Extensive preclinical evaluation of an infliximab biosimilar candidate

M. A. Velasco-Velázquez; N. Salinas-Jazmín; E. Hisaki-Itaya; L. Cobos-Puc; W. Xolalpa; G. González; A. Tenorio-Calvo; N. Piña-Lara; L. C. Juárez-Bayardo; L. F. Flores-Ortiz; E. Medina-Rivero; N. O. Pérez; S. M. Pérez-Tapia

doi:10.1016/j.ejps.2017.01.038

Extensive preclinical evaluation of an infliximab biosimilar candidate

M. A. Velasco-Velázquez, N. Salinas-Jazmín, E. Hisaki-Itaya, L. Cobos-Puc, W. Xolalpa, G. González, A. Tenorio-Calvo, N. Piña-Lara, L. C. Juárez-Bayardo, L. F. Flores-Ortiz, E. Medina-Rivero, N. O. Pérez, S. M. Pérez-Tapia

Escuela Nacional de Ciencias Biológicas (ENCB)

Producción científica: Contribución a una revista › Artículo › revisión exhaustiva

7 Citas (Scopus)

Resumen

Infliximab is therapeutic monoclonal antibody (mAb) against TNF-α employed in the treatment of immunoinflammatory diseases. The development of biosimilar mAbs is a global strategy to increase drug accessibility and reduce therapy-associated costs. Herein we compared key physicochemical characteristics and biological activities produced by infliximab and infliximab-Probiomed in order to identify functionally relevant differences between the mAbs. Binding of infliximab-Probiomed to TNF-α was specific and had kinetics comparable to that of the reference product. Both mAbs had highly similar neutralizing efficacy in HUVEC cell cultures stimulated with TNF-α. In vitro induction of CDC and ADCC were also similar between the evaluated products. In vivo comparability was assessed using a transgenic mouse model of arthritis that expresses human TNF-α in a 13-week multiple-administration study. Infliximab and infliximab-Probiomed showed comparable efficacy, safety, and pharmacokinetic profiles. Our results indicate that infliximab-Probiomed has highly similar activities to infliximab in preclinical models, warranting a clinical evaluation of its biosimilarity.

Idioma original	Inglés
Páginas (desde-hasta)	35-45
Número de páginas	11
Publicación	European Journal of Pharmaceutical Sciences
Volumen	102
DOI	https://doi.org/10.1016/j.ejps.2017.01.038
Estado	Publicada - 1 may. 2017

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Velasco-Velázquez, M. A., Salinas-Jazmín, N., Hisaki-Itaya, E., Cobos-Puc, L., Xolalpa, W., González, G., Tenorio-Calvo, A., Piña-Lara, N., Juárez-Bayardo, L. C., Flores-Ortiz, L. F., Medina-Rivero, E., Pérez, N. O., & Pérez-Tapia, S. M. (2017). Extensive preclinical evaluation of an infliximab biosimilar candidate. European Journal of Pharmaceutical Sciences, 102, 35-45. https://doi.org/10.1016/j.ejps.2017.01.038

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title = "Extensive preclinical evaluation of an infliximab biosimilar candidate",

abstract = "Infliximab is therapeutic monoclonal antibody (mAb) against TNF-α employed in the treatment of immunoinflammatory diseases. The development of biosimilar mAbs is a global strategy to increase drug accessibility and reduce therapy-associated costs. Herein we compared key physicochemical characteristics and biological activities produced by infliximab and infliximab-Probiomed in order to identify functionally relevant differences between the mAbs. Binding of infliximab-Probiomed to TNF-α was specific and had kinetics comparable to that of the reference product. Both mAbs had highly similar neutralizing efficacy in HUVEC cell cultures stimulated with TNF-α. In vitro induction of CDC and ADCC were also similar between the evaluated products. In vivo comparability was assessed using a transgenic mouse model of arthritis that expresses human TNF-α in a 13-week multiple-administration study. Infliximab and infliximab-Probiomed showed comparable efficacy, safety, and pharmacokinetic profiles. Our results indicate that infliximab-Probiomed has highly similar activities to infliximab in preclinical models, warranting a clinical evaluation of its biosimilarity.",

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Velasco-Velázquez, MA, Salinas-Jazmín, N, Hisaki-Itaya, E, Cobos-Puc, L, Xolalpa, W, González, G, Tenorio-Calvo, A, Piña-Lara, N, Juárez-Bayardo, LC, Flores-Ortiz, LF, Medina-Rivero, E, Pérez, NO & Pérez-Tapia, SM 2017, 'Extensive preclinical evaluation of an infliximab biosimilar candidate', European Journal of Pharmaceutical Sciences, vol. 102, pp. 35-45. https://doi.org/10.1016/j.ejps.2017.01.038

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T1 - Extensive preclinical evaluation of an infliximab biosimilar candidate

AU - Velasco-Velázquez, M. A.

AU - Salinas-Jazmín, N.

AU - Hisaki-Itaya, E.

AU - Cobos-Puc, L.

AU - Xolalpa, W.

AU - González, G.

AU - Tenorio-Calvo, A.

AU - Piña-Lara, N.

AU - Juárez-Bayardo, L. C.

AU - Flores-Ortiz, L. F.

AU - Medina-Rivero, E.

AU - Pérez, N. O.

AU - Pérez-Tapia, S. M.

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N2 - Infliximab is therapeutic monoclonal antibody (mAb) against TNF-α employed in the treatment of immunoinflammatory diseases. The development of biosimilar mAbs is a global strategy to increase drug accessibility and reduce therapy-associated costs. Herein we compared key physicochemical characteristics and biological activities produced by infliximab and infliximab-Probiomed in order to identify functionally relevant differences between the mAbs. Binding of infliximab-Probiomed to TNF-α was specific and had kinetics comparable to that of the reference product. Both mAbs had highly similar neutralizing efficacy in HUVEC cell cultures stimulated with TNF-α. In vitro induction of CDC and ADCC were also similar between the evaluated products. In vivo comparability was assessed using a transgenic mouse model of arthritis that expresses human TNF-α in a 13-week multiple-administration study. Infliximab and infliximab-Probiomed showed comparable efficacy, safety, and pharmacokinetic profiles. Our results indicate that infliximab-Probiomed has highly similar activities to infliximab in preclinical models, warranting a clinical evaluation of its biosimilarity.

AB - Infliximab is therapeutic monoclonal antibody (mAb) against TNF-α employed in the treatment of immunoinflammatory diseases. The development of biosimilar mAbs is a global strategy to increase drug accessibility and reduce therapy-associated costs. Herein we compared key physicochemical characteristics and biological activities produced by infliximab and infliximab-Probiomed in order to identify functionally relevant differences between the mAbs. Binding of infliximab-Probiomed to TNF-α was specific and had kinetics comparable to that of the reference product. Both mAbs had highly similar neutralizing efficacy in HUVEC cell cultures stimulated with TNF-α. In vitro induction of CDC and ADCC were also similar between the evaluated products. In vivo comparability was assessed using a transgenic mouse model of arthritis that expresses human TNF-α in a 13-week multiple-administration study. Infliximab and infliximab-Probiomed showed comparable efficacy, safety, and pharmacokinetic profiles. Our results indicate that infliximab-Probiomed has highly similar activities to infliximab in preclinical models, warranting a clinical evaluation of its biosimilarity.

KW - Biosimilar

KW - Infliximab

KW - Rheumatoid arthritis

KW - TNF-α

KW - Therapeutic mAb

KW - anti-TNF-α

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U2 - 10.1016/j.ejps.2017.01.038

DO - 10.1016/j.ejps.2017.01.038

M3 - Artículo

C2 - 28188909

AN - SCOPUS:85014178291

SN - 0928-0987

VL - 102

SP - 35

EP - 45

JO - European Journal of Pharmaceutical Sciences

JF - European Journal of Pharmaceutical Sciences

ER -

Extensive preclinical evaluation of an infliximab biosimilar candidate

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