Population Pharmacokinetics of the Interleukin-23 Inhibitor Risankizumab in Subjects with Psoriasis and Crohn’s Disease: Analyses of Phase I and II Trials

Suleiman, Ahmed A.; Khatri, Amit; Minocha, Mukul; Othman, Ahmed A.

doi:10.1007/s40262-018-0704-z

Cited by 27 publications

(27 citation statements)

References 29 publications

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“…ADA titers in the patients who were ADA positive ranged from one to 16; these low-titer ADAs did not affect risankizumab exposure based on the comparable risankizumab trough concentrations in ADA-positive and ADA-negative subjects in the study (data not shown). These results are consistent with the population pharmacokinetic analysis of risankizumab conducted using data from phase I and II studies in patients with psoriasis and Crohn's disease [13].…”

Section: Pharmacokineticssupporting

confidence: 85%

“…Blood samples for determination of risankizumab plasma concentrations and detection of risankizumab anti-drug antibody (ADA) were collected just prior to risankizumab dosing on days 8, 36, 64, 92, 105, and 204; an additional blood sample for risankizumab plasma concentrations was collected on day 98. Risankizumab plasma concentrations and ADA were measured as previously described [5,13]. Briefly, risankizumab plasma concentrations were determined using a validated, enzyme-linked immunosorbent assay method in which a polyclonal anti-risankizumab antibody was used as the capture reagent and a biotinylated anti-idiotypic risankizumab antibody was used as the detection reagent.…”

Section: Pharmacokinetic Sampling and Bioanalytical Methodsmentioning

confidence: 99%

“…Phase III studies in Crohn's disease [10,11] and ulcerative colitis [12] are currently ongoing. Risankizumab exhibits linear pharmacokinetics and has an estimated elimination half-life (t ½ ) of approximately 4 weeks in patients with psoriasis [13].…”

Section: Introductionmentioning

confidence: 99%

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Lack of Effect of 12-Week Treatment with Risankizumab on the Pharmacokinetics of Cytochrome P450 Probe Substrates in Patients with Moderate to Severe Chronic Plaque Psoriasis

et al. 2018

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Objective The objective of this study was to characterize the effects of risankizumab on the in vivo activity of cytochrome P450 (CYP) 1A2, CYP2C9, CYP2C19, CYP2D6, and CYP3A in psoriasis patients using a cocktail approach. Methods Patients with moderate to severe chronic plaque psoriasis (n = 21) received single oral doses of sensitive probe substrates for CYP1A2 (caffeine 100 mg), CYP2C9 (warfarin 10 mg), CYP2C19 (omeprazole 20 mg), CYP2D6 (metoprolol 50 mg), and CYP3A (midazolam 2 mg) on day 1, followed by 12 weeks of subcutaneous risankizumab treatment of 150 mg once every 4 weeks from day 8 to day 92, and again the same cocktail of substrates on day 98. Serial blood samples were collected for determination of the CYP probe drugs and metabolites with and without risankizumab. Trough samples were collected for risankizumab. Results The 90% confidence intervals (CIs) for the area under the plasma concentration-time curve (AUC) from time zero to infinity (AUC ∞ ) ratios for the CYP probe substrates administered with risankizumab versus without risankizumab were within the default 0.8-1.25 equivalence bounds. Similar results were observed for maximum plasma concentration (C max ), except for omeprazole, for which the lower bound of the 90% CI for C max (0.73) extended slightly below the default equivalence limit. No differences were observed in metabolite-to-parent drug C max or AUC ratios with risankizumab versus without risankizumab. Risankizumab trough plasma concentrations significantly exceeded those of the phase III regimen of risankizumab in psoriasis (150 mg subcutaneously at weeks 0 and 4 and every 12 weeks thereafter). Conclusions Risankizumab did not affect the in vivo activity of CYP1A2, CYP2C9, CYP2C19, CYP2D6, or CYP3A enzymes in patients with moderate or severe plaque psoriasis and therefore has no potential for drug interactions through these enzymes. Clinical trial registration ClinicalTrials.gov Identifier: NCT02772601. Key Points12 weeks of treatment with risankizumab 150 mg administered subcutaneously every 4 weeks had no relevant effects on cytochrome P450 (CYP) 1A2, CYP2C9, CYP2C19, CYP2D6, or CYP3A in vivo.No dose adjustment is needed for concomitant medications that are substrates of these CYP enzymes during coadministration with risankizumab.

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Section: Pharmacokineticssupporting

confidence: 85%

Section: Pharmacokinetic Sampling and Bioanalytical Methodsmentioning

confidence: 99%

See 1 more Smart Citation

Lack of Effect of 12-Week Treatment with Risankizumab on the Pharmacokinetics of Cytochrome P450 Probe Substrates in Patients with Moderate to Severe Chronic Plaque Psoriasis

et al. 2018

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“…An approximately dose proportional increase in risankizumab exposure was observed following repeated administration of 90 and 180 mg subcutaneous doses in the global phase II study [17,23], and between 75 and 150 mg subcutaneous doses in the Japanese phase II/III studies [13].…”

Section: Multiple-dose Pharmacokineticsmentioning

confidence: 92%

Clinical Pharmacokinetics and Pharmacodynamics of Risankizumab in Psoriasis Patients

et al. 2019

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Risankizumab is a humanized immunoglobulin (Ig) G1 monoclonal antibody developed and approved for the treatment of moderate-to-severe plaque psoriasis at a dose of 150 mg administered subcutaneously at weeks 0 and 4, and every 12 weeks thereafter. Ongoing trials are investigating the use of risankizumab in other inflammatory autoimmune diseases. Risankizumab exhibits linear pharmacokinetics when administered intravenously (0.01 mg/kg-1200 mg) or subcutaneously (0.25 mg/ kg-300 mg), with a long terminal half-life of approximately 28 days. Following subcutaneous administration, peak plasma concentration was reached approximately 3-14 days after dosing, with an estimated bioavailability of 89%. Population pharmacokinetic analyses identified bodyweight, high titers of antidrug antibodies occurring in < 2% of evaluated subjects, baseline serum albumin, baseline high-sensitivity C-reactive protein, and baseline serum creatinine to be statistically correlated with risankizumab clearance, but none of them had a clinically meaningful impact on risankizumab efficacy in psoriasis patients following the clinical dosing regimen. Exposure-response analyses in psoriasis patients demonstrated that the maximum efficacy was achieved with the clinically approved regimen and there was no apparent correlation between risankizumab exposure and safety. A dedicated drug interaction cocktail study in patients with psoriasis demonstrated a lack of therapeutic protein-drug interaction potentials for risankizumab and various cytochrome P450 substrates. In this article, we review the clinical pharmacology data available to date for risankizumab, which supported the clinical development program and ultimately regulatory approvals for risankizumab in the treatment of patients with moderate-to-severe plaque psoriasis.

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“…In psoriasis patients with inactive IBD, we recommend that the TNF antagonists: adalimumab, certolizumab pegol and infliximab; the IL12/23 inhibitor: ustekinumab; the IL23/p19 inhibitors: guselkumab, risankizumab and tildrakizumab; as well as the synthetic drug apremilast, and the conventional drugs, methotrexate, cyclosporine, fumarates and acitretin, can all be used as systemic treatments as they also have a beneficial or neutral effect on IBD symptoms. [15][16][17] We advise caution with use of the following anti-IL17 biological drugs: secukinumab, ixekizumab and brodalumab, to treat psoriasis patients with inactive IBD, and in those patients with a family history of IBD. 6 We also advise not using etanercept in these patients due to the possibility of a flare-up of IBD symptoms.…”

Section: Clinical Recommendationsmentioning

confidence: 99%

Practical recommendations for systemic treatment in psoriasis in case of coexisting inflammatory, neurologic, infectious or malignant disorders (BETA‐PSO: Belgian Evidence‐based Treatment Advice in Psoriasis; part 2)

Lambert

Segaert²,

Ghislain

et al. 2020

Acad Dermatol Venereol

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Background Psoriasis patients carry an increased risk for associated comorbidities. Dermatologists have to be aware of the effects of systemic treatments not only on psoriasis but also on co‐occurring diseases. In case of other coexisting inflammatory diseases, the right psoriasis treatment may improve both disorders. For infectious and malignant disorders, some treatments have to be avoided as they may be harmful. Objective The primary objective of this project was to collect evidence for the creation of practice guidelines for systemic treatment of psoriasis (BETA‐PSO: Belgian Evidence‐based Treatment Advice in Psoriasis). Methods Evidence‐based recommendations were formulated using a quasi‐Delphi methodology after a systematic search of the literature and a consensus procedure involving eight psoriasis experts. Results Recommendations are given on the use of systemic treatment in psoriatic arthritis, inflammatory bowel disease, demyelinating disorders, hepatitis B and C, HIV and cancer. Conclusion This expert opinion is a practical guide for dermatologists when handling psoriasis patients with these specific conditions.

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Population Pharmacokinetics of the Interleukin-23 Inhibitor Risankizumab in Subjects with Psoriasis and Crohn’s Disease: Analyses of Phase I and II Trials

Cited by 27 publications

References 29 publications

Lack of Effect of 12-Week Treatment with Risankizumab on the Pharmacokinetics of Cytochrome P450 Probe Substrates in Patients with Moderate to Severe Chronic Plaque Psoriasis

Lack of Effect of 12-Week Treatment with Risankizumab on the Pharmacokinetics of Cytochrome P450 Probe Substrates in Patients with Moderate to Severe Chronic Plaque Psoriasis

Clinical Pharmacokinetics and Pharmacodynamics of Risankizumab in Psoriasis Patients

Practical recommendations for systemic treatment in psoriasis in case of coexisting inflammatory, neurologic, infectious or malignant disorders (BETA‐PSO: Belgian Evidence‐based Treatment Advice in Psoriasis; part 2)

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