Influence of Trough Serum Levels and Immunogenicity on Long-term Outcome of Adalimumab Therapy in Crohn's Disease
Background & Aims
Adalimumab is an efficacious therapy for active Crohn's disease, but long-term data are scarce. We conducted an observational study to assess the long-term clinical benefit of adalimumab in patients who failed to respond to infliximab, specifically focusing on the influence of trough serum concentration and antibodies against adalimumab on clinical outcome.
Methods
A total of 168 patients with Crohn's disease treated with adalimumab in a tertiary center were included in a prospective follow-up program. Trough serum concentration and antibodies against adalimumab were measured at predefined time points using enzyme-linked immunosorbent assays.
Results
A total of 71% and 67% of patients responded by weeks 4 and 12, respectively; among them, 61.5% demonstrated sustained clinical benefit until the end of follow-up (median [interquartile range], 20.4 [11.7–30.0] months). Of the 156 patients receiving maintenance therapy, 102 (65.4%) had to step up to 40 mg weekly and 60 (38.5%) eventually stopped adalimumab therapy mainly due to loss of response. Significantly lower adalimumab trough serum concentrations were measured throughout the follow-up period in patients who discontinued therapy as compared with patients who stayed on adalimumab. Antibodies against adalimumab were present in 9.2% of the patients and affected trough serum concentration. Serious adverse events occurred in 12% of the patients.
Conclusions
Introduction of adalimumab after failure of infliximab therapy resulted in a sustained clinical benefit in two thirds of patients during a median follow-up period of almost 2 years. Discontinuation was directly related to low adalimumab trough serum concentration, which was observed more frequently in patients who developed antibodies against adalimumab.
Abbreviations used in this paper: CRP, C-reactive protein, IQR, interquartile range, OR, odds ratio, SAE, severe adverse events, TNF, tumor necrosis factor
This article has an accompanying continuing medical education activity on page 1836. Learning Objective: Upon completion of this examination, successful learners will be able to interpret the role of immunogenicity in the use of biologic agents in inflammatory bowel diseases.
Conflicts of interest The authors disclose the following: Dr Paintaud is on an advisory committee for Roche, has a research contract with Innate Pharma, is a consultant for LFB, and receives a speaker fee from Pierre Fabre; Dr Van Assche receives a speaker fee/research support from Centocor, Schering-Plough, Abbott, and UCB; Dr Vermeire receives grants/research support from UCB; is a consultant for AstraZeneca, Ferring, and Pfizer; is on the speakers bureau for Schering-Plough, Abbott, Ferring, and UCB; and is on an advisory committee for Shire and Ferring; and Dr Rutgeerts receives research grants, lecture fees, and consultant fees from Abbott, Centocor, Schering-Plough, and UCB. The remaining authors disclose no conflicts.
Funding Supported by a grant from European Crohn's and Colitis Organisation and the Hellenic Society of Gastroenterology.
PII: S0016-5085(09)01387-0
doi:10.1053/j.gastro.2009.07.062
© 2009 AGA Institute. Published by Elsevier Inc. All rights reserved.
Refers to article:
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Timing of Myelosuppression During Thiopurine Therapy for Inflammatory Bowel Disease: Implications for Monitoring Recommendations
, 23 July 2009