Pharmacodynamic Study of Parallel Groups Comparing the Effect of Rivaroxaban 20 Mg (Laboratorios Leti, S.A.V.) vs Rivaroxaban 20 Mg (Bayer Laboratories) on Prothrombin Time
Background: The prevalence of both atrial fibrillation (FA) and diabetes mellitus (DM) is increasing and they often occur together and constitute a high risk of thrombosis. Rivaroxaban is a Factor Xa inhibitor with a rapid onset and disappearance of action after oral administration; it acts by inhibiting the active form of the coagulation factor. In order to reflect the effect of the action of Rivaroxaban, we used the prothrombin time (PT); however, it′s not the most accurate, but it is the one available in our community. Methods: This was a prospective, randomized, analyst-blinded, parallel group clinical study to verify the efficacy of Rivaroxaban Leti 20 mg (RL) (12 volunteers vs Rivaroxaban Bayer 20 mg (RB) (13 volunteers). The variables were determination of PT and Partial Thromboplastin Time (aPTT) at baseline and at 24, 48 and 72 hours after administering a daily dose of 20 mg for three days. The determination was carried out with the IDG method (Integrated Diagnostics Group Sanzay Corporation) with an International Sensitivity Index (ISI) of 1.17 PT and aPTT were taken before the first dose, and then, every day during the next 3 days, three hours after the ingestion of their daily dose at 7 am. Results: The 25 healthy volunteers were similar in age, BMI, and SBP/DBP level with a greater number of men in the Bayer group. The efficacy of rivaroxaban was similar in both groups with prolongation of PTT to the 2nd day of treatment with PT, and percentage changes from baseline (14.46 ± 0.97 for RB vs 14.17 ± 0.94 RL p: 0.45), PTT results and percentage changes from the base (RB: 34 ± 4.53 RL: 33.46 ± 2.82). The safety of rivaroxaban was good in both groups with no serious adverse events. The equivalence in the logarithmically transformed PT result (ln) on day two, Mean and CI (90%) 99.2 (94.4-104) and 100 (99.5-100.8); neither the means nor the 90% confidence intervals of the PT variable transformed logarithmically to ensure its normality, were far from the 80%-125% allowed for declaration of similarity. Conclusion: The test formulation Rivaroxaban Asarap? 20 mg, manufactured by Leti Laboratories, is interchangeable or bioequivalent in clinical and laboratory response to the reference formulation Xarelto? manufactured by Bayer Laboratories.
References
[1]
López-Santiago, N. (2016) Pruebas De Coagulación. Acta Pediátrica De México, 37, 241-245. https://doi.org/10.18233/APM37No4pp241-245
[2]
Konkle, B.A. (2016) Direct Oral Anticoagulants Monitoring Anticoagulant Effect. Hematology/Oncology Clinics of North America, 30, 995-1006. https://doi.org/10.1016/j.hoc.2016.05.004
[3]
Tripodi, A., Chantarangkul, V., Guinet, C. and Samama, M.M. (2011) The International Normalized Ratio Calibrated for Rivaroxaban Has the Potential to Normalize Prothrombin Time Results for Rivaroxaban-Treated Patients Results of an in Vitro Study. Journal of Thrombosis and Haemostasis, 9, 226-228. https://doi.org/10.1111/j.1538-7836.2010.04106.x
[4]
WHO/BS/2016.2294 Calibration of the Proposed 5th IS for Thromboplastin, Human, Recombinant, Plain (rTF/16; Study Code 14/001) and the Proposed 5th IS for Thromboplastin, Rabbit, Plain (RBT/16; study code 15/001).
[5]
Retamales Castelletto, E. and Moscoso Espinoza, H. (2021) Recomendaciones para la etapa pre-analítica, analítica y post-analítica en las pruebas de coagulación. Departamento Laboratorio Biomédico Nacional y de Referencia. Instituto de Salud Pública de Chile.
[6]
Perzborn, E., Roehrig, S., Straub, A., Kubitza, D. and Misselwitz, F. (2011) The Discovery and Development of Rivaroxaban, an Oral, Direct Factor Xa Inhibitor. Nature Reviews Drug Discovery, 10, 61-75. https://doi.org/10.1038/nrd3185
[7]
Xarelto, INN-rivaroxaban. Summary of Product Characteristics 2013. https://ec.europa.eu/health/documents/community-register/2013/20130805126532/anx_126532_en.pdf
[8]
Kreutz, R. (2012) Pharmacodynamic and Pharmacokinetic Basics of Rivaroxaban. Fundamental & Clinical Pharmacology, 26, 27-32. https://doi.org/10.1111/j.1472-8206.2011.00981.x
[9]
Mueck, W., Stampfuss, J., Kubitza, D. and Becka, M. (2014) Clinical Pharmacokinetic and Pharmacodynamic Profile of Rivaroxaban. Clinical Pharmacokinetics, 53, 1-16. https://doi.org/10.1007/s40262-013-0100-7
[10]
Samama, M.M., Contant, G., Spiro, T.E., Perzborn, E., Le Flem, L., Guinet, C., Gourmelin, Y., Rohde, G. and Martinoli, J.L. (2013) Laboratory Assessment of Rivaroxaban: A Review. Thrombosis Journal, 11, Article No. 11. https://doi.org/10.1186/1477-9560-11-11
[11]
Kubitza, D., Becka, M., Voith, B., Zuehlsdorf, M. and Wensing, G. (2005) Safety, Pharmacodynamics, and Pharmacokinetics of Single Doses of Bay 59-7939, an Oral, Direct Factor Xa Inhibitor. Clinical Pharmacology & Therapeutics, 78, 412-421. https://doi.org/10.1016/j.clpt.2005.06.011
[12]
Mueck, W., Lensing, A.W., Agnelli, G., Decousus, H., Prandoni, P. and Misselwitz, F. (2011) Rivaroxaban: Population Pharmacokinetic Analyses in Patients Treated for Acute Deep-Vein Thrombosis and Exposure Simulations in Patients with Atrial Fibrillation Treated for Stroke Prevention. Clinical Pharmacokinetics, 50, 675-686. https://doi.org/10.2165/11595320-000000000-00000
[13]
Mueck, W., Eriksson, B.I., Bauer, K.A., Borris, L., Dahl, O.E., Fisher, W.D., Gent, M., Haas, S., Huisman, M.V., Kakkar, A.K., Kalebo, P., Kwong, L.M., Misselwitz, F. and Turpie, A.G. (2008) Population Pharmacokinetics and Pharmacodynamics of Rivaroxaban—An Oral, Direct Factor Xa Inhibitor—In Patients Undergoing Major Orthopaedic Surgery. Clinical Pharmacokinetics, 47, 203-216. https://doi.org/10.2165/00003088-200847030-00006
[14]
Kubitza, D., Becka, M., Wensing, G., Voith, B. and Zuehlsdorf, M. (2005) Safety, Pharmacodynamics, and Pharmacokinetics Of Bay 59-7939—An Oral, Direct Factor Xa Inhibitor—After Multiple Dosing in Healthy Male Subjects. European Journal of Clinical Pharmacology, 61, 873-880. https://doi.org/10.1007/s00228-005-0043-5
[15]
Kubitza, D., Becka, M., Roth, A. and Mueck, W. (2008) Dose-Escalation Study of the Pharmacokinetics and Pharmacodynamics of Rivaroxaban in Healthy Elderly Subjects. Current Medical Research and Opinion, 24, 2757-2765. https://doi.org/10.1185/03007990802361499
[16]
Weinz, C., Schwarz, T., Kubitza, D., Mueck, W. and Lang, D. (2009) Metabolism and Excretion of Rivaroxaban, an Oral, Direct Factor Xa Inhibitor, in Rats, Dogs and Humans. Drug Metabolism & Disposition, 37, 1056-1064. https://doi.org/10.1124/dmd.108.025569
[17]
Mueck, W., Schwers, S. and Stampfuss, J. (2013) Rivaroxaban and Other Novel Oral Anticoagulants: Pharmacokinetics in Healthy Subjects, Specific Patient Populations and Relevance of Coagulation Monitoring. Thrombosis Journal, 11, Article No. 10. https://doi.org/10.1186/1477-9560-11-10
[18]
Ding, S.J., Wang, L., Xie, L.J., Zhou, S.F., Chen, J., Zhao, Y.Q., Deng, W.J., Liu, Y., Zhang, H.W. and Shao, F. (2020) Bioequivalence Study of 2 Formulations of Rivaroxaban, a Narrow-Therapeutic-Index Drug, in Healthy Chinese Subjects Under Fasting and Fed Conditions. Clinical Pharmacology in Drug Development, 9, 346-352. https://doi.org/10.1002/cpdd.742
[19]
Genis-Najera, L., Sañudo-Maury, M.E. and Moquete, T. (2022) A Single-Blind, Randomized, Single-Dose, Two-Sequence, Two-Period, Crossover Study to Assess the Bioequivalence between Two Oral Tablet Formulations of Rivaroxaban 20 mg in Healthy Mexican Volunteers. Clinical Pharmacology in Drug Development, 11, 826-831. https://doi.org/10.1002/cpdd.1092
[20]
Pena, E., Inatti, A. and Martin, X.S. (2023) Bioequivalence Study of Two Formulations of Rivaroxaban in Healthy Adult Subjects under Fasting Conditions. American Journal of Pharmacotherapy and Pharmaceutical Sciences, 2, Article No. 8. https://doi.org/10.25259/AJPPS_2023_008
