The performance of Remicade®-optimized quantification assays in the assessment of Flixabi® levels

The performance of Remicade®-optimized quantification assays in the assessment of Flixabi® levels

Background: The advent of Remicade® biosimilars, Remsima®, Inflectra® and, more recently, Flixabi®, has brought along the potential to decrease the costs associated with this therapy, therefore increasing its access to a larger group of patients. However, and in order to assure a soft transition, on...

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Main Authors: F. Magro, C. Rocha, A. I. Vieira, H. T. Sousa, I. Rosa, S. Lopes, J. Carvalho, C. C. Dias, J. Afonso
Format: Article
Language:English
Published: SAGE Publishing 2018-09-01
Series:Therapeutic Advances in Gastroenterology
Online Access:https://doi.org/10.1177/1756284818796956
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spelling doaj-dd4c90c518cc4b74ab6f26e1d1ed28c22020-11-25T03:15:33ZengSAGE PublishingTherapeutic Advances in Gastroenterology1756-28482018-09-011110.1177/1756284818796956The performance of Remicade®-optimized quantification assays in the assessment of Flixabi® levelsF. MagroC. RochaA. I. VieiraH. T. SousaI. RosaS. LopesJ. CarvalhoC. C. DiasJ. AfonsoBackground: The advent of Remicade® biosimilars, Remsima®, Inflectra® and, more recently, Flixabi®, has brought along the potential to decrease the costs associated with this therapy, therefore increasing its access to a larger group of patients. However, and in order to assure a soft transition, one must make sure the assays and algorithms previously developed and optimized for Remicade perform equally well with its biosimilars. This study aimed to: (a) validate the utilization of Remicade-optimized therapeutic drug monitoring assays for the quantification of Flixabi; and (b) determine the existence of Remicade, Remsima and Flixabi cross-immunogenicity. Methods: Healthy donors’ sera spiked with Remicade, Remsima and Flixabi were quantified using three different Remicade-quantification assays, and the reactivity of anti-Remicade and anti-Remsima sera to Remicade and to its biosimilars was assessed. Results: The results show that all tested Remicade-infliximab-optimized assays measure Flixabi as accurately as they measure Remicade and Remsima: the intraclass correlation coefficients between theoretical and measured concentrations varied from 0.920 to 0.990. Moreover, the interassay agreement values for the same compounds were high (intraclass correlation coefficients varied from 0.936 to 0.995). Finally, the anti-Remicade and anti-Remsima sera reacted to the different drugs in a similar fashion. Conclusions: The tested assays can be used to monitor Flixabi levels. Moreover, Remicade, Remsima and Flixabi were shown to have a high cross-immunogenicity, which supports their high similarity but prevents their switching in nonresponders with antidrug antibodies.https://doi.org/10.1177/1756284818796956
collection DOAJ
language English
format Article
sources DOAJ
author F. Magro
C. Rocha
A. I. Vieira
H. T. Sousa
I. Rosa
S. Lopes
J. Carvalho
C. C. Dias
J. Afonso
spellingShingle F. Magro
C. Rocha
A. I. Vieira
H. T. Sousa
I. Rosa
S. Lopes
J. Carvalho
C. C. Dias
J. Afonso
The performance of Remicade®-optimized quantification assays in the assessment of Flixabi® levels
Therapeutic Advances in Gastroenterology
author_facet F. Magro
C. Rocha
A. I. Vieira
H. T. Sousa
I. Rosa
S. Lopes
J. Carvalho
C. C. Dias
J. Afonso
author_sort F. Magro
title The performance of Remicade®-optimized quantification assays in the assessment of Flixabi® levels
title_short The performance of Remicade®-optimized quantification assays in the assessment of Flixabi® levels
title_full The performance of Remicade®-optimized quantification assays in the assessment of Flixabi® levels
title_fullStr The performance of Remicade®-optimized quantification assays in the assessment of Flixabi® levels
title_full_unstemmed The performance of Remicade®-optimized quantification assays in the assessment of Flixabi® levels
title_sort performance of remicade®-optimized quantification assays in the assessment of flixabi® levels
publisher SAGE Publishing
series Therapeutic Advances in Gastroenterology
issn 1756-2848
publishDate 2018-09-01
description Background: The advent of Remicade® biosimilars, Remsima®, Inflectra® and, more recently, Flixabi®, has brought along the potential to decrease the costs associated with this therapy, therefore increasing its access to a larger group of patients. However, and in order to assure a soft transition, one must make sure the assays and algorithms previously developed and optimized for Remicade perform equally well with its biosimilars. This study aimed to: (a) validate the utilization of Remicade-optimized therapeutic drug monitoring assays for the quantification of Flixabi; and (b) determine the existence of Remicade, Remsima and Flixabi cross-immunogenicity. Methods: Healthy donors’ sera spiked with Remicade, Remsima and Flixabi were quantified using three different Remicade-quantification assays, and the reactivity of anti-Remicade and anti-Remsima sera to Remicade and to its biosimilars was assessed. Results: The results show that all tested Remicade-infliximab-optimized assays measure Flixabi as accurately as they measure Remicade and Remsima: the intraclass correlation coefficients between theoretical and measured concentrations varied from 0.920 to 0.990. Moreover, the interassay agreement values for the same compounds were high (intraclass correlation coefficients varied from 0.936 to 0.995). Finally, the anti-Remicade and anti-Remsima sera reacted to the different drugs in a similar fashion. Conclusions: The tested assays can be used to monitor Flixabi levels. Moreover, Remicade, Remsima and Flixabi were shown to have a high cross-immunogenicity, which supports their high similarity but prevents their switching in nonresponders with antidrug antibodies.
url https://doi.org/10.1177/1756284818796956
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