Please use this identifier to cite or link to this item: http://localhost:80/xmlui/handle/123456789/14269
Title: VALIDATION AND APPLICATION OF REVERSED PHASE HIGH-PERFORMANCE LIQUID CHROMATOGRAPHIC METHOD FOR QUANTIFICATION OF PIZOTIFEN MALATE IN PHARMACEUTICAL SOLID DOSAGE FORMULATIONS
Authors: MUKIDUR RAHMAN, SHAIKH
KALAM LUTFUL KABIR, ABUL
JAHAN, MD. ARSHAD
RUHUL MOMEN, AZM
SHARA SHAMSUR ROUF, ABU
Keywords: Chromatography
pizotifen malate
placebo study
sedating antihistamine
system suitability
ultraviolet detection
Issue Date: 14-Oct-2010
Publisher: Karachi: Faculty of Pharmacy & Pharmaceutical Sciences, Karachi
Citation: Rahman, S. M., Kabir, A. K. L., Jahan, A. M., Momen, A. R., & Rouf, A. S. S. (2010). Validation and application of reversed phase high-performance liquid chromatographic method for quantification of pizotifen malate in pharmaceutical solid dosage formulations. Pakistan journal of pharmaceutical sciences, 23(4), 435-442.
Abstract: The aim of this study was to develop and validate an isocratic reversed phase high-performance liquid chromatographic method for quantification of pizotifen malate in pharmaceutical solid dosage formulations. Good chromatographic separation of pizotifen malate was achieved by using an analytical column, C18 ODS column. The system was operated at 40°C oven temperature using a mobile phase consisting of acetonitrile and acetate buffer pH 7.0 (60:40) at a flow rate of 2 ml/min. The method showed high sensitivity with good linearity (r2 = 0.99997) over the tested concentration range of 0.0020 - 0.0300 mg/ml for pizotifen malate. Detection was carried out at 231 nm and retention time was 2.838 min. Placebo and blank studies were performed and no peak was observed at the retention time of pizotifen malate. The intermediate precision and accuracy results (mean ± RSD, n=3) were (99.11±0.21) % and (99.19±0.55) % respectively with tailing factor (1.26±0.19). The proposed method was validated in terms of selectivity, linearity, accuracy, precision, range, detection and quantitation limit, system suitability and solution stability. This method can be successfully employed for simultaneous quantitative analysis of pizotifen malate in pharmaceutical solid dosage formulations.
URI: http://142.54.178.187:9060/xmlui/handle/123456789/14269
ISSN: 1011-601X
Appears in Collections:Issue 04

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