Chromatographic analysis of penicillins in pharmaceutical formulations and biological fluids

Samanidou, Victoria F.; Evaggelopoulou, Evaggelia N.; Papadoyannis, Ioannis N.

doi:10.1002/jssc.200600137

Cited by 29 publications

(18 citation statements)

References 156 publications

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“…[4][5][6][7][8][9][10][11][12][13] However, last few decades witnessed an upsurge in electrochemical methods for the detection and determination of these compounds. Therapeutic drug monitoring (TDM) is a clinical strategy that measures drug concentration in a patient's bloodstream to monitor its compliance, efficacy and toxicity, thus optimizing and managing individual medication regimen.…”

Section: Introductionsupporting

confidence: 86%

Research progress in electroanalytical techniques for determination of antimalarial drugs in pharmaceutical and biological samples

et al. 2016

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Section: Introductionsupporting

confidence: 86%

Research progress in electroanalytical techniques for determination of antimalarial drugs in pharmaceutical and biological samples

et al. 2016

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“…HPLC methodology for all these analytes exists in the literature, although too numerous to recite here; in recent years the bioanalysis of the penicillins and the Cephalosporins have been reviewed [7,8]. Whilst the patients in our project would usually be administered only one of the antibiotics at a time, and we are only interested in measuring one antibiotic in each sample, for the purposes of simplicity and efficiency we desired the minimum number of methods for measuring our multiple analytes.…”

Section: Introductionmentioning

confidence: 98%

Analysis of 12 beta-lactam antibiotics in human plasma by HPLC with ultraviolet detection

McWhinney

Wallis

Hillister

et al. 2010

Journal of Chromatography B

188

130

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“…Penicillins' determination in pharmaceutical formulations and biological fluids is based mainly on reversed‐phase high performance liquid chromatography (HPLC) using bonded silica analytical columns. From the currently available methods 90% use C 18 columns, 7% use C 8 and 3% use other types of analytical columns, such as CN, SCX, MAX, MIP, cyclodextrin, etc 8. The same conclusion can also be drawn for food samples (fish, milk), in cattle, pig, and chicken tissues (muscle, kidney, liver), animal feed 9–12…”

Section: Introductionmentioning

confidence: 90%

On the use of Kinetex^™‐C₁₈ core‐shell 2.6 µm stationary phase to the multiclass determination of antibiotics

Samanidou¹,

Karageorgou²

2010

Drug Testing and Analysis

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Fast and accurate analysis is a prerequisite in all analytical fields especially in food, biological, pharmaceutical, and environmental samples. The new trend of ultra performance liquid chromatography (LC) has the main drawback of expensive instrumentation, which can't be easily found in low-budget analytical laboratories. The evolution of core shell technology has contributed to this direction, since ultra high efficiency can be achieved on common LC instrument platforms. Herein the novel core shell analytical column, KINETEX (™) 2.6 µm, (150 mm × 4.6 mm) was comparatively studied against two conventional reversed-phase silica-based and one monolithic column. Eight antimicrobial agents representing two different classes: penicillins and amphenicols, were separated using a typical 400 bar high performance liquid chromatography (HPLC) equipment. Comparison of column performance was carried out by calculation of the number of theoretical plates N, the tailing factor T(f) , the relative retention time RRT, the retention factor k, the resolution factor R(s) , and the precision of the retention time and peak area. Optimal chromatographic conditions were used to validate the method. Its applicability was proven by the analysis of veterinary drug formulations. The examined antibiotics were well resolved within 17 min. Limit of quantitation values were 25.9 ng for amoxicillin, 14.1 ng for ampicillin, 41.6 ng for thiamphenicol, 9.6 ng for oxacillin, 23.5 ng for florfenicol, 26.7 for cloxacillin, 23.5 ng for chloramphenicol and 42.3 ng for dicloxacillin for 20 µL injection volume. The developed method can be easily and readily transferred to any laboratory.

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Chromatographic analysis of penicillins in pharmaceutical formulations and biological fluids

Cited by 29 publications

References 156 publications

Research progress in electroanalytical techniques for determination of antimalarial drugs in pharmaceutical and biological samples

Research progress in electroanalytical techniques for determination of antimalarial drugs in pharmaceutical and biological samples

Analysis of 12 beta-lactam antibiotics in human plasma by HPLC with ultraviolet detection

On the use of Kinetex^™‐C₁₈ core‐shell 2.6 µm stationary phase to the multiclass determination of antibiotics

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Chromatographic analysis of penicillins in pharmaceutical formulations and biological fluids

Cited by 29 publications

References 156 publications

Research progress in electroanalytical techniques for determination of antimalarial drugs in pharmaceutical and biological samples

Research progress in electroanalytical techniques for determination of antimalarial drugs in pharmaceutical and biological samples

Analysis of 12 beta-lactam antibiotics in human plasma by HPLC with ultraviolet detection

On the use of Kinetex™‐C18 core‐shell 2.6 µm stationary phase to the multiclass determination of antibiotics

Contact Info

Product

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On the use of Kinetex^™‐C₁₈ core‐shell 2.6 µm stationary phase to the multiclass determination of antibiotics