Pharmacokinetics, Pharmacodynamics, and Immunogenicity of Infliximab in Pediatric Inflammatory Bowel Disease

Winter, D.A.; Joosse, Maria E.; Taminiau, J. A. J. M.; Ridder, Lissy de; Escher, Johanna C.

doi:10.1097/mpg.0000000000002631

Cited by 30 publications

(30 citation statements)

References 86 publications

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“…However, half of the patients required an increased dose or a shortened dosing interval to maintain a clinical response 29 . While the dose adjustments in the REACH trial were based on clinical evaluation and response, a target trough concentration of 3 to 5 μg/mL was soon identified for therapeutic drug monitoring in practice 30–32 . Revisiting the original analyses by Fasanmade et al revealed that 60% of children would achieve subtherapeutic trough concentrations with the labeled dose 33 .…”

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confidence: 99%

“…The European Society for Paediatric Gastroenterology Hepatology and Nutrition subsequently revised their recommendations and advocates for up‐front intensification of the induction regimen for children <10 years of age 31 . Results of a systematic review further suggest that dose increases are necessary for all pediatric patients with inflammatory bowel disease with low serum albumin or with no concurrent immunomodulator therapy 32 . In retrospect, it can be concluded that the adult weight‐based dosing was not appropriate for the pediatric label 32 …”

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confidence: 99%

“…Results of a systematic review further suggest that dose increases are necessary for all pediatric patients with inflammatory bowel disease with low serum albumin or with no concurrent immunomodulator therapy 32 . In retrospect, it can be concluded that the adult weight‐based dosing was not appropriate for the pediatric label 32 …”

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Pediatric Dose Selection for Therapeutic Proteins

Malik

Temrikar

Chelle

et al. 2021

The Journal of Clinical Pharma

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In selecting optimal dosing regimens in support of the clinical use of monoclonal antibodies and other therapeutic proteins in pediatric indications, the unique pharmacokinetic properties of this class of biologics, as well as the underlying physiologic and pathophysiologic processes and their modulation by childhood growth and development, needs to be appreciated. During drug development, first‐in‐pediatric dose selection is a capstone event in the pediatric investigation plan that relies heavily on extrapolation of pharmacokinetic and pharmacodynamic data from adult to pediatric populations. It is facilitated by combinations of pharmacometric approaches, including allometry, physiologically based pharmacokinetic modeling, and population pharmacokinetic analyses, although data on reliability and qualification of some of these tools in the context of therapeutic proteins are still limited but emerging. Presented data suggest nonlinear relationships between body weight and both clearance and volume of distribution for therapeutic proteins in pediatric populations, with allometric exponents of 0.75 and 0.8, respectively. For newborns and infants (<1 year), even higher nonlinearity seems to occur. Translation of the quantitative characterization of the pediatric pharmacokinetics of therapeutic proteins into dosing regimens for the drug label requires compromising between precision dosing and clinical practicability, with tiered dosing algorithms based on size or age strata being the currently most frequently applied methodology.

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Pediatric Dose Selection for Therapeutic Proteins

Malik

Temrikar

Chelle

et al. 2021

The Journal of Clinical Pharma

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“…Furthermore, only patients with IBD had detectable ADAs in our cohort, begging the question whether the real-world dosing practices observed in our IBD cohort (median [IQR] of 7.7 [6.2,9.4] mg/kg every 6 [4,8] weeks) are adequate to prevent loss of treatment response to IFX. Two other recent analyses have similarly questioned the adequacy of standard 5 mg/kg IFX dosing every 8 weeks for pediatric IBD, advocating for treat-to-target approaches for IFX [25,26]. No patients with uveitis or JIA had ADAs or trough levels < 5 μg/mL, however, unlike IBD, there are no established IFX therapeutic trough targets currently utilized for JIA or uveitis.…”

Section: Discussionmentioning

confidence: 99%

Factors associated with reduced infliximab exposure in the treatment of pediatric autoimmune disorders: a cross-sectional prospective convenience sampling study

et al. 2021

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Background Inadequate systemic exposure to infliximab (IFX) is associated with treatment failure. This work evaluated factors associated with reduced IFX exposure in children with autoimmune disorders requiring IFX therapy. Methods In this single-center cross-sectional prospective study IFX trough concentrations and anti-drug antibodies (ADAs) were measured in serum from children diagnosed with inflammatory bowel disease (IBD) (n = 73), juvenile idiopathic arthritis (JIA) (n = 16), or uveitis (n = 8) receiving maintenance IFX infusions at an outpatient infusion clinic in a tertiary academic pediatric hospital. IFX concentrations in combination with population pharmacokinetic modeling were used to estimate IFX clearance. Patient demographic and clinical data were collected by chart review and evaluated for their relationship with IFX clearance. Results IFX trough concentrations ranged from 0 to > 40 μg/mL and were 3-fold lower in children with IBD compared to children with JIA (p = 0.0002) or uveitis (p = 0.001). Children with IBD were found to receive lower IFX doses with longer dosing intervals, resulting in dose intensities (mg/kg/day) that were 2-fold lower compared to children with JIA (p = 0.0002) or uveitis (p = 0.02). Use of population pharmacokinetic analysis to normalize for variation in dosing practices demonstrated that increased IFX clearance was associated with ADA positivity (p = 0.004), male gender (p = 0.02), elevated erythrocyte sedimentation rate (ESR) (p = 0.02), elevated c-reactive protein (CRP) (p = 0.001), reduced serum albumin concentrations (p = 0.0005), and increased disease activity in JIA (p = 0.009) and IBD (p ≤ 0.08). No significant relationship between diagnosis and underlying differences in IFX clearance was observed. Multivariable analysis by covariate population pharmacokinetic modeling confirmed increased IFX clearance to be associated with anti-IFX antibody positivity, increased ESR, and reduced serum albumin concentrations. Conclusions Enhanced IFX clearance is associated with immunogenicity and inflammatory burden across autoimmune disorders. Higher systemic IFX exposures observed in children with rheumatologic disorders are driven primarily by provider drug dose and interval selection, rather than differences in IFX pharmacokinetics across diagnoses. Despite maintenance IFX dosing at or above the standard recommended range for IBD (i.e., 5 mg/kg every 8 weeks), the dosing intensity used in the treatment of IBD is notably lower than dosing intensities used to treat JIA and uveitis, and may place some children with IBD at risk for suboptimal maintenance IFX exposures necessary for treatment response.

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“…For adalimumab, the approved induction regimen in PIBD ranges from 40 mg at week 0 and 20 mg at week 2 to 160 mg at week 0 and 80 mg at week 2 based on the weight of the patient, and disease severity assessed by a physician. Maintenance therapy with adalimumab is administered biweekly but may be enhanced to weekly therapy and/or by doubling the maintenance dose [8,9]. Infliximab and its biosimilars are licensed for use in children who are at least six years of age and have moderate to severe Crohn's disease or ulcerative colitis, and adalimumab only recently for such patients with ulcerative colitis in addition to Crohn's disease.…”

Section: Introductionmentioning

confidence: 99%

Therapy outcome related to adalimumab trough levels in pediatric patients with inflammatory bowel disease

Lehtomäki

Nikkonen

Merras‐Salmio

et al. 2021

Scandinavian Journal of Gastroenterology

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Objectives: We evaluated the relationship between serum concentration and efficacy of adalimumab (ADA), an anti-tumor necrosis factor-alpha agent, in pediatric patients with inflammatory bowel disease (PIBD). Materials and methods: This retrospective cross-sectional study traced 75 patients with PIBD (Crohn's disease, n ¼ 57) treated with ADA at two tertiary centers in Finland in 2012-2018. Drug levels and drug antibody titers were chart-reviewed, and the treatment continuation rate of ADA therapy was evaluated. We also assessed the impact of trough levels in the first 3 months on the continuation of ADA within one year of therapy. Results: ADA was introduced at a median age of 13.4 years, and the median disease duration was 2.7 years. During the first year, 22 patients (29%) discontinued ADA due to either loss of response (20%, n ¼ 15) or anti-drug antibody formation (5.3%, n ¼ 4). Regarding trough levels in the first 3 months, 9/ 16 patients (56%) with trough levels <5 mg/L and 12/20 (60%) with trough levels <7.5 mg/L at 3 months discontinued the therapy by the end of the first year. In comparison, only 8/32 patients (25%) with trough levels >7.5 mg/L at 3 months discontinued treatment during the first year (p ¼ .005). At the last follow-up (median 1.5 years), 52% of the 75 patients were on maintenance therapy and had a median trough level of 8.8 mg/L. Conclusion: Higher trough levels in the first 3 months of adalimumab treatment are associated with lower rates of discontinuation due to loss of response during the first year.

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Pharmacokinetics, Pharmacodynamics, and Immunogenicity of Infliximab in Pediatric Inflammatory Bowel Disease

Cited by 30 publications

References 86 publications

Pediatric Dose Selection for Therapeutic Proteins

Pediatric Dose Selection for Therapeutic Proteins

Factors associated with reduced infliximab exposure in the treatment of pediatric autoimmune disorders: a cross-sectional prospective convenience sampling study

Therapy outcome related to adalimumab trough levels in pediatric patients with inflammatory bowel disease

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