Simultaneous determination of dorzolamide and timolol by first-order derivative UV spectroscopy in simulated biological fluid for in vitro drug release testing

Srushti Tambe; Divya Jain; Purnima Amin

doi:10.1016/j.saa.2021.119682

Simultaneous determination of dorzolamide and timolol by first-order derivative UV spectroscopy in simulated biological fluid for in vitro drug release testing

Spectrochim Acta A Mol Biomol Spectrosc. 2021 Jul 5:255:119682. doi: 10.1016/j.saa.2021.119682. Epub 2021 Mar 13.

Authors

Srushti Tambe¹, Divya Jain¹, Purnima Amin²

Affiliations

¹ Institute of Chemical Technology, Department of Pharmaceutical Science and Technology, Mumbai 400019, India.
² Institute of Chemical Technology, Department of Pharmaceutical Science and Technology, Mumbai 400019, India. Electronic address: pd.amin@ictmumbai.edu.in.

PMID: 33770736
DOI: 10.1016/j.saa.2021.119682

Abstract

Dorzolamide hydrochloride and timolol maleate is a well-established fixed-dose combination for the treatment of glaucoma worldwide. The utilization of simulated biological fluids can give a superior understanding of the release mechanisms and practicable in vivo nature of a dosage form that can improve the predictive potential of in vitro drug release testing. No method has been reported so far for the simultaneous estimation of dorzolamide and timolol in simulated tear fluid. In the present study, a simple, precise, and accurate first-order derivative ultraviolet spectrophotometric method for the routine analysis of dorzolamide and timolol in simulated tear fluid is proposed for in vitro drug release testing. The developed method was validated as per International Conference on Harmonization guidelines Q2 (R1). First-order derivative UV spectrophotometry was successfully applied to separate the overlapping peaks of dorzolamide and timolol by measuring peak amplitude at 251.80 nm and absorbance at 295.00 nm, respectively. The method was found to be accurate and precise, with a recovery range of 98.0 -101.0% and low relative standard deviations (<2.0%). The developed method was successfully applied for in vitro drug release testing of in-house in situ gel and marketed eye drops containing dorzolamide and timolol. Various mathematical models were adopted to fit the in vitro drug release profile. It was observed that the drug release of both drugs from the in situ gel and the marketed solution were best fitted by the Higuchi and first-order kinetic models, respectively. Moreover, the analysis of variance (ANOVA) provision was used for the validation of results. Overall, with the advantages of simple and fast operations, as well as reliability, the proposed method offers an ideal platform for routine analysis as compared to other high-cost and time-consuming chromatographic techniques. Having access to such a robust method will encourage the use of simulated tear fluid for in vitro drug release testing of ocular products and help to predict the in vivo performances of ophthalmic preparations.

Keywords: Dorzolamide; First-order derivative spectroscopy; Fixed dose combinations; Simulated tear fluid; Timolol.

MeSH terms

Antihypertensive Agents
Drug Combinations
Drug Liberation
Ophthalmic Solutions
Reproducibility of Results
Sulfonamides
Thiophenes*
Timolol*

Substances

Antihypertensive Agents
Drug Combinations
Ophthalmic Solutions
Sulfonamides
Thiophenes
Timolol
dorzolamide