Jörgen Vessman scite author profile

Tranexamic acid 1 g was given intravenously to three healthy volunteers. Plasma concentrations decayed in three monoexponential phases. Most elimination took place during the first eight hours, giving an apparent elimination half-life of approximately two hours. Plasma clearance ranged between 110-116 ml/min. The urinary recovery of tranexamic acid exceeded 95% of the dose. Ten healthy volunteers were given tranexamic acid 2 g orally on an empty stomach, and together with a meal. Food had no influence on the absorption of tranexamic acid, as judged by comparison of the peak plasma concentration, the time required to reach the peak, the AUC from zero to six hours, and the urinary excretion data. The oral bioavailability of tranexamic acid, calculated from 24 h urinary excretion after oral and intravenous administration, was 34% of the dose.

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Selectivity in analytical chemistry (IUPAC Recommendations 2001)

Vessman

et al. 2001

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Republication or reproduction of this report or its storage and/or dissemination by electronic means is Selectivity in analytical chemistry (IUPAC Recommendations 2001)Abstract: The correct use of the term "selectivity" and its clear distinction from the term "specificity" are discussed. A definition of selectivity is given, and it is recommended that the use of this term be promoted and that the use of the term "specificity" be discouraged.

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Polar organic phase liquid chromatography with packed capillary columns using a vancomycin chiral stationary phase

et al. 2000

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Vancomycin immobilized on silica served as the chiral stationary phase (CSP) in this investigation with polar organic solvents as the mobile phase in liquid chromatography (LC). It was shown that trace amounts of water were beneficial for improving peak shape and efficiency. To regulate the retention and selectivity an acid and/or base were added to the mobile phase where an excess of acid was shown to be preferential for enantioseparation. An unusual increase in selectivity with increasing temperature was shown for the acidic drug, thalidomide. Additionally, nonlinear van't Hoff plots were obtained for metoprolol enantiomers that showed increased retention with increasing temperature. Metoprolol also showed unusual behavior in the polar organic phase when water was added to resemble reversed-phase chromatography, with minimum retention observed at high water or high methanol concentrations. In both instances a high degree of electrostatic interaction between metoprolol and vancomycin was concluded. Metoprolol and ten of its analogs were examined on this CSP to evaluate the enantiorecognition process. A comparison in enantioselectivity for a number of acidic and basic drugs using this CSP was also carried out using the polar organic phase, reversed phase, and normal phase LC which were all compared to the results obtained in supercritical fluid chromatography (SFC). Polar organic phase LC offered a better separation of basic molecules while reversed phase LC was preferred for the resolution of acids. SFC showed the broadest enantioselectivity overall and normal phase LC indicated similar properties, as expected, to SFC but with lower column efficiency. Copyright 2000 Wiley-Liss, Inc.

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Selectivity or specificity? Validation of analytical methods from the perspective of an analytical chemist in the pharmaceutical industry

Vessman

1996

Journal of Pharmaceutical and Biomedical Analysis

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Evaluation of a vancomycin chiral stationary phase in packed capillary supercritical fluid chromatography

et al. 1999

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Jörgen Vessman

Pharmacokinetics and bioavailability of tranexamic acid

Selectivity in analytical chemistry (IUPAC Recommendations 2001)

Polar organic phase liquid chromatography with packed capillary columns using a vancomycin chiral stationary phase

Selectivity or specificity? Validation of analytical methods from the perspective of an analytical chemist in the pharmaceutical industry

Evaluation of a vancomycin chiral stationary phase in packed capillary supercritical fluid chromatography

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