The stereoselective disposition of the enantiomers of ibuprofen in blood, blister and synovial fluid.

Seideman, P; Lohrer, F.; Graham, Gerald G.; Duncan, Mark W.; Williams, Katie; Day, RO

doi:10.1111/j.1365-2125.1994.tb04345.x

Cited by 24 publications

(9 citation statements)

References 22 publications

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“…isomer as well as values of AUC S(?) always exceed those of the R(-) enantiomer (Day et al 1988;Cox et al 1991;Geisslinger et al 1993;Seideman et al 1994) with similar selective accumulation being shown in experimentally induced skin suction blisters (Seideman et al 1994). The patterns of synovial fluid accumulation of the enantiomers follows that of the peak plasma levels with broad peaks of R(-) and S(?)…”

Section: Pharmacokinetics In Adultsmentioning

confidence: 84%

“…The patterns of synovial fluid accumulation of the enantiomers follows that of the peak plasma levels with broad peaks of R(-) and S(?) ibuprofen at about 2-4 h and extending to about 12-15 h (Seideman et al 1994) thus showing persistence of the enantiomers in synovial fluids well past those of the peak plasma concentrations of these enantiomers.…”

Section: Pharmacokinetics In Adultsmentioning

confidence: 91%

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Ibuprofen: pharmacology, efficacy and safety

2009

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This assessment of the safety and benefits of ibuprofen can be summarized thus: (1) Ibuprofen at OTC doses has low possibilities of serious GI events, and little prospect of developing renal and associated CV events. Ibuprofen OTC does not represent a risk for developing liver injury especially the irreversible liver damage observed with paracetamol and the occasional liver reactions from aspirin. (2) The pharmacokinetic properties of ibuprofen, especially the short plasma half-life of elimination, lack of development of pathologically related metabolites (e.g. covalent modification of liver proteins by the quinine-imine metabolite of paracetamol or irreversible acetylation of biomolecules by aspirin) are support for the view that these pharmacokinetic and notably metabolic effects of ibuprofen favour its low toxic potential. (3) The multiple actions of ibuprofen in controlling inflammation combine with moderate inhibition of COX-1 and COX-2 and low residence time of the drug in the body may account for the low GI, CV and renal risks from ibuprofen, especially at OTC doses.

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Section: Pharmacokinetics In Adultsmentioning

confidence: 84%

Section: Pharmacokinetics In Adultsmentioning

confidence: 91%

Ibuprofen: pharmacology, efficacy and safety

2009

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“…The indirect techniques include HPLC using UV [26,27], fluorescence [28,29], and mass spectrometric detection [30][31][32][33]. Gas chromatography-mass spectrometry (GC/ MS) methods have been reported as well [2,6,[34][35][36].…”

Section: Introductionmentioning

confidence: 99%

“…GC/MS methods can be stereoselective, but they use a larger sample size for analysis (i.e., 0.8 mL plasma or 1 mL of serum) [34,6], and their sensitivity is insufficient (i.e., 0.25 µg/mL or LOQ 5 µg/mL) [34,35], or they are not stereoselective [35,36]. Several indirect HPLC/ MS/MS methods were reported for various in vitro [30][31][32] and in vivo [33] analyses of ibuprofen, but these methods are not stereoselective and do not represent significant improvement in comparison to the methodologies reported above.…”

Section: Introductionmentioning

confidence: 99%

A Validated Enantioselective Assay for the Determination of Ibuprofen in Human Plasma Using Ultra Performance Liquid Chromatography with Tandem Mass Spectrometry (UPLC-MS/MS)

Szeitz¹,

Edginton²,

Peng³

et al. 2010

AJAC

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A modified ultra performance liquid chromatography-tandem mass spectrometry (UPLC-MS/MS) method was developed and validated for the quantitation of ibuprofen enantiomers in human plasma. Ibuprofen and flurbiprofen (internal standard) were extracted from human plasma at acidic pH, using a single-step liquid-liquid extraction with methyl-tert-butyl ether. The enantiomers of ibuprofen and flurbiprofen were derivatized to yield the corresponding diastereomers. Chromatographic separation was achieved using a phenyl column with a run time of 20 min. (R)-and (S)-ibuprofen were quantitated at the multiple reaction monitoring (MRM) transition of m/z 360.2  232.1, and (R)-and (S)-flurbiprofen were monitored at the MRM transition of m/z 398.3  270.1. The method was validated for accuracy, precision, linearity, range, limit of quantitation (LOQ), limit of detection (LOD), selectivity, absolute recovery, matrix effect, dilution integrity, and evaluation of carry-over. Accuracy for (R)-ibuprofen ranged between -11.8% and 11.2%, and for (S)-ibuprofen between -8.6% and -0.3%. Precision for (R)-ibuprofen was ≤ 11.2%, and for (S)-ibuprofen ≤ 7.0%. The calibration curves were weighted (1/X 2 , n = 7) and were linear with r 2 for (R)-ibuprofen ≥ 0.988 and for (S)-ibuprofen ≥ 0.990. The range of the method was 50 to 5000 ng/mL with the LOQ of 50 ng/mL, and LOD of 1 ng/mL, for (R)-and (S)-ibuprofen requiring 100 µL of sample. The method was applied successfully to a pharmacokinetic study with the administration of a single oral dose of ibuprofen capsules to human subjects.

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“…The concentrations of tepoxalin and its carboxylic acid metabolite in plasma and synovial fluid were determined according to Seidemann et al (1994) and Depre et al (1993).…”

Section: Measurement Of Tepoxalinmentioning

confidence: 99%