Risankizumab: Complete Drug Monograph

Pharmacokinetic Profile

Half-Life

~28 days (psoriasis); ~22–27 days (CD)

Metabolism

Catabolic (IgG degradation)

Bioavailability

~89% (SC, psoriasis); ~84% (PsA)

Volume of Distribution

Vss ~11.2 L (psoriasis)

Protein Binding

Not applicable (mAb)

Clinical Information

Drug Class

Selective IL-23 p19 Inhibitor (biologic)

Available Doses

90 mg, 150 mg, 180 mg, 360 mg (SC); 600 mg/10 mL (IV)

Route

SC (all indications); IV (IBD induction)

Renal Adjustment

Not studied; not expected to be needed

Hepatic Adjustment

Not studied; monitor LFTs for IBD

Pregnancy

Insufficient data; use if benefit outweighs risk

Lactation

No human data; consider benefit/risk

Schedule

Prescription only (biologic)

Generic / Biosimilar

Not yet available

Indications

Indication	Approved Population	Therapy Type	Status
Moderate-to-severe plaque psoriasis	Adults candidates for systemic therapy or phototherapy	Monotherapy	FDA Approved
Active psoriatic arthritis	Adults	Monotherapy or with non-biologic DMARDs	FDA Approved
Moderately-to-severely active Crohn’s disease	Adults	IV induction then SC maintenance	FDA Approved
Moderately-to-severely active ulcerative colitis	Adults	IV induction then SC maintenance	FDA Approved

Risankizumab is a selective IL-23 inhibitor that targets the p19 subunit, distinguishing it from ustekinumab which blocks the shared p40 subunit of both IL-12 and IL-23. This selectivity preserves IL-12-mediated Th1 responses involved in host defense while specifically suppressing Th17-driven inflammation. In dermatology, risankizumab has demonstrated very high rates of complete skin clearance (PASI 100) and is positioned as a first-line biologic for moderate-to-severe plaque psoriasis. In inflammatory bowel disease, it is approved for both Crohn’s disease and ulcerative colitis, using distinct IV induction dose levels for each condition.

Off-Label Uses

Hidradenitis suppurativa: Phase 2 data and case series suggest benefit; phase 3 trials ongoing. Evidence quality: Low.

Ankylosing spondylitis / axial spondyloarthritis: Evaluated in clinical trials; mixed results. IL-23 inhibitors as a class have shown limited efficacy in axial disease. Evidence quality: Low.

Dose

Dosing

Adult Dosing by Clinical Scenario

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Plaque psoriasis — moderate-to-severe	150 mg SC at Weeks 0 and 4	150 mg SC q12w	150 mg q12w	Single injection with prefilled pen or syringe; no weight-based adjustment Self-injection after training is appropriate
Psoriatic arthritis — active disease	150 mg SC at Weeks 0 and 4	150 mg SC q12w	150 mg q12w	May use alone or with non-biologic DMARDs (e.g., methotrexate) Same dosing as psoriasis
Crohn’s disease — induction	600 mg IV at Weeks 0, 4, and 8	—	600 mg per infusion	Infuse over at least 1 hour; single 600 mg vial per dose Check baseline LFTs and bilirubin before first dose
Crohn’s disease — maintenance	180 mg or 360 mg SC at Week 12	180 mg or 360 mg SC q8w	360 mg q8w	Use the lowest effective dose to maintain response; on-body injector or prefilled syringes available 360 mg: two 180 mg syringes or one 360 mg cartridge
Ulcerative colitis — induction	1,200 mg IV at Weeks 0, 4, and 8	—	1,200 mg per infusion	Infuse over at least 2 hours; requires two 600 mg vials Double the CD induction dose; longer infusion time required
Ulcerative colitis — maintenance	180 mg or 360 mg SC at Week 12	180 mg or 360 mg SC q8w	360 mg q8w	Same maintenance options as Crohn’s disease Use lowest effective dosage needed to maintain response

Clinical Pearl: Distinct Induction Doses for CD vs UC

A key prescribing difference between risankizumab’s IBD indications is the induction dose: 600 mg IV for Crohn’s disease versus 1,200 mg IV for ulcerative colitis, with correspondingly different infusion durations (at least 1 hour vs at least 2 hours). Both indications then transition to the same SC maintenance options (180 mg or 360 mg q8w). This dose-escalation for UC reflects the higher drug exposure needed to achieve clinical response in colitis, as demonstrated in the INSPIRE and COMMAND trials. Clinicians should also obtain baseline liver enzymes and bilirubin before initiating IV induction for either IBD indication due to reports of hepatotoxicity.

Pharmacology

Mechanism of Action

Risankizumab is a humanized IgG1 monoclonal antibody that selectively binds to the p19 subunit of interleukin-23 (IL-23), blocking its interaction with the IL-23 receptor complex. Unlike agents targeting the shared p40 subunit (e.g., ustekinumab), risankizumab does not interfere with IL-12 signaling, preserving Th1-mediated immune surveillance including interferon-gamma production. IL-23 is a key driver of Th17 cell differentiation and maintenance, and its blockade reduces downstream production of IL-17A, IL-17F, IL-22, and other pro-inflammatory mediators central to psoriatic disease and intestinal inflammation. This targeted selectivity is hypothesized to contribute to the favorable safety profile observed in clinical trials, particularly the low rates of candidal infections compared with direct IL-17 blockade.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	SC bioavailability ~89% (psoriasis phase III); Tmax 3–14 days	High bioavailability allows reliable SC dosing; no food effect considerations
Distribution	Vss ~11.2 L (90 kg psoriasis patient); ~8.5 L (65 kg CD patient)	Confined to vascular and interstitial space; body weight affects Vd but no dose adjustment required
Metabolism	Degraded via catabolic pathways into peptides and amino acids; not CYP-mediated	No hepatic CYP interactions expected; no dose adjustment for renal or hepatic impairment anticipated
Elimination	Terminal t½ ~28 days (psoriasis); ~22–27 days (CD); CL ~0.31 L/day; steady state by Week 16	Long half-life supports q12w (psoriasis/PsA) and q8w (IBD) maintenance intervals

Side Effects

≥10%Very Common

Adverse Effect	Incidence	Clinical Note
Upper respiratory infections	13.0% vs 9.7% placebo (PsO Wk 16)	Broad category including nasopharyngitis, sinusitis, pharyngitis, and viral URI; similar rates in CD induction (10.6%)

1–10%Common

Adverse Effect	Incidence	Clinical Note
Headache	3.5% vs 2.0% (PsO); 6.6% vs 5.6% (CD induction)	Usually mild; includes tension and sinus headache subtypes
Arthralgia	5.0% vs 4.4% (CD induction); 9.2% vs 8.4% (CD maint 360 mg); 3% vs 1% (UC induction)	Most consistently reported adverse effect across all IBD trials; distinguish from underlying joint disease
Fatigue	2.5% vs 1.0% (PsO)	Includes asthenia; dose-independent
Injection site reactions	1.5% vs 1.0% (PsO); 5.6% vs 2.8% (CD maint 360 mg)	Includes erythema, pain, swelling, bruising; rotate injection sites
Tinea infections	1.1% vs 0.3% (PsO)	Includes tinea pedis, cruris, and versicolor; treat with topical antifungals; does not require drug discontinuation
Abdominal pain	8.5% vs 4.2% (CD maint 360 mg)	Higher with 360 mg dose; distinguish from underlying Crohn’s symptoms
Pyrexia	4.9% vs 2.8% (CD maint 360 mg); 4.0–4.7% vs 3.5% (UC maint)	Low-grade; evaluate for infection if persistent
Anemia	4.5–4.9% vs 4.2% (CD maintenance)	May reflect ongoing disease activity rather than direct drug effect
Back pain	4.2% vs 2.1% (CD maint 360 mg)	More prominent at higher maintenance dose
Rash	4.1% vs 1.7% (UC maint 180 mg)	Includes macular rash; also reported as postmarketing event

SeriousSerious Adverse Effects

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Serious infections (cellulitis, osteomyelitis, sepsis, herpes zoster)	≤0.4% (PsO controlled period); 2.6–5.6% (CD maint)	Any time during treatment	Hold risankizumab; initiate appropriate antimicrobial therapy; reassess before resuming
Anaphylaxis / serious hypersensitivity	Rare (1 case in phase 2 PsA trial)	Within hours of administration	Discontinue permanently; emergency treatment
Drug-induced liver injury (IBD induction)	Very rare (1 serious case reported in CD trials: ALT 54x ULN)	During IV induction phase (after 2 doses reported)	Monitor LFTs at baseline and during induction up to 12 weeks; interrupt if DILI suspected; corticosteroids may be needed
Lipid elevations (CD/UC)	Common (mean increase): total cholesterol +9.4 mg/dL, LDL-C +6.6 mg/dL by Wk 12	First 4 weeks of induction; remains stable	Monitor fasting lipids; manage per cardiovascular risk guidelines; generally modest elevations

DiscontinuationDiscontinuation Rates

Psoriasis (Through Week 52)

Very low no new adverse reactions identified

Context: Adverse reaction rates through 52 weeks were similar to the first 16 weeks. Serious infections leading to discontinuation included pneumonia. Long-term retention rates are high in registry data.

IBD (Maintenance Through Week 52)

Low safety profile consistent across indications

Top reasons: Loss of response, serious infection, hepatotoxicity (rare). One serious DILI case led to discontinuation during CD induction.

Hepatotoxicity Monitoring in IBD

A unique safety signal for risankizumab in IBD is drug-induced liver injury during IV induction. One patient with Crohn’s disease developed severe hepatotoxicity (ALT 54x ULN) after two induction doses, requiring hospitalization and corticosteroid treatment. The PI mandates baseline liver enzyme and bilirubin measurement before IV induction and monitoring at least through the first 12 weeks. Clinicians should consider alternative therapies in patients with pre-existing liver cirrhosis and promptly investigate any unexplained transaminase elevation.

Int

Drug Interactions

Risankizumab is not metabolized by cytochrome P450 enzymes and is not expected to directly alter CYP activity. As an IgG1 monoclonal antibody, it undergoes catabolic degradation independently of hepatic metabolic pathways. No formal in vivo drug interaction studies have been conducted. Population pharmacokinetic analyses confirm that concomitant methotrexate, NSAIDs, and corticosteroids do not affect risankizumab clearance. However, as with other immunomodulatory biologics, resolution of chronic inflammation may theoretically normalize suppressed CYP450 enzyme activity, potentially affecting narrow-therapeutic-index substrates.

MajorLive Vaccines

MechanismImmunosuppression may allow replication of live vaccine organisms

EffectRisk of vaccine-strain infection; no data on response to live or inactive vaccines

ManagementAvoid live vaccines during treatment; complete all age-appropriate immunizations before initiating risankizumab

FDA PI

ModerateOther Biologic Immunosuppressants

MechanismAdditive immunosuppression with combination biologic therapy

EffectIncreased risk of serious infections

ManagementNot recommended; allow adequate washout between biologic agents when switching

FDA PI

ModerateCYP450 Narrow-TI Substrates (warfarin, cyclosporine, theophylline)

MechanismInflammation resolution may restore CYP enzyme activity suppressed by chronic cytokine elevation

EffectPotential decrease in drug levels of CYP substrates

ManagementMonitor drug levels or therapeutic effect (e.g., INR for warfarin) at initiation and discontinuation of risankizumab

Pharmacologic Class Effect

MinorMethotrexate / Non-Biologic DMARDs

MechanismNo pharmacokinetic interaction; MTX does not alter risankizumab clearance

EffectNo change in risankizumab exposure

ManagementCombination use in PsA is approved and well-studied; standard monitoring for both agents

FDA PI / PopPK Data

Mon

Monitoring

TB ScreeningBaseline
RoutineTST or IGRA before first dose. Consider anti-TB therapy if latent TB is confirmed and adequate prior treatment cannot be documented. In psoriasis trials, no patients with latent TB on prophylaxis developed active TB.
Liver Enzymes (IBD)Baseline, then during induction up to 12 weeks
RoutineALT, AST, and total bilirubin before initiating IV induction for CD or UC. Monitor during induction; continue per routine patient management thereafter. Interrupt if drug-induced liver injury is suspected.
Infection SignsEvery visit
RoutineAssess for fever, cough, skin changes, urinary symptoms. Hold therapy for clinically significant infections.
Lipid Panel (IBD)Baseline, then at 12 weeks
RoutineTotal cholesterol and LDL-C increase modestly during induction (mean +9.4 mg/dL and +6.6 mg/dL respectively). Monitor and manage per cardiovascular risk profile.
Hepatic Events (PsA)Periodic
Trigger-basedALT/AST elevations were more common in PsA trials (5.4% vs 3.9% placebo). No serious hepatic events reported, but monitor if symptoms arise.
ImmunogenicityIf loss of response
Trigger-basedAnti-drug antibodies develop in ~24% (PsO), ~12% (PsA), ~3.4% (CD), and ~4–9% (UC). High-titer ADA (≥128) in ~1% of PsO patients associated with reduced drug levels and efficacy. Consider drug level measurement before switching.

Contraindications & Cautions

Absolute Contraindications

History of serious hypersensitivity reaction to risankizumab-rzaa or any excipient (glacial acetic acid, polysorbate 20, sodium acetate, trehalose, succinic acid, sodium succinate, sorbitol)

Relative Contraindications (Specialist Input Recommended)

Clinically important active infection — delay initiation until infection resolves or is adequately treated
Active tuberculosis — do not administer; treat TB first
Pre-existing liver cirrhosis (for IBD indications) — consider alternative treatment options given hepatotoxicity signal
Chronic or recurrent infection history — careful risk-benefit assessment required

Use with Caution

Pregnancy — insufficient human data; animal studies showed dose-dependent fetal/infant loss at 50 mg/kg (5x human exposure at maximum induction dose). Discuss contraception timing with prescriber given the drug’s long half-life (~28 days).
Lactation — no human milk data; weigh breastfeeding benefits against potential infant exposure
Patients scheduled for vaccination — complete all age-appropriate vaccines before treatment; avoid live vaccines during therapy

FDA Safety Warning Hepatotoxicity in Inflammatory Bowel Disease

Drug-induced liver injury requiring hospitalization has been reported during IV induction with risankizumab in Crohn’s disease (ALT 54x ULN, AST 30x ULN, bilirubin 2.2x ULN after two 600 mg IV doses). The PI mandates liver enzyme and bilirubin monitoring at baseline and during induction for at least 12 weeks. This warning is specific to the IBD IV induction regimen and is not replicated in the psoriasis or PsA prescribing guidance.

Patient Counselling

Purpose of Therapy

Risankizumab works by selectively blocking IL-23, a single immune messenger that drives the inflammation underlying psoriasis, psoriatic arthritis, Crohn’s disease, and ulcerative colitis. Because it targets only one pathway rather than broadly suppressing the immune system, it has a favorable safety profile. For psoriasis, treatment results in sustained skin clearance for many patients, with injections needed only every 12 weeks after the initial loading period. For bowel disease, the first three doses are given as an IV infusion in a clinic, followed by self-administered injections at home every 8 weeks.

How to Take

For psoriasis and psoriatic arthritis, the drug is self-injected using a prefilled pen or syringe at Weeks 0 and 4, then every 12 weeks. For Crohn’s disease and ulcerative colitis, the initial doses are infused intravenously in a healthcare setting, followed by subcutaneous injections (using a prefilled syringe or on-body injector) every 8 weeks starting at Week 12. Allow the pen or syringe to reach room temperature (15–90 minutes depending on formulation) before injection. Inject into the thigh or abdomen, rotating sites each time. Do not inject into skin that is tender, bruised, or affected by psoriasis.

Infection Risk

Tell patientThis medication slightly reduces your ability to fight certain infections. Most patients tolerate it well, and infection rates in trials were only slightly higher than placebo. Wash hands regularly and avoid close contact with people who are actively sick.

Call prescriberIf you develop a fever above 38.5 °C, a persistent cough, painful or spreading redness of the skin, or urinary burning that does not resolve.

Injection Technique & Storage

Tell patientStore the pen or syringe in the refrigerator (2–8 °C). Before injecting, let it warm to room temperature out of direct sunlight. Do not freeze or shake. The solution should look clear to slightly yellow; do not use if cloudy or discolored. After use, dispose of the syringe in a sharps container.

Call prescriberIf you notice significant swelling, drainage, or spreading redness at the injection site, or if you experience difficulty breathing, throat tightness, or widespread rash after injection.

Liver Monitoring (IBD Only)

Tell patientDuring the initial IV infusion phase for bowel disease, blood tests are needed to check your liver function. This is a precaution based on a rare but serious side effect seen in clinical trials. Most patients have no liver problems.

Call prescriberImmediately if you develop yellowing of skin or eyes, dark urine, severe nausea, right-sided abdominal pain, or unexplained fatigue during the infusion phase.

Vaccinations

Tell patientLive vaccines should be avoided during treatment. Inactivated vaccines (flu shot, COVID-19, pneumococcal) are safe and recommended. Complete all routine vaccinations before starting risankizumab.

Call prescriberIf you are unsure whether a vaccine is live or inactivated before receiving it.

Pregnancy & Family Planning

Tell patientRisankizumab has not been adequately studied in pregnant women. Animal studies showed increased pregnancy loss at very high doses. If you are planning a pregnancy, discuss the timing with your prescriber. A pregnancy registry exists to track outcomes in women exposed during pregnancy (1-877-302-2161).

Call prescriberIf you become pregnant or plan to become pregnant during treatment.

Ref

Sources

Regulatory (PI / SmPC)

Skyrizi (risankizumab-rzaa) prescribing information. AbbVie Inc. Revised 3/2026. Full Prescribing InformationPrimary source for all dosing, indications, adverse reactions, warnings, PK data, and hepatotoxicity guidance in this monograph.
Skyrizi (risankizumab) European Medicines Agency Summary of Product Characteristics. EMA SmPCEuropean regulatory perspective with supplementary safety and efficacy data.

Key Clinical Trials

Gordon KB, Strober B, Lebwohl M, et al. Efficacy and safety of risankizumab in moderate-to-severe plaque psoriasis (UltIMMa-1 and UltIMMa-2): results from two double-blind, randomised, placebo-controlled and ustekinumab-controlled phase 3 trials. Lancet. 2018;392(10148):650–661. DOIPivotal phase 3 trials demonstrating risankizumab superiority over ustekinumab and placebo in plaque psoriasis.
Kristensen LE, Keiserman M, Engel K, et al. Efficacy and safety of risankizumab for active psoriatic arthritis: 24-week results from the randomised, double-blind, phase 3 KEEPsAKE 1 and KEEPsAKE 2 trials. Ann Rheum Dis. 2022;81(3):367–375. DOIPhase 3 trials establishing risankizumab efficacy in PsA, including biologic-experienced patients.
D’Haens G, Panaccione R, Baert F, et al. Risankizumab as induction therapy for Crohn’s disease: results from the phase 3 ADVANCE and MOTIVATE induction trials. Lancet. 2022;399(10340):2015–2030. DOICo-primary induction trials (ADVANCE, MOTIVATE) establishing IV induction efficacy in Crohn’s disease.
Ferrante M, Panaccione R, Baert F, et al. Risankizumab as maintenance therapy for moderately to severely active Crohn’s disease: results from the multicentre, randomised, double-blind, placebo-controlled, withdrawal phase 3 FORTIFY maintenance trial. Lancet. 2022;399(10340):2031–2046. DOIFORTIFY maintenance trial establishing SC maintenance dosing (180 mg and 360 mg q8w) for Crohn’s disease.
Louis E, Schreiber S, Panaccione R, et al; INSPIRE and COMMAND Study Group. Risankizumab for ulcerative colitis: two randomized clinical trials. JAMA. 2024;332(11):881–897. DOIPivotal phase 3 induction (INSPIRE) and maintenance (COMMAND) trials for the UC indication using 1,200 mg IV induction dose.

Guidelines

Feuerstein JD, Ho EY, Shmidt E, et al. AGA clinical practice guidelines on the medical management of moderate to severe luminal and perianal fistulizing Crohn’s disease. Gastroenterology. 2021;160(7):2496–2508. DOIAGA guideline positioning IL-23 inhibitors in the Crohn’s disease treatment algorithm.
Singh S, Loftus EV Jr, Limketkai BN, et al. AGA living clinical practice guideline on pharmacological management of moderate-to-severe ulcerative colitis. Gastroenterology. 2024;167(7):1307–1343. DOIUpdated AGA guideline recommending risankizumab as a higher-efficacy option for UC.

Mechanistic / Basic Science

Gaffen SL, Jain R, Garg AV, Cua DJ. The IL-23–IL-17 immune axis: from mechanisms to therapeutic testing. Nat Rev Immunol. 2014;14(9):585–600. DOIComprehensive review of IL-23/IL-17 biology underpinning the rationale for selective p19 blockade.

Pharmacokinetics / Special Populations

Suleiman AA, Minocha M, Khatri A, Pang Y, Othman AA. Population pharmacokinetics of risankizumab in healthy volunteers and subjects with moderate to severe plaque psoriasis: integrated analyses of phase I–III clinical trials. Clin Pharmacokinet. 2019;58(10):1309–1321. DOIIntegrated PopPK analysis establishing Vss (11.2 L), CL (0.31 L/day), t½ (28 days), and SC bioavailability (89%) for risankizumab in psoriasis.
Suleiman AA, Khatri A, Minocha M, Othman AA. Population pharmacokinetics of the interleukin-23 inhibitor risankizumab in subjects with psoriasis and Crohn’s disease: analyses of phase I and II trials. Clin Pharmacokinet. 2019;58(3):375–387. DOIPopPK model comparing risankizumab disposition in psoriasis (Vss 11.7 L, t½ 27 days) versus Crohn’s disease (Vss 8.45 L, t½ 22 days).
Pang Y, Khatri A, Suleiman AA, Othman AA. Clinical pharmacokinetics and pharmacodynamics of risankizumab in psoriasis patients. Clin Pharmacokinet. 2020;59(3):311–326. DOIComprehensive PK/PD review confirming dose-exposure-response relationships supporting the 150 mg SC q12w regimen.

Skyrizi (Risankizumab)