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Liquid chromatographic-mass spectrometric method for determination of drug content uniformity of two commonly used dermatology medications in a split-tablet dosage form
A Kadi, Adnan; S Abdelhameed, Ali; Attwa, Mohamed W; Al- Haddab, Mohammad & Angawi, Rihab F
Abstract
Purpose: To develop and validate a simple, efficient and reliable Liquid chromatographic-mass
spectrometric (LC-MS/MS) method for the quantitative determination of two dermatological drugs,
Lamisil® (terbinafine) and Proscar® (finasteride), in split tablet dosage form.
Methods: Thirty tablets each of the 2 studied medications were randomly selected. Tablets were
weighed and divided into 3 groups. Ten tablets of each drug were kept intact, another group of 10
tablets were manually split into halves using a tablet cutter and weighed with an analytical balance; a
third group were split into quarters and weighed. All intact and split tablets were individually dissolved in
a water: methanol mixture (4:1), sonicated, filtered and further diluted with mobile phase. Optimal
chromatographic separation and mass spectrometric detection were achieved using an Agilent 1200
HPLC system coupled with an Agilent 6410 triple quadrupole mass spectrometer. Analytes were eluted
through an Agilent eclipse plus C8 analytical column (150 mm × 4.6 mm, 5 μm) with a mobile phase
composed of solvent A (water) containing 0.1% formic acid and 5mM ammonium formate pH 7.5, and
solvent B (acetonitrile mixed with water in a ratio A:B 55:45) at a flow rate of 0.8 mL min-1 with a total
run time of 12 min. Mass spectrometric detection was carried out using positive ionization mode with
analyte quantitation monitored by multiple reaction monitoring (MRM) mode.
Results: The proposed analytical method proved to be specific, robust and adequately sensitive. The
results showed a good linear fit over the concentration range of 20 - 100 ng mL-1 for both analytes, with
a correlation coefficient (r2) ≥ 0.999 and 0.998 for finasteride and terbinafine, respectively. Following
tablet splitting, the drug content of the split tablets fell outside of the proxy USP specification for at least
14 halves (70 %) and 34 quarters (85 %) of FIN, as well as 16 halves (80 %) and 37 quarters (92.5 %)
of TBN. Mean weight loss, after splitting, was 0.58 and 2.22 % for FIN half- and quarter tablets,
respectively, and 3.96 and 4.09 % for TBN half- and quarter tablets,respectively.
Conclusion: The proposed LC-MS/MS method has successfully been used to provide precise drug
content uniformity of split tablets of FIN and TBN. Unequal distribution of the drug on the split tablets is
indicated by the high standard deviation beyond the accepted value. Hence, it is recommended not to
split non-scored tablets especially, for those medications with significant toxicity
Keywords
Tablet splitting; Finasteride; Terbinafine; Drug content uniformity; LC-MS/MS
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