Your search keyword '"Baraldi, Cecilia"' showing total 5 results

1. DFT, molecular docking and SERS (concentration and solvent dependant) investigations of a methylisoxazole derivative with potential antimicrobial activity.

Author

Sheena Mary, Y., Shyma Mary, Y., Krátký, Martin, Vinsova, Jarmila, Baraldi, Cecilia, and Gamberini, Maria Cristina

Subjects

*SURFACE enhanced Raman effect, *MOLECULAR docking, *SERS spectroscopy, *METALLIC surfaces, *SURFACE interactions

Abstract

• Concentration dependant SERS studies. • Nucleophilic and electrophilic sites are identified. • Biological properties studies. • Molecular docking studies identifies the pharmacological property. Spectroscopic analysis, DFT studies and surface enhanced Raman scattering of antimicrobial bioactive 4-[(2‑ hydroxy -3,5- diiodobenzylidene) amino ]- N -(5-methylisoxazole-3-yl)benzenesulfonamide (HDMB) have been studied. Changes in intensity and enhancement variations are observed for Raman and SERS bands. Changes observed in the ring mode vibrations may be due to surface π-electron interactions which means molecule is orientated in a tilted position with respect to metal surface. Changes in orientation are seen in SERS spectra depending on concentration. The molecular docking results show that binding affinity and interactions with the receptors may be supporting evidence for further studies in design further HDMB pharmaceutical applications. Reactivity properties are obtained from DFT analysis. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2021

2. Concentration and solvent dependent SERS, DFT, MD simulations and molecular docking studies of a thioxothiazolidine derivative with antimicrobial properties.

Author

Mary, Y. Sheena, Mary, Y. Shyma, Armaković, Stevan, Armaković, Sanja J., Krátký, Martin, Vinsova, Jarmila, Baraldi, Cecilia, and Gamberini, Maria Cristina

Subjects

*MOLECULAR docking, *SURFACE enhanced Raman effect, *SERS spectroscopy, *METALLIC surfaces, *SURFACE interactions, *SOLVENTS, *ACETIC acid

Abstract

Spectroscopic analysis, DFT studies and surface enhanced Raman scattering of antimicrobial bioactive (Z)-2-[5-(5-bromo-2-hydroxybenzylidene)-4-oxo-2-thioxothiazolidin-3-yl]acetic acid (BPTA) have been studied on different silver sols. Very large changes are observed for Raman and SERS bands. Observed variations in the ring modes may be due to surface π-electron interactions and presence of this indicated that molecule is inclined with respect to the metal surface. Changes in orientation are seen in SERS spectra depending on concentration. The molecular docking results show that binding affinity and interactions with the receptors may be supporting evidence for further studies in design further BPTA pharmaceutical applications. Reactivity properties are obtained from DFT and MD simulations. The quantum-mechanical level of theory has been applied to obtain information about the MEP and ALIE surfaces. These calculations give sensitivity of BPTA towards autoxidation mechanism. An influence of water has been studied computationally, via the MD simulations and RDF analysis. This level of theory was also used to identify possible excipient substance for this molecule. [Display omitted] • Concentration dependent SERS studies. • Nucleophilic and electrophilic sites are identified. • Reactivity properties by ALIE and MEP. • Identified maltose as a suitable excipient for title compound. [ABSTRACT FROM AUTHOR]

Published

2021

3. Concentration dependent SERS, DFT and molecular docking studies of a ureido derivative with antitubercular properties.

Author

Mary, Y. Sheena, Mary, Y. Shyma, Krátký, Martin, Vinsova, Jarmila, Baraldi, Cecilia, and Cristina Gamberini, Maria

Subjects

*MOLECULAR docking, *SERS spectroscopy, *UREA derivatives, *DENSITY functional theory, *ELECTRIC potential, *SURFACE interactions

Abstract

• Concentration dependent SERS studies. • Nucleophilic and electrophilic sites are identified. • Biological properties studies. • Molecular docking studies identifies the pharmacological property. Spectroscopic analysis, density functional theory (DFT) studies and surface enhanced Raman scattering (SERS) of antimycobactetial 4-[3-(4-acetylphenyl)ureido]-2-hydroxybenzoic acid (AUHB) have been studied on different silver sols. For Raman and SERS wavenumbers, very large changes are observed. Observed variations in the modes of ring may be due to surface π-electron interactions and presence of this indicated that poly substituted ring is more inclined than para substituted phenyl ring and assumes a inclined position for concentration 10−3 M. Changes in orientation are seen in SERS spectra depending on concentration. In order to find electron-rich and poor sites of AUHB, molecular electrostatic potential was also constructed. The molecular docking results show that binding affinity and interactions with the receptor DprE1 may be supporting evidence for further studies in design further AUHB pharmaceutical applications. Based on antitubercular activity of 4-aminosalicylic acid (PAS) and urea derivatives we designed, synthesized and investigated mutual PAS-urea derivatives as potential antimycobacterial agents. [ABSTRACT FROM AUTHOR]

Published

2021

4. DFT, SERS-concentration and solvent dependent and docking studies of a bioactive benzenesulfonamide derivative.

Author

Sheena Mary, Y., Shyma Mary, Y., Krátký, Martin, Vinsova, Jarmila, Baraldi, Cecilia, and Gamberini, Maria Cristina

Subjects

*SURFACE enhanced Raman effect, *SERS spectroscopy, *MOLECULAR docking, *METALLIC surfaces, *SURFACE interactions

Abstract

• Concentration dependent SERS studies • Nucleophilic and electrophilic sites are identified • Docking studies reveals the pharmacological properties Spectroscopic analysis, DFT studies and surface enhanced Raman scattering (SERS) of antimicrobial bioactive 4-[(5- tert -butyl)2-hydroxybenzylidene]amino- N -(4,6-dimethylpyrimidin-2-yl)benzenesulfonamide (THPB) have been studied on different silver sols. Intensity and hence enhancement variations are observed for Raman and SERS bands. Observed changes in the ring modes may be due to surface π-electron interactions and presence of this indicated that molecule is inclined with respect to the metal surface. Changes in orientation are seen in SERS spectra depending on concentration. The molecular docking results show that binding affinity and interactions with the receptors may be supporting evidence for further studies in design further THPB pharmaceutical applications. Reactivity properties are obtained from DFT analysis. Image, graphical abstract [ABSTRACT FROM AUTHOR]

Published

2021

5. Spectroscopic investigations, concentration dependent SERS, and molecular docking studies of a benzoic acid derivative.

Author

Gamberini, Maria Cristina, Mary, Y. Shyma, Mary, Y. Sheena, Krátký, Martin, Vinsova, Jarmila, and Baraldi, Cecilia

Subjects

*MOLECULAR docking, *ACID derivatives, *BENZOIC acid, *DENSITY functional theory, *ELECTRIC potential, *SERS spectroscopy, *CHEMICAL species

Abstract

• Concentration dependent SERS studies. • Nucleophilic and electrophilic sites are identified. • Studied NLO properties, DSSC, MEP and NBO. • Molecular docking studies identifies the pharmacological property. Spectroscopic analysis, density functional theory (DFT) studies and surface enhanced Raman scattering of 4-((3-bromo-5-chloro-2-hydroxybenzylidene)amino)benzoic acid (BCHB) have been studied on different silver colloids concentrations in order to know the particular chemical species responsible for the spectra. For Raman and surface enhanced Raman scattering (SERS) wavenumbers, changes are observed. Observed variations in the modes of ring may be due to interaction of the π-electrons and presence of this indicated that RingII is more inclined than RingI and the BCHB assumes inclined orientation for concentration 10-3 M. Changes in orientation are seen in SERS spectra depending on concentration. In order to determine the electron-rich and poor sites of BCHB, the molecular electrostatic potential was also constructed. The molecular docking studies show that the bindings and interactions with the receptors may be supporting evidence for further studies in design further BCHB pharmaceutical applications. [ABSTRACT FROM AUTHOR]

Published

2021