling of p '-heterocyclo-substituted-benzene-sulphonyl diazonium salts with 2-mercapto-benzothiazole in acid medium. The corresponding iron(III), cobalt(II), nickel(II), copper(II), and mercury(II) chelates were prepared in a 1:1 metal to ligand molar ratio. The ligands and their chelates were characterized on the basis of microanalysis, UV, IR, and H 1 -NMR spectrometry. Thermal decomposition of the complexes was studied in static air. On the basis of the thermogravimetric curves some decomposition steps could be correlated with the proper decomposition products. The photochemical behavior of the ligands and their complexes were investigated. The photosensitivity shown by the complexes was attributed to the photoreactivity of their free ligands. The ligands and their chelates were screened in vitro for their antimicrobial activities (antibacterial and antifungal). The complexes induce a remarkable increase in the antimicrobial activity compared to the corresponding ligands.     

Synthesis of Novel Derivatives of 1,5-Benzothiazepines (Part 1)

Synthesis of 2,4-disubstituted 1,5-benzothiazepines 3a-3i is reported by the condensation of 2-aminothiophenol 1 with 1,3-diones in pyridine. The structures of the compounds have been established by elemental, IR, 1 H NMR, 13 C NMR, and mass spectral analyses.     

Identification of novel HDAC8 selective inhibitors through ligand and structure based studies: Exploiting the acetate release channel differences among class I isoforms

Histone deacetylases (HDACs) are key regulators of gene expression and have emerged as crucial therapeutic targets for cancer. Among the HDACs, inhibition of HDAC8 enzyme has been reported to be a novel strategy in the treatment of female-specific cancers. Most of the HDAC inhibitors discovered so far inhibit multiple HDAC isoforms causing toxicities in the clinic thus limiting their potential. Therefore, the discovery of isoform-selective HDAC8 inhibitors is highly desirable. In the present study, a combination of ligand and structure based drug design tools were utilized to build a statistically significant pharmacophore based 3D QSAR model with statistical parameters R²: 0.9964, and Q²: 0.7154, from a series of 31 known HDAC8 inhibitors. Top 1000 hits obtained from Virtual screening of Phase database were subjected to docking studies against HDAC8. Top 100 hits obtained were redocked into HDAC Class I (HDAC 1,2,3) and Class II isoforms (HDAC 4, 6) and rescored with XP Glide Score. Based on fitness score, XP glide score and interacting amino acid residues, five HDAC8 inhibitors (1–5) were selected for in vitro studies. The HDAC8 activity assay followed by enzyme kinetics clearly indicated Compounds 1, 2 and 3 to be potent HDAC8 selective inhibitors with IC₅₀ of 126 pM, 112 nM, and 442 nM respectively. These compounds were cytotoxic to HeLa cells where HDAC8 is overexpressed but not to normal cells, HEK293. Also, they were able to induce apoptosis by modulating Bax/Bcl2, cleavage of PARP and release of Cytochrome C. Molecular Dynamics simulations observed most favorable interaction patterns and presented a rationale for the activities of the identified compounds. Selectivity against HDAC8 was due to exploitation of the architectural difference in the acetate release channel among class I HDAC isoforms.     

Gold-Catalyzed 1,2-Dicarbofunctionalization of Alkynes with Organohalides**

Herein, we report the first gold-catalyzed 1,2-dicarbofunctionalization of alkynes using organohalides as non-prefunctionalized coupling partners. The mechanism of the reaction involves an oxidative addition/π-activation mechanism in contrast to the migratory insertion/cis-trans isomerization pathway that is predominantly observed with other transition metals yielding products with anti-selectivity. Mechanistic insights include several control experiments, NMR studies, HR-MSMS analyses, and DFT calculations that strongly support the proposed mechanism.     

Phase diagram of magnetic polymers

We consider polymers made of magnetic monomers (Ising or Heisenberg-like) in a good solvent. These polymers are modeled as self-avoiding walks on a cubic lattice, and the ferromagnetic interaction between the spins carried by the monomers is short-ranged in space. At low temperature, these polymers undergo a magnetic induced first order collapse transition, that we study at the mean field level. Contrasting with an ordinary point, there is a strong jump in the polymer density, as well as in its magnetization. In the presence of a magnetic field, the collapse temperature increases, while the discontinuities decrease. Beyond a multicritical point, the transition becomes second order and -like. Monte Carlo simulations for the Ising case are in qualitative agreement with these results. Received 11 February 1999     

Single crystal study of the one dimensional Ca Co O compound: five stable configurations for the Ising triangular lattice

Single crystals of the one-dimensional phase Ca₃Co₂O₆ of several mm length have been grown. The magnetic study of such a crystal confirms the previous observations on polycrystalline samples: it consists of a triangular lattice of ferromagnetic [Co₂O₆] chains ( K) antiferromagnetically coupled ( K). The dynamic of these chains array, probed by AC susceptibility, is very slow as shown from the large shift of the freezing temperature from 12 K to 16.5 K as the excitation frequency increases by three orders of magnitude (10⁰ to 10³ Hz). The origin of this effect is believed to be the result of different arrangements with close energies for the chain ferromagnetic moments on the triangular lattice. Five stable magnetic configurations have been evidenced by the magnetization as a function of applied field curves registered at 2 K. Their relative magnetizations correspond to m =1/4, 1/2, 1, 2, 3 where m =3 represents the ferromagnetic ordering of three chains on the same triangle, each chain having a m =1 magnetization. A magnetic phase diagram is finally proposed. Received 7 December 1999     

Studies on the Stability of On-top Al13Inm (n = 1～12,m =-1,0,+1) Clusters

Energetic and electronic structures of the on-top Al13Inm (n = 1 ～12,m = -1,0,+1)clusters have been investigated by employing a first-principles pseudo-potential plane wave method.Several parameters such as binding energies,second differences of energy and vertical-electron detachment energies have been adopted to characterize and evaluate the structure stability of Al13In (n = 1 ～ 12) clusters.The optimized models show that the Al13 moieties in the clusters can not retain the original regular icosahedron structure.Results from binding energy and second difference of energy show that Al13In and Al13In- clusters with even n are more stable than those with odd n in contrast with Al13In+ clusters.The calculation of vertical-electron detachment energies (VDE) of Al13In clusters indicates that Al13In and Al13In- clusters with even n are closer to the closed shell of the Jellium model.Further analysis of electron density of states and electron density differences reveals that the enhanced stability of Al13In- clusters is not only associated with the closed shell of valence electrons but also with the bonding type between I and associated Al atoms.     

QSAR Studies on 7-Substituted Fluoroquinolones

1 INTRODUCTION Fluoroquionlones are potent antibacterials with a broad spectrum of activities against gram-positive and gram-negative organisims and mycobacteria by inhibiting bacterial topoisomerase II(DNA gyra- se)[1].These compounds have been successfully used in clinic for a decade and its market has risen in recent years only a little less than that of penicillins and macrolides[2]. The fluoroquinolones constitute a class of extremely potent and orally active broad spectrum antibact…     

A survey of sampling-based Bayesian analysis of financial data

The capability of implementing a complete Bayesian analysis of experimental data has emerged over recent years due to computational advances developed within the statistical community. The objective of this paper is to provide a practical exposition of these methods in the illustrative context of a financial event study. The customary assumption of Gaussian errors underlying development of the model is later supplemented by considering Student-t errors, thus permitting a Bayesian sensitivity analysis. The supplied data analysis illustrates the advantages of the sampling-based Bayesian approach in allowing investigation of quantities beyond the scope of classical methods.