Literature DB >> 12908733

Determination of the cardiac glycosides digoxin and digitoxin by liquid chromatography combined with isotope-dilution mass spectrometry (LC-IDMS)--a candidate reference measurement procedure.

Patricia Kaiser1, Udo Kramer, Dieane Meissner, Michael Kress, William Graham Wood, Hans Reinauer.   

Abstract

This article describes a method of high analytical sensitivity, reproducibility and trueness for the determination of digoxin and digitoxin in serum or plasma at therapeutic levels using a combination of high-pressure liquid chromatography (HPLC), isotope-dilution mass spectrometry (IDMS) and caesium-adduct formation. A method for threefold deuterium substitution in the glycosides was developed, which could be performed within 24 hours without distillation giving yields > 98% of the theoretical value. Extraction from a serum or plasma matrix was performed using a liquid-phase extraction with ammonium acetate buffer/tertiary butylmethyl ether/ethyl acetate at pH 9.5. The HPLC-separation used a 10 x 2 mm LiChrospher RP-18 5 microm guard column in combination with a 125 x 2 mm main column of the same material and a gradient containing methanol, caesium ions and formic acid. Quantification of digoxin and digitoxin was made with IDMS using deuterated internal standards and the system run in single ion monitoring (SIM) mode. The methods had a lower limit of determination of 0.25 microg/l for digoxin and digitoxin, a trueness between 97.5 and 104% for digoxin and between 98 and 101% for digitoxin, respectively and had a coefficient of variation of less than 3% in the therapeutic range for both glycosides. Maximally 1 ml serum or plasma was needed for the procedure. The method is used to set target values for materials used in external quality assessment surveys (EQAS) run by INSTAND as part of a national EQAS-programme.)

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Year:  2003        PMID: 12908733

Source DB:  PubMed          Journal:  Clin Lab        ISSN: 1433-6510            Impact factor:   1.138


  2 in total

1.  Proximal Roux-en-Y gastric bypass alters drug absorption pattern but not systemic exposure of CYP3A4 and P-glycoprotein substrates.

Authors:  Lingtak-Neander Chan; Yvonne S Lin; Jessica C Tay-Sontheimer; Dorothy Trawick; Brant K Oelschlager; David R Flum; Kristen K Patton; Danny D Shen; John R Horn
Journal:  Pharmacotherapy       Date:  2015-03-10       Impact factor: 4.705

2.  A new approach for the determination of immunosuppressive drugs using HPLC-MS/MS and Cs+ adducts.

Authors:  Patricia Kaiser; Theodorus Akerboom; William Graham Wood; Hans Reinauer
Journal:  Ger Med Sci       Date:  2006-01-18
  2 in total

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