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1.
Pakistan Journal of Pharmaceutical Sciences. 2017; 30 (3): 891-895
in English | IMEMR | ID: emr-186486

ABSTRACT

This study evaluated the impact of pH [7.4 and 6.5], bovine serum albumin [BSA], and human serum albumin [HSA] on Curcumin activity against 2 reference, 1 clinical, and 10 environmental strains of Staphylococcus aureus [S. aureus]. Minimal inhibitory concentrations [MICs] of Curcumin against S. aureus were statistically indifferent [p>0.05] at pH7.4 and pH6.5. Activity of Curcumin against S. aureus was reduced by two folds in the presence of 1.25-5% BSA/HAS

2.
Pakistan Journal of Pharmaceutical Sciences. 2016; 29 (6): 2119-2124
in English | IMEMR | ID: emr-184159

ABSTRACT

Peptides derived from HIV-1 transmembrane proteins have been extensively studied for antimicrobial activities, and they are known as antimicrobial peptides [AMPs]. These AMPs have also been reported to potently combat the drug-resistant microbes. In this study, we demonstrated that peptide no. 6383 originated from HIV-1 MN strain membrane-spanning domain of gp41 was active [2-log reductions] at 100 micro g/mL [56.5 micro M] against methicillin-resistant Staphylococcus aureus [MRSA] in 10% and 50% human plasma-supplemented phosphate buffered saline [PBS]. The activity was further enhanced [3-log reductions] in the presence of 5% human serum albumin [HSA] alone. All bactericidal activities were achieved within 6 hours. At 100 micro g/mL, the peptide showed only 13% toxicity against human erythrocytes. This peptide can serve as an attractive template for a design of a novel peptide antibiotic against drugresistant bacteria. By sequence-specific engineering or modifications, we anticipated that the bactericidal activity and the reduced toxicity against human erythrocytes will be improved

3.
Pakistan Journal of Pharmaceutical Sciences. 2015; 28 (6): 2109-2114
in English | IMEMR | ID: emr-174521

ABSTRACT

This study evaluated the synergistic antibacterial activity of Curcumin with 8 different antibiotic groups. Two reference, one clinical and ten environmental strains of Staphylococcus aureus [S. aureus] were tested. Disc diffusion assay with 25[micro]g/mL Curcumin demonstrated synergism in combination with a majority of tested antibiotics against S. aureus. However, checkerboard micro dilution assay only showed synergism, fractional inhibitory concentration index [FICI] <0.5 in three antibiotics i.e. Gentamicin, Amikacin, and Ciprofloxacin. Other antibiotics showed indifferent interactions but no antagonism was observed. In time-kill curve, appreciable reduction of bacterial cells was also observed in combination therapy [Curcumin + antibiotics] compared to monotherapy [Curcumin or antibiotic[s] alone]. The antibiotics with higher synergistic interaction with Curcumin are arranged in a decreasing order: Amikacin > Gentamicin > Ciprofloxacin

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