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Drug Monograph

Calquence (Acalabrutinib)

acalabrutinib

Bruton Tyrosine Kinase (BTK) Inhibitor — Second Generation · Oral (capsules, tablets) · Hematology-Oncology
Pharmacokinetic Profile
Half-Life
~1–2 h (parent); ~6.4 h (active metabolite ACP-5862)
Metabolism
CYP3A4 (primary) → active metabolite ACP-5862
Protein Binding
97.5% (parent); 98.6% (ACP-5862)
Bioavailability
25% (absolute); food does not affect AUC
Volume of Distribution
~101 L (Vss)
Clinical Information
Drug Class
Second-Generation BTK Inhibitor (selective, covalent)
Available Doses
Capsules: 100 mg; Tablets: 100 mg
Route
Oral (BID dosing approximately every 12 hours)
Renal Adjustment
Not required (mild/moderate); unknown in severe impairment
Hepatic Adjustment
None for mild/moderate; avoid in severe impairment
Pregnancy
May cause fetal harm and dystocia — avoid
Lactation
Not recommended; avoid for 2 weeks after last dose
Schedule / Legal Status
Prescription only (not a controlled substance)
Generic Available
No
Rx

Indications

IndicationApproved PopulationTherapy TypeStatus
CLL or SLLAdultsMonotherapy, or combination with obinutuzumabFDA Approved
CLL or SLL — with venetoclaxAdults (previously untreated, no del(17p)/TP53 mutation)Fixed-duration combination (up to 14 cycles)FDA Approved (Feb 2026)
Previously untreated MCL — with BRAdults ineligible for autologous HSCTCombination with bendamustine + rituximabFDA Approved
Previously treated MCLAdults (≥1 prior therapy)MonotherapyAccelerated Approval

Acalabrutinib is a second-generation, highly selective covalent BTK inhibitor that has become a preferred treatment option for CLL/SLL across all lines of therapy. Its greater selectivity for BTK compared with ibrutinib translates into a lower incidence of off-target cardiac and vascular toxicities, particularly atrial fibrillation and hypertension. In February 2026, acalabrutinib received approval in combination with venetoclax as the first all-oral, fixed-duration regimen for previously untreated CLL based on the AMPLIFY trial. The MCL monotherapy indication remains under accelerated approval, with continued approval contingent on confirmatory trial results.

Off-Label Uses

Waldenström macroglobulinemia: Case series and retrospective data support activity in WM, particularly in patients intolerant of ibrutinib. Evidence quality: Low (retrospective/case series).

Ibrutinib-intolerant CLL/SLL: Phase 2 data demonstrate successful switch to acalabrutinib in patients who discontinued ibrutinib due to intolerance. Evidence quality: Moderate (prospective Phase 2).

Dose

Dosing

Adult Dosing by Clinical Scenario

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
CLL/SLL — monotherapy (any line)100 mg BID100 mg BID200 mg/dayContinue until progression or intolerance
Take approximately every 12 hours; with or without food
CLL/SLL — with obinutuzumab (treatment-naïve)100 mg BID100 mg BID200 mg/dayStart acalabrutinib Cycle 1; start obinutuzumab Cycle 2 for 6 cycles
Give acalabrutinib before obinutuzumab on same day
CLL/SLL — with venetoclax (treatment-naïve, fixed-duration)100 mg BID100 mg BID200 mg/dayUp to 14 cycles (28-day cycles); venetoclax starts Cycle 3 with 5-week ramp-up
AMPLIFY trial-based; first all-oral fixed-duration CLL regimen
Previously untreated MCL — with BR (ineligible for auto-HSCT)100 mg BID100 mg BID200 mg/dayStart Cycle 1 Day 1; BR for 6 cycles; maintenance rituximab every other cycle up to Cycle 30
Acalabrutinib continues beyond BR until progression
Previously treated MCL — monotherapy100 mg BID100 mg BID200 mg/dayAfter ≥1 prior therapy; continue until progression or intolerance
Accelerated approval indication

Dose Modifications for Drug Interactions

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
With moderate CYP3A4 inhibitor100 mg once daily100 mg once daily100 mg/day50% frequency reduction
Resume BID after inhibitor discontinued
With unavoidable strong CYP3A4 inducer200 mg BID200 mg BID400 mg/dayDoubled dose to compensate for reduced exposure
Avoid strong inducers when possible
Clinical Pearl: pH-Dependent Absorption (Capsules Only)

The capsule formulation requires gastric acidity for optimal absorption. Avoid concomitant proton pump inhibitors (PPIs) with capsules. Take acalabrutinib capsules 2 hours before H2-receptor antagonists, and separate from antacids by at least 2 hours. The tablet formulation (acalabrutinib maleate) has pH-independent release and can be co-administered with PPIs without exposure reduction.

Clinical Pearl: Dose Modification for Adverse Reactions

For Grade 3 or greater non-haematologic toxicities, Grade 3 thrombocytopenia with bleeding, or Grade 4 cytopenias lasting more than 7 days: interrupt acalabrutinib until recovery to Grade 1 or baseline. First and second occurrence: resume at 100 mg BID. Third occurrence: resume at 100 mg once daily. Fourth occurrence: discontinue permanently.

PK

Pharmacology

Mechanism of Action

Acalabrutinib is a second-generation, highly selective, irreversible covalent inhibitor of Bruton tyrosine kinase (BTK). It binds to cysteine-481 in the BTK active site via a 2-butynamide warhead that exhibits lower non-specific reactivity than the acrylamide warheads used in first-generation BTK inhibitors. This selectivity profile means acalabrutinib has minimal inhibitory activity against off-target kinases including EGFR, ITK, TEC, and Src family kinases at clinically relevant concentrations, which contributes to a more favourable cardiovascular and bleeding safety profile compared with ibrutinib. By inhibiting BTK, acalabrutinib blocks B-cell receptor signalling, disrupting downstream NF-kB and PI3K/Akt activation, thereby reducing malignant B-cell proliferation, survival, adhesion, and tissue migration. Like ibrutinib, acalabrutinib produces a redistribution lymphocytosis early in treatment that is pharmacodynamic in nature and resolves over time. Twice-daily dosing achieves sustained near-complete BTK occupancy despite the short plasma half-life of the parent compound.

ADME Profile

ParameterValueClinical Implication
AbsorptionRapid; median Tmax 0.5–1 h; absolute bioavailability 25%; food does not affect AUC but decreases Cmax by 54–73%Can be taken with or without food; capsule absorption is pH-dependent—avoid PPIs with capsule formulation
DistributionVss ~101 L; protein binding 97.5% (parent), 98.6% (ACP-5862); blood-to-plasma ratio 0.8Moderate volume of distribution; no clinically significant displacement interactions expected
MetabolismHepatic via CYP3A4 (primary) to active metabolite ACP-5862 (pyrrolidine ring-opened); ACP-5862 has approximately half the potency of parent against BTKCYP3A4 dependence creates significant interaction potential; ACP-5862 contributes to overall pharmacological activity with a longer half-life
EliminationParent t½ ~1–2 h; ACP-5862 t½ ~6.4 h; CL/F ~159 L/h; 84% faecal (<2% unchanged), 12% renalVery short parent half-life but sustained BTK occupancy from irreversible binding and active metabolite; BID dosing essential; no renal dose adjustment needed
SE

Side Effects

Adverse reaction data below are derived from the pooled safety population of 1,764 patients with haematologic malignancies who received acalabrutinib 100 mg approximately every 12 hours in clinical trials (FDA PI, revised January 2025). Acalabrutinib was given as monotherapy (1,256 patients) or in combination (508 patients); 88% were exposed for at least 6 months and 80% for at least 1 year.

≥10%Very Common
Adverse EffectIncidenceClinical Note
Diarrhea37%Usually Grade 1–2; self-limiting; loperamide for symptom control
Upper respiratory tract infection36%Includes nasopharyngitis and sinusitis; Grade 3+ uncommon (≤3%)
Headache35%Often Grade 1; characteristic of acalabrutinib; usually resolves within first months
Musculoskeletal pain33%Includes back pain, myalgia, arthralgia; Grade 3+ in 1–5%
Lower respiratory tract infection32%Includes pneumonia (9%), bronchitis; Grade 3+ in 6–17% (higher with combo)
Fatigue32%Usually Grade 1–2; manageable with supportive care
Neutropenia (lab)23–53%All grades; Grade 3/4 ANC decreased in 26% (monotherapy + obinutuzumab); Grade 4 in 14%
Anaemia (lab)47–53%All grades; Grade 3+ in 10–15%
Thrombocytopenia (lab)32–51%All grades; Grade 3/4 in 3–12%; monitor CBC regularly
Bruising10–31%Includes contusion and ecchymosis; typically cosmetic; Grade 3+ very rare
Rash9–26%Includes dermatitis and related terms; Grade 3+ in 0.6–2%; may require dose interruption in MCL combination setting (up to 12%)
Haemorrhage (any, excl. bruising)40%Any-grade bleeding events excluding bruising/petechiae
Second primary malignancy18%NMSC 10%; other solid tumours 9%; haematologic 1%; annual skin exam recommended
1–10%Common
Adverse EffectIncidenceClinical Note
Atrial fibrillation / flutter3.6–7%All grades; Grade 3/4 in 2.6%; significantly lower than ibrutinib (9.4% vs 16% in ELEVATE-RR)
Hypertension3–5%Lower incidence than ibrutinib; monitor BP at each visit
Arthralgia8–22%Usually Grade 1–2; manageable with analgesics
Nausea19–22%Grade 3 rare; usually transient
Urinary tract infection5–15%Grade 3+ in 1–3%
Constipation15–25%Grade 3 in ≤1%
Dizziness5–20%Usually Grade 1; self-limiting
Peripheral oedema5–20%Usually Grade 1–2
SeriousSerious Adverse Effects (Regardless of Frequency)
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Serious / Grade 3+ infections32%Throughout treatmentEvaluate promptly; respiratory tract infections most common (19%); pneumonia in 9%; consider PJP/antifungal prophylaxis; PML reported
Major haemorrhage (≥Grade 3 / serious / CNS)4.4%Any time; cumulative riskHold acalabrutinib; fatal haemorrhage in 0.2%; withhold 3–7 days pre/post-surgery; caution with antithrombotics
Grade 3/4 atrial fibrillation / flutter2.6%Variable; cumulativeECG; cardiology referral; rate/rhythm control; evaluate benefit-risk of continuation
Ventricular arrhythmias (Grade 3+)0.6%VariableFatal in 0.3%; urgent cardiology evaluation; consider permanent discontinuation
Grade 3/4 cytopeniasANC 26%; ALC 23%; Plt 10%; Hb 10%First months; monitor monthlyHold acalabrutinib; G-CSF for neutropenia; transfuse as needed; resume per dose modification table
Drug-induced liver injury (DILI)Rare (postmarketing)VariableMonitor LFTs; withhold if suspected; permanently discontinue if confirmed
DiscontinuationDiscontinuation Rates
CLL/SLL (ELEVATE-TN, ~28 months)
10–11%
Top reasons: Infections, second primary malignancies, pneumonia
R/R CLL (ASCEND, ~16 months)
10%
Top reasons: Second primary malignancies, infections
Reason for DiscontinuationIncidenceContext
Infections (including COVID-19)Most common in MCL+BRCOVID-19 and pneumonia were leading causes in ECHO trial (43% overall discontinuation with longer follow-up)
Second primary malignanciesNotable in ASCENDNMSC and other solid tumours; 18% overall SPM rate
Atrial fibrillationLower than ibrutinibLower AF-driven discontinuation vs ibrutinib (14.7% vs 21.3% for all-AE discontinuation in ELEVATE-RR)
Headache: A Distinctive Early Side Effect

Headache occurs in approximately 35% of patients receiving acalabrutinib, which is notably more frequent than with ibrutinib. It is typically Grade 1 in severity, occurs early in treatment, and usually resolves within the first few months without dose modification. Simple analgesics (paracetamol) are effective; if headache is severe or persistent, ensure adequate hydration and consider caffeine intake patterns.

Int

Drug Interactions

Acalabrutinib is extensively metabolised by CYP3A4 and its capsule formulation requires gastric acidity for optimal absorption, creating two distinct axes of clinically significant interactions. Acalabrutinib is also an inducer of CYP1A2, CYP2B6, and CYP3A4, and an inhibitor of BCRP. Co-administration with itraconazole (strong CYP3A4 inhibitor) increased acalabrutinib exposure approximately 2–3-fold.

MajorStrong CYP3A4 Inhibitors (ketoconazole, itraconazole, clarithromycin)
MechanismCYP3A4 inhibition increases acalabrutinib plasma concentrations
Effect2–3-fold increase in acalabrutinib exposure; increased toxicity risk
ManagementAvoid concomitant use. If short-term use needed (≤7 days), interrupt acalabrutinib during the course.
FDA PI
ModerateModerate CYP3A4 Inhibitors (fluconazole, erythromycin, diltiazem, verapamil)
MechanismPartial CYP3A4 inhibition
EffectModerate increase in acalabrutinib exposure
ManagementReduce acalabrutinib to 100 mg once daily (from BID). Resume BID after inhibitor is cleared.
FDA PI
MajorStrong CYP3A4 Inducers (rifampin, carbamazepine, phenytoin, St. John’s Wort)
MechanismCYP3A4 induction accelerates acalabrutinib clearance
EffectMarked reduction in acalabrutinib exposure; potential loss of efficacy
ManagementAvoid concomitant use. If unavoidable, increase acalabrutinib to 200 mg BID.
FDA PI
MajorProton Pump Inhibitors (omeprazole, pantoprazole, esomeprazole)
MechanismElevated gastric pH reduces capsule dissolution and absorption
EffectReduced acalabrutinib exposure with capsule formulation; may compromise efficacy
ManagementAvoid PPIs with capsules. The tablet formulation (acalabrutinib maleate) has pH-independent release and can be co-administered with PPIs.
FDA PI
ModerateH2-Receptor Antagonists (ranitidine, famotidine)
MechanismReduced gastric acidity impairs capsule absorption
EffectModerately reduced acalabrutinib levels
ManagementTake acalabrutinib 2 hours before the H2-receptor antagonist. Tablet formulation avoids this issue.
FDA PI
MinorAntacids (calcium carbonate, aluminium/magnesium hydroxide)
MechanismTransient gastric pH elevation
EffectPotentially reduced capsule absorption
ManagementSeparate dosing by at least 2 hours
FDA PI
ModerateAnticoagulants / Antiplatelet Agents
MechanismAdditive bleeding risk from BTK-related platelet effects
EffectMajor haemorrhage 4% with antithrombotics vs 7% without (note: paradoxical finding may reflect higher baseline risk in non-anticoagulated patients)
ManagementWeigh benefit-risk carefully; avoid warfarin if possible; prefer DOACs; monitor for bleeding
FDA PI
ModerateBCRP / MATE1 Substrates (rosuvastatin, methotrexate, topotecan)
MechanismAcalabrutinib inhibits BCRP transporter; its active metabolite ACP-5862 inhibits MATE1
EffectPotential increased exposure of BCRP substrate drugs
ManagementMonitor for substrate toxicity; consider dose adjustment of BCRP substrates if needed
FDA PI
Mon

Monitoring

  • Complete Blood CountRegularly during treatment
    Routine    Grade 3/4 cytopenias: ANC decreased 26%, ALC decreased 23%, platelets 10%, Hb 10%, Grade 4 neutropenia 14%. Interrupt, reduce, or discontinue per dose modification guidelines.
  • Hepatic FunctionBaseline, then periodically
    Routine    Bilirubin and transaminases at baseline and throughout treatment. DILI has been reported with BTK inhibitors including acalabrutinib (postmarketing). Increase monitoring frequency if abnormal values develop.
  • Cardiac RhythmBaseline + as indicated
    Routine    AF/flutter all grades in 7%, Grade 3/4 in 2.6%. Ventricular arrhythmias Grade 3+ in 0.6% (fatal in 0.3%). Evaluate symptoms of palpitations, syncope, or dyspnoea with ECG. Higher risk with cardiac comorbidities.
  • Bleeding SignsEach visit; ongoing
    Routine    Major haemorrhage in 4.4%, fatal in 0.2%. Assess bruising, petechiae, and signs of internal bleeding. Withhold 3–7 days pre/post-surgery depending on procedure type and bleeding risk.
  • Infection SurveillanceEach visit; ongoing
    Routine    Serious/Grade 3+ infections in 32%. Respiratory tract infections most common (19%); neutropenic infection in 2.7%. Consider PJP and antifungal prophylaxis. Evaluate new neurological symptoms for PML. HBV reactivation can occur—screen before initiation.
  • Skin ExaminationBaseline, then annually
    Routine    Second primary malignancies in 18%, NMSC in 10%, other solid tumours in 9%. Advise sun protection. Annual dermatological review recommended.
  • Blood PressureEach visit
    Routine    Hypertension reported in 3–5% (lower than ibrutinib). Initiate antihypertensives as needed.
  • Pregnancy StatusBefore initiation
    Trigger-based    Verify pregnancy status in females of reproductive potential. Advise contraception during treatment and for 1 week after last dose. May cause fetal harm and dystocia.
CI

Contraindications & Cautions

Absolute Contraindications

  • Pregnancy: Animal studies demonstrated fetal harm (reduced growth in rabbits) and dystocia (rats) at exposures 2 times the human dose. Must not be used in pregnant women.
  • Severe hepatic impairment: PK data unavailable; markedly increased exposure expected. Use should be avoided.

Relative Contraindications (Specialist Input Recommended)

  • Active severe bleeding or recent CNS haemorrhage: Major haemorrhage rate 4.4% with fatal events in 0.2%. Specialist risk-benefit assessment required.
  • Concomitant strong CYP3A4 inhibitor therapy (chronic): 2–3-fold exposure increase with strong inhibitors. Avoid if possible; short-term use (≤7 days) requires acalabrutinib interruption.
  • Pre-existing uncontrolled atrial fibrillation: Although AF risk is lower than ibrutinib, pre-existing arrhythmias warrant cardiology input before initiation.

Use with Caution

  • Patients on anticoagulants or antiplatelet agents: Additive bleeding risk. Avoid warfarin; DOACs preferred if anticoagulation required.
  • Patients on PPIs (capsule formulation): Switch to tablet formulation or alternative acid-reducing strategy to avoid absorption impairment.
  • Elderly (≥65 years): 67% of the pooled safety population were ≥65. Grade 3 or higher adverse reactions were more common in older patients.
  • Patients with cardiac risk factors: Higher susceptibility to arrhythmias; baseline cardiac evaluation recommended.
  • Planned surgery within 3–7 days: Withhold acalabrutinib peri-operatively due to haemorrhagic risk.
  • Patients at risk for HBV reactivation: Screen for hepatitis B before starting; reactivation has been reported.
FDA Class-Wide Safety Advisory Cardiac Arrhythmias — BTK Inhibitors

Fatal and serious cardiac arrhythmias have occurred with acalabrutinib. Grade 3 or 4 atrial fibrillation or flutter was reported in 2.6% of 1,764 treated patients. All-grade AF/flutter occurred in 7%. Grade 3 or higher ventricular arrhythmia events were reported in 0.6%, including fatal cases in 0.3%. The risk may be increased in patients with cardiac risk factors, hypertension, prior arrhythmias, and acute infection.

FDA Class-Wide Safety Advisory Hepatotoxicity, Including Drug-Induced Liver Injury — BTK Inhibitors

Severe, life-threatening, and potentially fatal cases of DILI have been reported with BTK inhibitors, including acalabrutinib. Monitor bilirubin and transaminases at baseline and throughout treatment. Withhold if DILI is suspected; permanently discontinue if confirmed.

Pt

Patient Counselling

Purpose of Therapy

Acalabrutinib works by blocking a protein called BTK that cancer cells need to grow and survive. It is a targeted oral therapy—not traditional chemotherapy. Most patients take it twice daily as a continuous treatment to keep their disease under control. A temporary rise in white blood cell count or swelling of lymph nodes early in treatment is expected and is not a sign of treatment failure.

How to Take

Take one capsule or tablet twice daily, approximately 12 hours apart, with or without food. Swallow capsules whole—do not open, break, or chew them. Tablets should not be crushed or cut. If a dose is missed by more than 3 hours, skip it and take the next dose at the scheduled time. Never double up on doses.

Headache
Tell patientHeadache is common with acalabrutinib, especially in the first few months, and usually resolves on its own. Paracetamol (acetaminophen) is safe to use for relief. Stay well hydrated.
Call prescriberSevere or persistent headache not relieved by over-the-counter pain medication, or headache accompanied by visual changes, confusion, or neck stiffness.
Bleeding & Bruising
Tell patientAcalabrutinib can affect how your blood clots. You may notice easier bruising. Avoid high-injury activities. Inform all healthcare providers, including dentists, that you take this medication. Avoid NSAIDs unless approved by your oncologist.
Call prescriberBlood in urine or stools, black tarry stools, prolonged nosebleeds, vomiting blood, severe headache with vision changes, or any unexpected heavy bleeding.
Infection Risk
Tell patientYour immune system may be weakened during treatment. Practice good hand hygiene, avoid close contact with sick individuals, and stay up to date with recommended vaccinations (avoid live vaccines).
Call prescriberFever ≥38°C (100.4°F), chills, persistent cough, painful urination, or any signs of infection.
Heart Rhythm Changes
Tell patientWhile less common than with some other BTK inhibitors, acalabrutinib can occasionally affect heart rhythm. Report any new symptoms promptly for early management.
Call prescriberPalpitations, racing or irregular heartbeat, dizziness, lightheadedness, fainting, unusual shortness of breath, or chest discomfort.
Acid-Reducing Medications
Tell patientIf you take the capsule form, avoid proton pump inhibitors (omeprazole, pantoprazole, etc.) as they reduce absorption. If you need acid-reducing medication, your doctor may switch you to the tablet form or recommend timing adjustments with H2-blockers or antacids.
Call prescriberIf you are prescribed a new acid-reducing medication by another healthcare provider, inform your oncologist before starting it.
Drug Interactions
Tell patientMany medications can interfere with acalabrutinib. Always inform your oncologist and pharmacist before starting any new prescription, over-the-counter medication, or herbal supplement—particularly antifungal drugs, antibiotics, and seizure medications. Avoid St. John’s Wort.
Call prescriberBefore starting any new medication from any healthcare provider.
Surgery & Dental Procedures
Tell patientAcalabrutinib needs to be paused before and after surgery due to bleeding risk. Your oncologist will advise on timing (usually 3–7 days). Always inform surgeons and dentists that you take this medication.
Call prescriberWhenever any procedure is being planned.
Pregnancy & Contraception
Tell patientAcalabrutinib can harm an unborn baby and cause problems during childbirth. Women who could become pregnant must use effective contraception during treatment and for at least 1 week after the last dose. Do not breastfeed during treatment and for at least 2 weeks after the last dose.
Call prescriberIf you become pregnant or suspect you may be pregnant.
Sun Protection
Tell patientThere is an increased risk of skin cancers during treatment. Use sunscreen (SPF 30+), wear protective clothing, and avoid prolonged sun exposure. Report any new or changing skin lesions to your doctor.
Call prescriberNew skin growths, moles that change in size/colour/shape, or non-healing skin wounds.
Ref

Sources

Regulatory (PI / SmPC)
  1. Calquence (acalabrutinib) capsules prescribing information. AstraZeneca Pharmaceuticals LP. Revised January 2025. FDA Label (Capsules)Primary source for all dosing, indications, adverse reactions, warnings, and pharmacokinetic data in this monograph.
  2. Calquence (acalabrutinib) tablets prescribing information. AstraZeneca Pharmaceuticals LP. 2025. FDA Label (Tablets)Tablet formulation PI with pH-independent PK data and additional clinical information.
Key Clinical Trials
  1. Sharman JP, Egyed M, Jurczak W, et al. Acalabrutinib with or without obinutuzumab versus chlorambucil and obinutuzumab for treatment-naïve chronic lymphocytic leukaemia (ELEVATE-TN): a randomised, controlled, phase 3 trial. Lancet. 2020;395(10232):1278–1291. doi:10.1016/S0140-6736(20)30262-2Pivotal Phase 3 trial demonstrating superiority of acalabrutinib ± obinutuzumab over chlorambucil-obinutuzumab in treatment-naïve CLL.
  2. Ghia P, Pluta A, Wach M, et al. Acalabrutinib versus investigator’s choice in relapsed/refractory chronic lymphocytic leukemia: final ASCEND trial results. Hemasphere. 2022;6(12):e801. doi:10.1097/HS9.0000000000000801Final 4-year analysis of ASCEND trial confirming durable PFS benefit of acalabrutinib monotherapy in relapsed/refractory CLL.
  3. Byrd JC, Hillmen P, Ghia P, et al. Acalabrutinib versus ibrutinib in previously treated chronic lymphocytic leukemia: results of the first randomized phase III trial. J Clin Oncol. 2021;39(31):3441–3452. doi:10.1200/JCO.21.01210ELEVATE-RR trial; first head-to-head Phase 3 comparison of two BTK inhibitors, demonstrating noninferior PFS and lower AF with acalabrutinib.
  4. Wang M, Rule S, Zinzani PL, et al. Acalabrutinib in relapsed or refractory mantle cell lymphoma (ACE-LY-004): a single-arm, multicentre, phase 2 trial. Lancet. 2018;391(10121):659–667. doi:10.1016/S0140-6736(17)33108-2Registration trial supporting accelerated approval in previously treated MCL; demonstrated 81% ORR.
  5. FDA Press Release: FDA approves acalabrutinib with venetoclax for chronic lymphocytic leukemia or small lymphocytic lymphoma. February 19, 2026. FDARegulatory announcement for the AMPLIFY trial-based approval of the first all-oral fixed-duration CLL regimen.
Guidelines
  1. National Comprehensive Cancer Network (NCCN). Clinical Practice Guidelines in Oncology: Chronic Lymphocytic Leukemia/Small Lymphocytic Lymphoma. Version 2.2026. NCCNPositions acalabrutinib as a preferred BTK inhibitor option for CLL/SLL across treatment lines.
Mechanistic / Basic Science
  1. Barf T, Covey T, Izumi R, et al. Acalabrutinib (ACP-196): a covalent Bruton tyrosine kinase inhibitor with a differentiated selectivity and in vivo potency profile. J Pharmacol Exp Ther. 2017;363(2):240–252. doi:10.1124/jpet.117.242909Preclinical characterisation of acalabrutinib demonstrating its selectivity advantage over ibrutinib across a kinase panel.
  2. Wu J, Zhang M, Liu D. Acalabrutinib (ACP-196): a selective second-generation BTK inhibitor. J Hematol Oncol. 2016;9:21. doi:10.1186/s13045-016-0250-9Review of acalabrutinib’s mechanism of action, selectivity profile, and early clinical development.
Pharmacokinetics / Special Populations
  1. Podoll T, Pearson PG, Evarts J, et al. Bioavailability, biotransformation, and excretion of the covalent Bruton tyrosine kinase inhibitor acalabrutinib in rats, dogs, and humans. Drug Metab Dispos. 2019;47(2):145–154. doi:10.1124/dmd.118.084459Human mass balance and bioavailability study confirming 25% oral bioavailability and metabolic pathways.
  2. Edlund H, Melin J, Parra-Guillen ZP, et al. Population pharmacokinetics of the BTK inhibitor acalabrutinib and its active metabolite in healthy volunteers and patients with B-cell malignancies. Clin Pharmacokinet. 2019;58(5):659–672. doi:10.1007/s40262-018-0731-8Population PK model characterising acalabrutinib and ACP-5862 absorption, distribution, and elimination.
  3. Sharma S, Lau H, Engst S, et al. Bioequivalence and relative bioavailability studies to assess a new acalabrutinib formulation that enables coadministration with proton-pump inhibitors. Clin Pharmacol Drug Dev. 2023;12(1):78–89. doi:10.1002/cpdd.1153Bioequivalence data for the acalabrutinib maleate tablet demonstrating pH-independent release enabling PPI co-administration.
  4. Sharman JP, Egyed M, Jurczak W, et al. Acalabrutinib-obinutuzumab improves survival vs chemoimmunotherapy in treatment-naive CLL in the 6-year follow-up of ELEVATE-TN. Blood. 2025;146(11):1276–1288. doi:10.1182/blood.20240274686-year follow-up confirming sustained PFS benefit and consistent long-term safety profile of acalabrutinib in CLL.