Simultaneous Determination of Atorvastatin and Glimepiride by LC-MS/MS in Human Plasma and Its Application to a Pharmacokinetic Study

Kishore Kumar Hotha; Narasimha Reddy Yarramu; Thriveni Kandibedala; Vijaya Bharathi Dasari; Venkateswarlu Vobalaboina

doi:10.4236/ajac.2012.38074

American Journal of Analytical Chemistry > Vol.3 No.8, August 2012

Simultaneous Determination of Atorvastatin and Glimepiride by LC-MS/MS in Human Plasma and Its Application to a Pharmacokinetic Study

Kishore Kumar Hotha, Narasimha Reddy Yarramu, Thriveni Kandibedala, Vijaya Bharathi Dasari, Venkateswarlu Vobalaboina
Bioanalytical Department, Integrated Product Development, Dr. Reddy’s Laboratories Ltd, Bachupalli, Hyderabad, India.
DOI: 10.4236/ajac.2012.38074 PDF HTML 6,451 Downloads 12,898 Views Citations

Abstract

The aim of the proposed research work was to develop and validate a simple, selective high sensitive and high-throughput assay for the simultaneous estimation of Atorvastatin and Glimepiride in human plasma using liquid chromatography tandem mass spectrometry (LC-MS/MS). Atorvastatin–Glimepiride combines a competitive inhibitor of HMG-CoA reductase and a sulfonylurea anti-diabetic drug. The purpose of this study was to develop single method for Atorvastatin and Glimepiride in plasma by liquid chromatography-tandem mass spectrometry (LC-MS/MS) that would result into a simultaneous estimation of Atorvastatin and Glimepiride avoiding acid –lactone inter conversions right from sample collections to analysis on the LC-MS/MS. Sample collection procedure optimized for Atorvastatin holds good for Glimepiride, hence resulting into a simultaneous estimation of Atorvastatin and Glimepiride. Liquid-liquid extraction and liquid chromatography coupled to positive ion mode tandem mass spectrometry was used to develop the method and was validated according to US FDA guidelines. The calibration curves for two analytes were linear (R2 ≥ 0.9950, n = 4) over the concentration range of 0.2 - 30 ng/mL for Atorvastatin and 1 - 250 ng/mL for Glimepiride. Mean extraction recoveries 80.34 ± 9.43 for Atorvastatin and 88.19 ± 7.13 for Glimepiride. Intra- and inter-run mean percent accuracy was between 85% - 115% and percent imprecision was ≤15%. Stability studies revealed that Atorvastatin and Glimepiride were stable in plasma during bench top (10.5 h at room temperature), in Injector (47.5 h), at the end of three successive freeze and thaw cycles and long term at -65℃ ± 15℃ for 114 days. The method was successfully applied to the study of pharmacokinetics of Atorvastatin and Glimepiride in healthy volunteers. Simultaneous estimation of Atorvastatin and Glimepiride is cost effective, reduces analysis cycle time, enables effective utilization of resources and reduces bleeding burden on human volunteers.

Keywords

Atorvastatin; Glimepiride; LC-MS/MS; Method Validation; Human Plasma and Pharmacokinetic Studies

Share and Cite:

K. Hotha, N. Yarramu, T. Kandibedala, V. Dasari and V. Vobalaboina, "Simultaneous Determination of Atorvastatin and Glimepiride by LC-MS/MS in Human Plasma and Its Application to a Pharmacokinetic Study," American Journal of Analytical Chemistry, Vol. 3 No. 8, 2012, pp. 559-569. doi: 10.4236/ajac.2012.38074.

Conflicts of Interest

The authors declare no conflicts of interest.

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