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Drug Monograph

Jakafi (Ruxolitinib)

ruxolitinib
JAK1/JAK2 Kinase Inhibitor·Oral (Tablets)
Pharmacokinetic Profile
Half-Life
~3 h (parent); ~5.8 h (ruxolitinib + active metabolites)
Metabolism
CYP3A4 (primary), CYP2C9 (secondary)
Protein Binding
~97% (albumin)
Bioavailability
>95%; food does not significantly affect AUC
Volume of Distribution
53–65 L (steady state in MF patients)
Clinical Information
Drug Class
Janus Kinase (JAK1/JAK2) Inhibitor
Available Doses
5 mg, 10 mg, 15 mg, 20 mg, 25 mg tablets
Route
Oral
Renal Adjustment
Required — varies by indication and degree of impairment
Hepatic Adjustment
Required — dose reduction or avoidance depending on severity and platelets
Pregnancy
Use only if potential benefit justifies risk to fetus
Lactation
Discontinue breastfeeding during treatment and for 2 weeks after last dose
Schedule / Legal Status
Rx Only (not a controlled substance)
Generic Available
No
Rx

Indications

IndicationApproved PopulationTherapy TypeStatus
Intermediate- or high-risk myelofibrosis (MF)Adults with primary MF, post-PV MF, or post-ET MFMonotherapy; dose based on platelet countFDA Approved
Polycythemia vera (PV)Adults with inadequate response to or intolerance of hydroxyureaMonotherapyFDA Approved
Steroid-refractory acute GVHD (aGVHD)Adults and pediatric patients ≥12 yearsMonotherapyFDA Approved
Chronic GVHD (cGVHD)Adults and pediatric patients ≥12 years after failure of 1–2 lines of systemic therapyMonotherapyFDA Approved

Ruxolitinib was the first JAK inhibitor approved by the FDA (2011) and remains the reference standard for JAK inhibition in myeloproliferative neoplasms. Its indications span two distinct therapeutic areas: myeloproliferative neoplasms (MF, PV) where it targets dysregulated JAK2 signalling, and graft-versus-host disease (aGVHD, cGVHD) where it modulates immune cell activation through JAK1/JAK2 pathway inhibition. There are no formal contraindications listed in the prescribing information.

Dose

Dosing

Starting Doses by Clinical Scenario

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
MF — platelets >200 × 109/L20 mg BIDTitrate by 5 mg BID increments25 mg BIDNo dose increase in first 4 weeks or more frequently than q2 weeks. Discontinue if no response after 6 months.
COMFORT-I/II trial setting
MF — platelets 100–200 × 109/L15 mg BIDTitrate by 5 mg BID increments25 mg BIDSame titration rules. Hold for platelets <50 × 109/L or ANC <0.5 × 109/L.
MF — platelets 50–<100 × 109/L5 mg BIDTitrate by 5 mg daily increments10 mg BIDHold for platelets <25 × 109/L or ANC <0.5 × 109/L. More conservative dose modifications apply.
Polycythemia vera10 mg BIDTitrate based on efficacy & safety25 mg BIDReduce or hold for Hb <8 g/dL, platelets <50 × 109/L, or ANC <1.0 × 109/L.
RESPONSE trial setting
Steroid-refractory acute GVHD5 mg BID5 mg BID10 mg BIDConsider tapering after 6 months if responding and off therapeutic corticosteroids. Taper q8 weeks (10 → 5 mg BID → 5 mg daily).
REACH2 trial setting
Chronic GVHD after 1–2 prior therapies10 mg BID10 mg BID10 mg BIDConsider tapering after 6 months if responding and off therapeutic corticosteroids. Same taper schedule as aGVHD.
REACH3 trial setting

Dose Modifications for Drug Interactions

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
MF/PV + strong CYP3A4 inhibitor or fluconazole ≤200 mg (platelets ≥100)10 mg BIDPer safety/efficacy10 mg BIDReduce dose by 50% (rounded up). If stabilised on 5 mg BID, reduce to 5 mg daily. If on 5 mg daily, avoid inhibitor or hold ruxolitinib (FDA PI).
MF/PV + strong CYP3A4 inhibitor or fluconazole ≤200 mg (platelets 50–<100)5 mg dailyPer safety/efficacy5 mg dailyAvoid combination if possible (FDA PI).
aGVHD + ketoconazole5 mg daily5 mg daily5 mg dailyNo dose adjustment for other CYP3A4 inhibitors in aGVHD except ketoconazole (FDA PI).
Any indication + fluconazole >200 mg/dayAvoid combinationFluconazole doses >200 mg cause excessive dual CYP3A4/CYP2C9 inhibition (FDA PI).
Any indication + strong CYP3A4 inducer (e.g., rifampicin)No dose adjustment; monitor closelyAUC decreases ~61%; titrate based on safety and efficacy (FDA PI).
Clinical Pearl: Platelet-Driven Dosing Is Unique to Ruxolitinib

Unlike most oral oncology agents, ruxolitinib starting dose for myelofibrosis is determined entirely by the patient’s baseline platelet count, not by body weight or body surface area. This reflects the drug’s primary dose-limiting toxicity: thrombocytopenia. The dose titration system is intricate, with different interruption, restart, and reduction rules depending on whether the patient started with platelets above or below 100 × 109/L. Familiarity with the full FDA PI dosing tables is essential for safe prescribing. Ruxolitinib should not be abruptly discontinued in MF patients as this can trigger acute symptom flare and rare septic shock-like events; gradual tapering is recommended.

PK

Pharmacology

Mechanism of Action

Ruxolitinib is a potent and selective inhibitor of Janus Associated Kinases JAK1 and JAK2, which mediate signalling for a range of cytokines and growth factors that are central to haematopoiesis and immune function. In myeloproliferative neoplasms, constitutive activation of JAK-STAT signalling (often driven by the JAK2 V617F mutation) leads to uncontrolled myeloid proliferation, splenomegaly, and systemic inflammatory symptoms. Ruxolitinib interrupts this aberrant signalling, reducing spleen size and alleviating constitutional symptoms such as fatigue, night sweats, pruritus, and bone pain. In GVHD, JAK-STAT pathways regulate the development, proliferation, and activation of alloreactive T cells and other immune cells driving tissue damage. By inhibiting JAK1/JAK2, ruxolitinib reduces inflammatory cytokine levels and immune cell infiltration into target organs.

ADME Profile

ParameterValueClinical Implication
AbsorptionRapid; Tmax ~1–2 h; bioavailability >95%; food decreases Cmax ~24% but does not significantly affect AUC; dose-proportional PK over 5–200 mg; steady state by Day 2Can be taken with or without food; rapid onset supports twice-daily dosing; very fast steady state achieved
DistributionVd 53–65 L at steady state (MF patients); protein binding ~97% (albumin); not a P-gp substrateModerate distribution; high protein binding; no P-gp-mediated interactions expected
MetabolismPrimarily CYP3A4 (~43–75%); secondarily CYP2C9 (~19–56%); forms pharmacologically active metabolites contributing 20–50% of total activityDual CYP pathway creates vulnerability to both CYP3A4 inhibitors and dual CYP3A4/CYP2C9 inhibitors (fluconazole); active metabolites extend effective half-life to ~5.8 h
Eliminationt½ ~3 h (parent), ~5.8 h (parent + metabolites); 74% urine, 22% feces (<1% as unchanged drug); almost completely eliminated by oxidative metabolismShort parent half-life supports rapid PD offset; renal impairment increases metabolite exposure, requiring dose reduction; eliminated almost entirely as metabolites
SE

Side Effects

Adverse reaction data are from the FDA prescribing information (June 2025 revision). Side effect profiles differ substantially between indications: haematological toxicities predominate in MF/PV, while infections are more prominent in GVHD. Incidence rates shown are from pivotal trials in the most relevant indication.

≥10%Very Common
Adverse EffectIncidenceClinical Note
Thrombocytopenia70–84% (MF)Primary dose-limiting toxicity in MF; Grade 3–4 in ~11% at week 24, increasing to ~23% with long-term treatment (5-year COMFORT-I); manage with dose reduction/interruption per platelet thresholds; transfusion may be needed (FDA PI)
Anaemia~99% (MF, lab abnormality)Nearly universal hemoglobin decline due to JAK2 inhibition of erythropoietin signalling; Grade 3–4 in ~45% (COMFORT-I); nadir at weeks 8–12 with partial recovery by week 24; transfusion frequently required early in treatment; women at higher risk (FDA PI)
Neutropenia19% (MF); >50% (aGVHD)Grade 3–4 in ~7% (MF); higher in GVHD setting; hold for ANC <0.5 (MF) or <0.75 (GVHD) × 109/L (FDA PI)
Infections>50% (GVHD)Bacterial, viral, fungal, and mycobacterial infections reported; herpes zoster, hepatitis B reactivation, TB, and PML are specific risks; screen for TB and hepatitis B before starting (FDA PI)
Bruising23% (MF)Related to thrombocytopenia; monitor for more significant bleeding
Dizziness18% (MF)Caution with driving and hazardous activities
Headache15% (MF)Usually mild; self-limiting
Diarrhoea15% (PV)Generally Grade 1–2; manage supportively
Oedema>50% (aGVHD)Common in GVHD setting; assess for fluid overload
1–10%Common
Adverse EffectIncidenceClinical Note
Weight gain7% (MF)May be partially related to improved appetite and symptom relief
Herpes zoster2–6%Prompt antiviral treatment required; consider prophylaxis in high-risk patients (FDA PI)
Hypercholesterolaemia / hypertriglyceridaemiaLipid elevations reportedCheck lipids 8–12 weeks after starting; treat per guidelines (FDA PI Section 5.5)
Urinary tract infection~9% (MF)Routine urinalysis if symptomatic; higher risk with immunosuppression
Non-melanoma skin cancer (NMSC)~6% (long-term MF)Periodic skin examinations recommended; most patients had prior HU use or risk factors (FDA PI Section 5.4)
Flatulence5% (PV)Generally mild and self-limiting
SeriousSerious Adverse Effects (Regardless of Frequency)
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Serious infections (TB, hepatitis B reactivation, PML, invasive fungal)Variable; includes fatal casesAny timeScreen for TB, HBV, HCV before starting. Resolve active serious infections before initiating. Treat promptly. Consider holding ruxolitinib for serious infections (FDA PI Section 5.2)
Symptom exacerbation / withdrawal syndrome (MF)Occurs with abrupt discontinuationWithin 1 week of discontinuationGradual taper recommended rather than abrupt cessation. Manage with supportive care; consider resuming ruxolitinib if severe. Rare septic shock-like syndrome reported (FDA PI Section 5.3)
Major adverse cardiovascular events (MACE)JAK inhibitor class warningAny timeMonitor for cardiovascular events. Consider risk factors before initiating, particularly in patients ≥50 years with cardiovascular risk factors (FDA PI Section 5.6)
Thrombosis (arterial and venous)JAK inhibitor class warningAny timeEvaluate and treat thrombotic symptoms promptly. Consider underlying thrombotic risk in MPN patients (FDA PI Section 5.7)
Secondary malignancies (including lymphoma)JAK inhibitor class warningAny time, particularly long-term useMonitor; particular risk in current/past smokers. Screen according to age-appropriate guidelines (FDA PI Section 5.8)
Severe thrombocytopenia / bleedingGrade 3–4: ~11% (MF)Weeks to monthsInterrupt for platelet count thresholds per indication; manage with dose reduction and platelet transfusions. Interrupt for any bleeding requiring intervention (FDA PI)
DiscontinuationDiscontinuation Rates
COMFORT-I (MF)
11%
Top reasons: Thrombocytopenia, infections, anaemia
REACH2 (aGVHD)
~20%
Top reasons: Infections, thrombocytopenia, treatment failure
Managing Cytopenias — The Central Safety Challenge

Thrombocytopenia, anaemia, and neutropenia are the defining dose-limiting toxicities of ruxolitinib. In COMFORT-I, the nadir for haemoglobin and platelets typically occurred at weeks 8–12, with partial recovery thereafter. Monthly CBC is mandatory during the dose-stabilisation phase (first 2–4 months), then as clinically indicated. Importantly, dose reduction and interruption are the primary management tools — not growth factor support or erythropoiesis-stimulating agents, which have not been formally studied in combination with ruxolitinib.

Int

Drug Interactions

Ruxolitinib is metabolised by both CYP3A4 (primary) and CYP2C9 (secondary). This dual metabolic pathway means that drugs inhibiting both enzymes simultaneously (notably fluconazole) can produce disproportionately large exposure increases. Ruxolitinib itself is not a clinically significant CYP inhibitor or inducer and is not a P-gp substrate.

MajorFluconazole >200 mg daily (dual CYP3A4/CYP2C9 inhibitor)
MechanismSimultaneous inhibition of both CYP3A4 and CYP2C9 blocks the two major metabolic pathways
EffectPredicted 3–4-fold AUC increase; substantially increased myelosuppression risk
ManagementAvoid combination with fluconazole doses >200 mg daily in all indications (FDA PI)
FDA PI
MajorStrong CYP3A4 inhibitors (e.g., ketoconazole, ritonavir, clarithromycin)
MechanismCYP3A4 inhibition increases ruxolitinib AUC ~91% (ketoconazole)
EffectApproximately doubled exposure; increased haematological toxicity
ManagementMF/PV: reduce dose by 50%. aGVHD + ketoconazole: 5 mg daily. cGVHD: no specific adjustment but monitor closely. See detailed dose tables in FDA PI (Section 2.6)
FDA PI
ModerateFluconazole ≤200 mg daily
MechanismDual CYP3A4/CYP2C9 inhibition at lower doses; estimated ~2-fold AUC increase
EffectModerately increased exposure with greater haematological toxicity risk
ManagementMF/PV: treat as strong CYP3A4 inhibitor — reduce by 50%. GVHD: same rules as strong CYP3A4 inhibitors (FDA PI)
FDA PI
ModerateStrong CYP3A4 inducers (e.g., rifampicin, phenytoin)
MechanismCYP3A4 induction decreases ruxolitinib AUC by 61% and Cmax by 32%
EffectSubstantially reduced ruxolitinib exposure; partially offset by increased active metabolite exposure (~100% increase)
ManagementNo dose adjustment recommended; but monitor closely and titrate based on safety and efficacy. pSTAT3 inhibition reduced by only ~10% despite 61% AUC reduction (FDA PI)
FDA PI
ModerateLive vaccines
MechanismJAK inhibition causes immunosuppression, potentially allowing live vaccine organisms to replicate
EffectRisk of vaccine-related infection
ManagementAvoid live vaccines; complete all recommended vaccinations (including herpes zoster) before initiating ruxolitinib when possible
Clinical practice
Mon

Monitoring

  • CBC with differentialBaseline, then q2–4 weeks until stable, then as indicated
    Routine    Critical for managing thrombocytopenia (dose-limiting), anaemia, and neutropenia. Dose modifications are tied to specific platelet, Hb, and ANC thresholds (FDA PI).
  • Lipid panel8–12 weeks after initiation
    Routine    Total cholesterol, LDL, and triglyceride elevations have been reported. Treat hyperlipidaemia according to standard guidelines (FDA PI Section 5.5).
  • Infection screeningBefore initiating treatment
    Routine    Screen for tuberculosis, hepatitis B (HBsAg, anti-HBc), hepatitis C, and herpes simplex/zoster history. Resolve active serious infections before starting. Consider herpes zoster prophylaxis (FDA PI Section 5.2).
  • Spleen size (MF)Baseline and periodically
    Routine    Measure by palpation or imaging (MRI/CT). Primary efficacy marker: ≥35% spleen volume reduction. Discontinue if no spleen response or symptom improvement after 6 months (FDA PI).
  • Skin examinationPeriodically
    Routine    Non-melanoma skin cancer reported (~6%); perform periodic skin examinations, particularly in patients with prior hydroxyurea use (FDA PI Section 5.4).
  • Cardiovascular risk assessmentBefore initiating and periodically
    Trigger-based    JAK inhibitor class warning for MACE and thrombosis. Assess cardiovascular risk factors; particular caution in patients ≥50 years with existing risk factors (FDA PI Sections 5.6, 5.7).
  • GVHD response assessmentAt 6 months and ongoing
    Trigger-based    Consider tapering ruxolitinib after 6 months in responding patients who have discontinued therapeutic corticosteroids. Taper q8 weeks (FDA PI).
CI

Contraindications & Cautions

Absolute Contraindications

The FDA prescribing information lists no formal contraindications for ruxolitinib.

Relative Contraindications (Specialist Input Recommended)

  • Active serious infection (including TB, hepatitis B, invasive fungal): Serious infections should have resolved before starting ruxolitinib. Screen for TB and hepatitis B before initiation (FDA PI Section 5.2).
  • Severe thrombocytopenia (platelets <50 × 109/L for MF, or <50 for PV): Starting doses cannot be safely administered. Consider alternative therapy or wait for platelet recovery.
  • Pregnancy: Adverse developmental outcomes observed in animal studies at maternally toxic doses. Use only if potential benefit justifies potential risk to the fetus (FDA PI Section 8.1).

Use with Caution

  • Hepatic impairment with low platelets: AUC increases 28–87% across impairment severity. Dose reduction required for any hepatic impairment when platelets are between 100–150 × 109/L. Avoid use if platelets <100 × 109/L and hepatic impairment present (FDA PI Section 2.7).
  • Renal impairment (moderate-to-severe, ESRD on dialysis): Metabolite exposure increases. Dose reduction required for MF patients with platelets 100–150 × 109/L and moderate/severe renal impairment. ESRD patients not on dialysis: avoid use. ESRD on dialysis: give dose after dialysis session only on dialysis days (FDA PI Section 2.7).
  • Concurrent fluconazole >200 mg: Causes excessive ruxolitinib exposure via dual CYP3A4/CYP2C9 inhibition; avoid combination (FDA PI Section 2.6).
  • JAK inhibitor class warnings (MACE, thrombosis, secondary malignancies): These class-wide concerns apply to all JAK inhibitors including ruxolitinib. Consider cardiovascular risk, thrombotic risk, and malignancy risk before initiation (FDA PI Sections 5.6–5.8).
FDA Class-Wide Safety Communication JAK Inhibitor Class Warnings: MACE, Thrombosis, Malignancy, Infections

The FDA requires all JAK inhibitors, including ruxolitinib, to carry warnings for major adverse cardiovascular events (MACE), thrombosis (arterial and venous), secondary malignancies (including lymphoma), and serious infections including tuberculosis, hepatitis B reactivation, herpes zoster, and progressive multifocal leukoencephalopathy (PML). Additional ruxolitinib-specific warnings include symptom exacerbation following abrupt discontinuation in MF patients (including rare septic shock-like syndrome), non-melanoma skin cancer, and lipid elevations. Monthly CBC monitoring during dose stabilisation is mandatory for all indications.

Pt

Patient Counselling

Purpose of Therapy

Ruxolitinib works by blocking specific proteins (JAK1 and JAK2) that are overactive in the condition being treated. For myelofibrosis and polycythemia vera, it helps reduce spleen enlargement and relieve symptoms like fatigue, night sweats, itching, and bone pain, but it does not cure the underlying disease. For graft-versus-host disease, it calms the overactive immune system that is attacking the body’s own tissues after a transplant.

How to Take

Take ruxolitinib at the prescribed dose twice daily, approximately 12 hours apart, with or without food. The dose may be different from other patients because it is based on blood test results. Do not change the dose or stop taking ruxolitinib without talking to the prescriber first, as stopping suddenly can cause symptoms to return quickly and sometimes severely. Ruxolitinib can be given through a nasogastric tube if the patient cannot swallow tablets.

Blood Count Changes
Tell patientRuxolitinib commonly lowers blood counts including platelets, red cells, and white cells. Regular blood tests are needed, especially during the first few months. Patients may feel tired, bruise easily, or need blood transfusions. Report any unusual bleeding, bruising, or signs of infection immediately.
Call prescriberIf experiencing unusual bleeding, unexplained bruising, persistent fatigue, breathlessness, or fever.
Infection Risk
Tell patientRuxolitinib can lower the immune system’s ability to fight infections. Common risks include shingles (herpes zoster), urinary tract infections, and respiratory infections. More serious infections such as tuberculosis and hepatitis B reactivation are possible. Avoid live vaccines while on treatment. Complete all recommended vaccinations before starting if possible.
Call prescriberIf developing fever, chills, painful blistering rash (shingles), persistent cough, or any signs of infection.
Do Not Stop Suddenly (MF/PV)
Tell patientFor patients with myelofibrosis or polycythemia vera: stopping ruxolitinib suddenly can cause disease symptoms to return rapidly, sometimes within days, and can be severe. If treatment needs to be stopped, the prescriber will provide a gradual dose reduction plan.
Call prescriberIf unable to take ruxolitinib for any reason (e.g., surgery, illness, access issues) or if symptoms return after discontinuation.
Skin Checks
Tell patientNon-melanoma skin cancers have been reported in patients taking ruxolitinib. Use sun protection and report any new or changing skin lesions to the prescriber. Regular skin examinations may be recommended.
Call prescriberIf noticing any new skin growths, non-healing sores, or changes to existing moles or skin lesions.
Pregnancy & Breastfeeding
Tell patientRuxolitinib may harm an unborn baby. Discuss pregnancy plans with the prescriber before starting treatment. Breastfeeding should be stopped during treatment and for 2 weeks after the last dose.
Call prescriberIf pregnancy occurs or is suspected during treatment.
Ref

Sources

Regulatory (PI / SmPC)
  1. Jakafi (ruxolitinib) prescribing information. Incyte Corporation. Revised June 2025. DailyMedPrimary regulatory source for all dosing, safety, pharmacokinetic, and drug interaction data cited in this monograph.
Key Clinical Trials
  1. Verstovsek S, Mesa RA, Gotlib J, et al. A double-blind, placebo-controlled trial of ruxolitinib for myelofibrosis. N Engl J Med. 2012;366(9):799–807. doi:10.1056/NEJMoa1110557COMFORT-I trial — first phase 3 evidence establishing ruxolitinib for intermediate/high-risk myelofibrosis with significant spleen volume reduction.
  2. Harrison C, Kiladjian JJ, Al-Ali HK, et al. JAK inhibition with ruxolitinib versus best available therapy for myelofibrosis. N Engl J Med. 2012;366(9):787–798. doi:10.1056/NEJMoa1110556COMFORT-II trial — randomised comparison of ruxolitinib vs best available therapy in MF, demonstrating superiority in spleen volume reduction.
  3. Vannucchi AM, Kiladjian JJ, Griesshammer M, et al. Ruxolitinib versus standard therapy for the treatment of polycythemia vera. N Engl J Med. 2015;372(5):426–435. doi:10.1056/NEJMoa1409002RESPONSE trial — established ruxolitinib in PV patients with inadequate response to or intolerance of hydroxyurea.
  4. Zeiser R, von Bubnoff N, Butler J, et al. Ruxolitinib for glucocorticoid-refractory acute graft-versus-host disease. N Engl J Med. 2020;382(19):1800–1810. doi:10.1056/NEJMoa1917635REACH2 trial — phase 3 evidence for ruxolitinib in steroid-refractory acute GVHD with superior overall response rate.
  5. Zeiser R, Polverelli N, Ram R, et al. Ruxolitinib for glucocorticoid-refractory chronic graft-versus-host disease. N Engl J Med. 2021;385(3):228–238. doi:10.1056/NEJMoa2033122REACH3 trial — established ruxolitinib for chronic GVHD after failure of 1–2 systemic therapies.
Guidelines
  1. Marchetti M, Palandri F, Cattaneo D, et al. Recommendations for the management of myelofibrosis: the SIE, SIES, GITMO position. Blood Adv. 2022;6(2):575–588. doi:10.1182/bloodadvances.2021004856Contemporary consensus guideline on MF management including JAK inhibitor positioning and response assessment criteria.
Mechanistic / Basic Science
  1. Quintás-Cardama A, Vaddi K, Liu P, et al. Preclinical characterization of the selective JAK1/2 inhibitor INCB018424: therapeutic implications for the treatment of myeloproliferative neoplasms. Blood. 2010;115(15):3109–3117. doi:10.1182/blood-2009-04-214957Preclinical characterisation of ruxolitinib demonstrating selective JAK1/JAK2 inhibition and efficacy in MPN models.
Pharmacokinetics / Special Populations
  1. Appeldoorn TYJ, Munnink THO, Morsink LM, et al. Pharmacokinetics and pharmacodynamics of ruxolitinib: a review. Clin Pharmacokinet. 2023;62(4):559–571. doi:10.1007/s40262-023-01225-7Comprehensive PK/PD review covering absorption, distribution, metabolism, drug interactions, and special populations.
  2. Chen X, Shi JG, Emm T, et al. Pharmacokinetics and pharmacodynamics of orally administered ruxolitinib (INCB018424 phosphate) in renal and hepatic impairment patients. Clin Pharmacol Drug Dev. 2014;3(1):34–42. doi:10.1002/cpdd.72Key PK study establishing dose adjustments for patients with renal and hepatic impairment.
  3. Shi JG, Chen X, Emm T, et al. The effect of CYP3A4 inhibition or induction on the pharmacokinetics and pharmacodynamics of orally administered ruxolitinib (INCB018424 phosphate) in healthy volunteers. J Clin Pharmacol. 2012;52(6):809–818. doi:10.1177/0091270011405663Clinical DDI study establishing the effects of ketoconazole (CYP3A4 inhibitor) and rifampicin (CYP3A4 inducer) on ruxolitinib exposure.