Mohammad Arif Cheema
University of Santiago de Compostela
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Featured researches published by Mohammad Arif Cheema.
Molecular Physics | 2006
Mohammad Arif Cheema; Pablo Taboada; Silvia Barbosa; Mohammad Siddiq; Víctor Mosquera
Apparent molal volumes and adiabatic compressibilities of aqueous solutions of the amphiphilic cationic antidepressant drugs butriptyline and doxepin hydrochlorides have been determined from density and ultrasound velocity measurements in the temperature range 20–50°C. Critical concentrations for aggregation of these drugs were obtained from ultrasound velocity measurements. Negative deviations from the Debye–Hückel limiting law of the apparent molal volume were obtained from both drugs in all temperature ranges, except for doxepin at 50°C, which provides evidence of no pre-association at concentrations below the critical concentration. Apparent molal adiabatic compressibilities of the aggregates formed by these drugs were typical of those corresponding for an aggregate formed by a stacking process.
Colloids and Surfaces B: Biointerfaces | 2008
Mohammad Arif Cheema; Pablo Taboada; Silvia Barbosa; Manuel Gutiérrez-Pichel; Emilio Castro; Mohammad Siddiq; Víctor Mosquera
The interactions and complexation process of the structurally related amphiphilic phenothiazines promazine and triflupromazine hydrochlorides with horse myoglobin in aqueous buffered solutions of pH 2.5, 5.5 and 9.0 have been examined by zeta-potential, isothermal titration calorimetry (ITC), UV-vis spectroscopy and dynamic light-scattering techniques with the aim of analyzing the effect of hydrophobic and electrostatic forces, the alteration of protein conformation and the effect of substituents in the drug molecular structure on the binding mechanism and structure of the resulting complexes. The energetics and stoichiometry of the binding process was derived from ITC. The enthalpies of binding obtained are small and exothermic, and the Gibbs energies of binding are dominated by large increases in entropy consistent with hydrophobic interactions. Binding isotherms were obtained from microcalorimetric data by using a theoretical model based on the Langmuir isotherm. zeta-Potential data showed a reversal in the sign of the protein charge at pH 9.0 as a consequence of drug binding. Gibbs energies of drug binding per mole of drug were also derived from zeta-potential data. On the other hand, binding of the phenothiazines causes a conformational transition on protein structure which was followed as a function of drug concentration by using UV-vis spectroscopy. These data were analyzed to obtain the Gibbs energy of the transition in water (DeltaG(w)(degrees)) and in a hydrophobic environment (DeltaG(hc)(degrees)). Finally, the population distribution of the different species in solution and their size was analyzed through dynamic light scattering. The existence of an aggregation process of drug/protein complexes, mainly at pH 2.5, was observed. We think this is a consequence of the already expanded structure of the protein at this pH and the subsequent binding of drug molecules to the protein.
Chemical Physics | 2006
Mohammad Arif Cheema; Silvia Barbosa; Pablo Taboada; Emilio Castro; Mohammad Siddiq; Víctor Mosquera
The Journal of Chemical Thermodynamics | 2009
Mohammad Arif Cheema; Pablo Taboada; Silvia Barbosa; Josué Juárez; Manuel Gutiérrez-Pichel; Mohammad Siddiq; Víctor Mosquera
Journal of Chemical & Engineering Data | 2008
Mohammad Arif Cheema; Mohammad Siddiq; Silvia Barbosa; Pablo Taboada; Víctor Mosquera
Journal of Physical Chemistry B | 2007
Silvia Barbosa; Mohammad Arif Cheema; Pablo Taboada; Víctor Mosquera
Biomacromolecules | 2007
Mohammad Arif Cheema; Pablo Taboada; Silvia Barbosa; Emilio Castro; Mohammad Siddiq; Vfctor Mosquera
The Journal of Chemical Thermodynamics | 2008
Mohammad Arif Cheema; Pablo Taboada; Silvia Barbosa; Emilio Castro; Mohammad Siddiq; Víctor Mosquera
Journal of Chemical & Engineering Data | 2007
Mohammad Arif Cheema; Emilio Castro; Pablo Taboada; Mohammad Siddiq; Víctor Mosquera
Chemical Physics | 2007
Mohammad Arif Cheema; Mohammad Siddiq; Silvia Barbosa; Emilio Castro; José A. Egea; Luis T. Antelo; Pablo Taboada; Víctor Mosquera