Infliximab Dosing Strategies and Predicted Trough Exposure in Children With Crohn Disease

Frymoyer, Adam; Piester, Travis L.; Park, K.T.

doi:10.1097/mpg.0000000000001123

Cited by 36 publications

(32 citation statements)

References 27 publications

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“…The trough levels during induction were higher during 2016, and it is very likely that this reflects a change in clinical practice during this period, as studies carried out around this time reported better responses in young children with higher doses. 16,17 Disappointingly, although the trough levels during induction were higher, we did not observe any increase in the proportion of patients that maintained their therapeutic response. There were no major adverse events during the study period, no alarming signs and no acute infusion reactions with either of these drugs.…”

Section: Discussioncontrasting

confidence: 62%

Infliximab and its biosimilar produced similar first‐year therapy outcomes in patients with inflammatory bowel disease

Nikkonen

Kolho

2019

Acta Paediatrica

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Aim Tumour necrosis factor α inhibitors (anti‐TNFα) are the main therapy for moderate to severe inflammatory bowel disease (IBD) in children. Biosimilars to the original drug infliximab are now available, but there are few reports on their real‐life use. We compared the outcomes of patients treated with infliximab and its biosimilar, CT‐P13. Methods We collected outcome data on anti‐TNFα‐naive patients who started infliximab in the Children's Hospital, University of Helsinki, Finland, in 2015‐2016. We studied 51 paediatric patients with IBD at a median age of 12 (range 4‐16): 65% had Crohn disease, 23 received the original infliximab drug and 28 received the biosimilar. During 2015, infliximab was introduced to all treatment‐naïve patients, and during 2016, all treatment‐naïve patients received the biosimilar. Results We found no statistically significant differences between the two drug products related to the outcome of the therapy during the first year. There were no significant differences in the trough levels between the treatment groups. Likewise, the proportion of patients with therapy enhancement was comparable between the two treatment groups. Conclusion The first‐year therapy outcomes of infliximab and its biosimilar were comparable. There were no alarming signs of differences in safety.

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Section: Discussioncontrasting

confidence: 62%

Infliximab and its biosimilar produced similar first‐year therapy outcomes in patients with inflammatory bowel disease

Nikkonen

Kolho

2019

Acta Paediatrica

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“…The pharmacokinetics of infliximab are highly variable in this population and consequently dose requirements will vary between patients. (3,11) In the cohort of children examined in the current study, the predicted infliximab maintenance dosing strategy needed to achieve a trough concentration >3 μg/ml was quite heterogeneous and ranged from the standard dosing of 5 mg/kg every 8 weeks up to 5 mg/kg every 4 weeks (Figure 3A). Our cohort was homogenous in terms of serum albumin (only 1 patient had a serum albumin < 3.5), and serum albumin is the most influential predictor of infliximab clearance and trough achievement.…”

Section: Discussionmentioning

confidence: 99%

“…Our cohort was homogenous in terms of serum albumin (only 1 patient had a serum albumin < 3.5), and serum albumin is the most influential predictor of infliximab clearance and trough achievement. (11) Even greater heterogeneity in dose needs will likely be present in a larger, more diverse population. In addition, we demonstrated the potential challenges of achieving trough concentrations >3 μg/ml with even the most aggressive dosing (i.e.…”

Section: Discussionmentioning

confidence: 99%

“…(11) Higher infliximab doses and/or shorter dosing intervals were predicted to be needed to consistently achieve a trough concentration >3 μg/ml during maintenance dosing. Similarly, a prospective observational study found that 44% (n=10/23) of children with Crohn's disease had a trough concentration <3 μg/ml when receiving standard infliximab maintenance dosing of 5 mg/kg every 8 weeks.…”

Section: Introductionmentioning

confidence: 99%

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Application of Population Pharmacokinetic Modeling for Individualized Infliximab Dosing Strategies in Crohn Disease

Frymoyer

Hoekman

Piester

et al. 2017

Journal of Pediatric Gastroenterology &Amp; Nutrition

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Objectives The pharmacokinetics of infliximab are highly variable in children with Crohn's disease (CD), and a one-size-fits-all approach to dosing is inadequate. Model-based drug dosing can help individualize dosing strategies. We evaluated the predictive performance and clinical utility of a published population pharmacokinetic model of infliximab in children with CD. Methods Within a cohort of 34 children with CD who had infliximab trough concentrations measured, the pharmacokinetics of each patient was estimated in NONMEM® using a published population pharmacokinetic model. Infliximab concentrations were then predicted based on each patient's dosing history and compared to actual measured concentrations (n=59). In addition, doses 5-10 mg/kg and dosing intervals every 4-8 weeks were simulated in each patient to examine dose-trough relationships. Results Predicted concentrations were within ±1.0 μg/ml of actual measured concentrations for 88% of measurements. The median prediction error (i.e. measure of bias) was -0.15 μg/ml (95%CI: -0.37 to -0.05 μg/ml) and absolute prediction error (i.e. measure of precision) was 0.26 μg/ml (95%CI: 0.15 to 0.40 μg/ml). At standard maintenance dosing of 5 mg/kg every 8 weeks, a trough >3 μg/ml was predicted to be achieved in 32% of patients. To achieve a trough >3 μg/ml, a dosing interval ≤ every 6 weeks was predicted to be required in 29% of patients. Conclusions A published infliximab population pharmacokinetic model demonstrated accurate predictive performance in a pediatric CD population. Individualized infliximab dosing strategies in children with CD will be critical to consistently achieve trough concentrations associated with optimal outcomes.

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“…For example, reliance on adult dosing in children with Crohn's disease can lead to less than 41% probability of adequate drug exposure. 24 Such significant discrepancies in drug clearance profiles between children and adults can result in early drug failure and worse outcomes for children with IBD. 24 Choosing the correct pharmacotherapy and targeting pharmacotherapy in an evidencebased way is critical to ensuring appropriate patient care aimed at optimizing future health gains.…”

Section: Second Challenge: Optimization Of Targeted Pharmacotherapymentioning

confidence: 99%

Targeted Dosing as a Precision Health Approach to Pharmacotherapy in Children with Inflammatory Bowel Disease

Wren

Park

2018

AMA Journal of Ethics

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Infliximab Dosing Strategies and Predicted Trough Exposure in Children With Crohn Disease

Cited by 36 publications

References 27 publications

Infliximab and its biosimilar produced similar first‐year therapy outcomes in patients with inflammatory bowel disease

Infliximab and its biosimilar produced similar first‐year therapy outcomes in patients with inflammatory bowel disease

Application of Population Pharmacokinetic Modeling for Individualized Infliximab Dosing Strategies in Crohn Disease

Targeted Dosing as a Precision Health Approach to Pharmacotherapy in Children with Inflammatory Bowel Disease

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