Development and Validation of RP-HPLC Method for Quantification of Total, Free and Entrapped Ritonavir in Lipid Nanocarriers and Drug content of Film Coated Fixed Dose Formulation

Introduction. Qualitative and quantitative analysis of pharmaceutical substances using reverse-phase high-performance liquid chromatography based on domestic hardware is an important stage in the approval of medicines. Drug «Kalidavir» is widely used in the treatment of human immunodeficien-cy virus. The developed methodology assumes significant advantages in comparison with foreign methods involving the use of imported equipment and standards from the United States recommended by regulatory documentation. The aim of the study was to develop and conduct validation procedures for the quantitative analysis of ritonavir and lopinavir in the combined drug «Kalidavir». Material and methods. The optimized parameters of chromatographic operations included the column size (752 mm), the choice of the polymer sorbent ProntoSil 120-5C AQ, as well as a binary mobile phase consisting of a 0.1% solution of trifluoroacetic acid in an aqueous medium and metha-nol, respectively, with a flow rate setting of 150 µl per minute and a column temperature of 35oC. An isocratic elution regime was applied, ensuring a continuous supply of eluent and the correctness of the analytical conclusion. Additionally, the injection volume of 2 µl and the determination of absorp-tion at four wavelengths from the range from 200 to 240 nm were established. Results. Retention times of ritonavir and lopinavir were 7.2 min and 11.9 min, respectively. Linearity was observed in the range from 0.025 mg/ml for ritonavir and 0.1 mg/ml for lopinavir and reached 0.5 mg/ml for both substances, with a good correlation coefficient (> 0.999). Relative errors accord-ing to the developed quantitative determination methods did not exceed 0.85% for lopinavir and 0.96% for ritonavir. Conclusions. The methods of qualitative and quantitative determination of lopinavir and ritonavir in the combined tablet dosage form "Kalidavir" by high-performance liquid chromatography using domestic equipment have been developed and approved, which allowed to obtain sufficiently reliable and reproducible results.

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Development and validation of a new RP-UPLC method for the simultaneous estimation of nirmatrelvir and ritonavir in bulk and copacked tablet dosage forms

Pallavi,

Sowjanya

2023

RJPT

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The objective of this work is to develop a simple, accurate, precise and validated RP-UPLC method for effective simultaneous determination of nirmatrelvir and ritonavir in bulk and copacked tablet formulation. Separation of drugs was optimized after several trials by changing mobile phase composition, stationary phase, flow rate and column temperature. Finally the separation of drugs was achieved on a phenyl column (100 x 2.1 mm, 1.7 µ) using isocratic elution with a mobile phase of acetonitrile and triethyl amine (30:70 v/v). A flow rate of 0.5 mL/min. and a detector wavelength of 267 nm utilizing the PDA detector were given in the instrumental settings. Validation of the proposed method was carried out according to the International Council for Harmonization (ICH) guidelines. The system suitability parameters were within the limits, the retention time (Rt) for nirmatrelvir and ritonavir was achieved at 1.262 min. and 1.873 min. respectively over a total runtime of five minutes. The method showed linearity between the concentration range of 37.5-225 µg/mL for nirmatrelvir (R² = 0.99956) and 25-150 µg/mL of ritonavir (R² = 0.9998). The percentage recovery results by standard addition method for nirmatrelvir and ritonavir were found to be in the range of 99.3 % - 100.3 %. The proposed method is specific, accurate and robust. During stability tests, it can be used for routine analysis of the selected drugs.

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Development and Validation of RP-HPLC Method for Quantification of Total, Free and Entrapped Ritonavir in Lipid Nanocarriers and Drug content of Film Coated Fixed Dose Formulation

Cited by 4 publications

References 22 publications

Quality-by-design driven analytical method (AQbD) development and validation of HPLC–UV technique to quantify rivastigmine hydrogen tartrate in lipidic nanocarriers: Forced degradation, and assessment of drug content and in vitro release studies

Quality-by-design driven analytical method (AQbD) development and validation of HPLC–UV technique to quantify rivastigmine hydrogen tartrate in lipidic nanocarriers: Forced degradation, and assessment of drug content and in vitro release studies

Development and Validation of a Methodology for the Analysis of Ritonavir and Lopinavir in Combined Dosage Form by High-Performance Liquid Chromatography

Development and validation of a new RP-UPLC method for the simultaneous estimation of nirmatrelvir and ritonavir in bulk and copacked tablet dosage forms

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