How to access Calquence for CLL/SLL or mantle cell lymphoma from the UAE: 2026 pathway via UAE haematology and pharmacy supply
*Clinically reviewed by Mohammad Ali, MD (US-trained physician, Chief AI Officer, Reserve Meds). Last reviewed 2026-05-20.
The UAE has one of the deepest adult haematology and lymphoma networks in the wider region. Cleveland Clinic Abu Dhabi haematology, Sheikh Shakhbout Medical City (SSMC) with its MD Anderson affiliation, Tawam Hospital oncology, Burjeel Medical City, American Hospital Dubai, Mediclinic City Hospital, NMC Specialty, and the wider private and DHA-coordinated network run programmes that treat chronic lymphocytic leukemia, small lymphocytic lymphoma, and mantle cell lymphoma through the full therapeutic arc. Calquence (acalabrutinib, AstraZeneca) is the selective second-generation Bruton tyrosine kinase (BTK) inhibitor that has become a default option since the November 2019 FDA approval in CLL/SLL, the October 2017 accelerated approval in mantle cell lymphoma, and the January 2025 expansion to newly-diagnosed MCL in combination with bendamustine plus rituximab. For a UAE-resident adult with CLL, SLL, or MCL whose treating haematologist is weighing BTK inhibitor therapy, the operational question is no longer whether selective second-generation BTK blockade is reachable: it is whether Calquence is the right fit, which formulation (capsule or maleate tablet), how the prescription is dispensed, what insurance will and will not cover, and how the twice-daily oral routine fits into a UAE family's life over years.
This page explains how the pathway works in 2026 for a UAE-resident patient: who qualifies, where the prescribing haematologist conversation happens, how Calquence is dispensed, what the dosing and monitoring look like, what the realistic out-of-pocket exposure band is in AED, what to monitor (atrial fibrillation, hypertension, second primary malignancies, hepatitis B reactivation), and how the long-term treatment course fits into UAE life. It is concierge documentation written for a family already in conversation with a treating haematologist who wants the operational reality laid out plainly.
Why Calquence, and why now
Calquence is acalabrutinib, a selective second-generation Bruton tyrosine kinase inhibitor developed by AstraZeneca. The mechanism distinguishes Calquence from the first-generation BTK inhibitor Imbruvica (ibrutinib): Calquence has greater selectivity for BTK and less off-target activity at EGFR, ITK, TEC, and other kinases that drive ibrutinib-class toxicity. The clinical translation in the head-to-head ELEVATE-RR trial in relapsed or refractory CLL was a meaningful reduction in atrial fibrillation (9.4% with acalabrutinib versus 16.0% with ibrutinib), hypertension, major bleeding, and treatment discontinuation for adverse events, with non-inferior progression-free survival.
The FDA approved Calquence for mantle cell lymphoma after one prior therapy in October 2017 (accelerated approval), then for CLL and SLL in November 2019. The Calquence Maleate Tablet formulation was approved in August 2022; same 100 mg twice-daily dosing but no pH-dependent absorption, so patients on PPIs or H2 blockers can take the tablet form without dose timing constraints. The January 2025 approval added newly-diagnosed mantle cell lymphoma in combination with bendamustine and rituximab. UAE EDE registration status is verified at intake.
For a UAE-resident adult with CLL, SLL, or MCL whose treating haematologist is weighing BTK inhibitor therapy, Calquence is the selective second-generation option with the strongest head-to-head safety data versus ibrutinib. The conversation about which BTK inhibitor (Calquence, Imbruvica, Brukinsa, or Jaypirca) the patient should start, or whether to use a BCL2 inhibitor combination (venetoclax plus obinutuzumab) instead, is the central clinical decision. This page is the operational layer underneath that conversation.
Reserve Meds does not promote one BTK inhibitor over another. The page describes the Calquence pathway because Calquence is the drug the patient has asked about.
What Calquence is, in plain language
Calquence is an oral capsule or tablet taken twice daily. There is no infusion, no inpatient stay, no specialty-centre administration. The standard dose is 100 mg twice daily, with or without food, approximately 12 hours apart. The capsule formulation has pH-dependent absorption: patients taking proton pump inhibitors should switch to the maleate tablet form or separate the capsule dose from antacid by the prescribing information schedule. The tablet form has no PPI interaction.
This is not a short-course therapy. Calquence is taken for as long as the disease responds and the patient tolerates the drug.
Eligibility at a UAE haematologist clinic
For UAE-resident patients, the major haematology and lymphoma services apply the FDA criteria with local insurance adaptation:
1. Confirmed indication. CLL or SLL meeting iwCLL treatment criteria; mantle cell lymphoma confirmed by pathology with cyclin D1 expression; for newly-diagnosed MCL combination, multi-disciplinary tumour board decision. 2. Treatment history. For relapsed or refractory CLL/SLL or MCL, prior therapy documentation. For newly-diagnosed MCL, candidacy for the bendamustine and rituximab combination assessed by the treating haematologist. 3. Adult (18+). No paediatric indication for Calquence. 4. Hepatitis B and HIV screening. HBsAg and anti-HBc are mandatory before BTK inhibitor initiation because of documented HBV reactivation risk; patients with prior HBV exposure require antiviral prophylaxis and hepatology co-management. 5. Pregnancy planning discussion for women of childbearing potential. Effective contraception during treatment and for two days after the last dose. 6. Drug interaction review. Strong CYP3A inhibitors and strong CYP3A inducers require dose adjustment or alternative. For capsule users on PPIs or H2 blockers, conversion to the maleate tablet form is the cleaner solution. 7. Second primary malignancy counsel. BTK inhibitor class has a documented signal for second primary malignancies, especially non-melanoma skin cancers; annual dermatology review is the standard. 8. Atrial fibrillation and cardiovascular risk review. Baseline ECG and blood pressure check. Patients with pre-existing AF or significant cardiovascular disease require cardiology co-management. 9. Tumour lysis syndrome risk assessment in CLL with high tumour burden.
A UAE patient should arrive at the BTK inhibitor conversation with pathology and immunophenotyping confirming CLL, SLL, or MCL, prior treatment history with response durations, HBV and HIV serology, baseline ECG and blood pressure, CBC with differential, CMP, and the insurance preauthorisation paperwork that the prescribing office typically initiates.
The UAE prescribing and supply picture, plainly
Calquence UAE EDE registration status is verified at intake. AstraZeneca MENA commercial supply runs through regional distributors with Cleveland Clinic Abu Dhabi, SSMC, Tawam, Burjeel Medical City, American Hospital Dubai, Mediclinic City, and the wider DHA-coordinated network as major dispensing centres. Where in-country registration is current, in-country pharmacy dispensing applies. Where the newer maleate tablet formulation has not yet caught up with the FDA label, a named-patient supply pathway covers the case.
1. Prescribing physician: a board-certified UAE haematologist or medical oncologist with lymphoma experience. Cleveland Clinic Abu Dhabi haematology, SSMC, Tawam, Burjeel Medical City, American Hospital Dubai, Mediclinic City, NMC Specialty, and the wider network are the major centres. 2. Pharmacy dispensing: hospital pharmacy if prescribed in the specialty outpatient setting; community pharmacy with prescribing physician coordination for ongoing maintenance. Capsules and tablets stored at room temperature. 3. Insurance pre-authorisation: Thiqa coverage for Emirati nationals has historically extended to BTK inhibitor therapy in CLL and MCL on a case-by-case basis with documented indication. Daman and the major commercial insurers (Oman Insurance, AXA Gulf, MetLife, Cigna, others) require similar documentation. `` 4. Ongoing monitoring: haematology follow-up at week 2, week 4, then monthly for the first 6 months, then every 3 months. CBC, CMP, blood pressure, and HBV viral load (if applicable) at each visit. Annual dermatology review.
Cost band and insurance positioning
US list price for Calquence is approximately USD 15,000 to 17,500 per month at WAC. Annual cost at list price is approximately USD 175,000 to 210,000. At 2026 indicative cross rates, the AED-equivalent annual cost band is approximately AED 642,000 to 771,000 at list price.
For Emirati nationals with Thiqa coverage, the financial pre-authorisation conversation needs to start before the first dispensing. Daman and other commercial covers vary; the prescribing office is the gating step.
What to expect on Calquence, week-by-week
Week 0: Baseline workup completed (HBV, HIV, ECG, blood pressure, CBC, CMP, dermatology baseline if applicable). First Calquence dose dispensed.
Week 1 to 2: Headache is very common in the first 1 to 2 weeks (more than 30% of patients), typically transient and responsive to paracetamol or caffeine. Mild diarrhoea is also common. Most patients report these settle by week 4.
Week 2 to 4: First haematology follow-up. CBC to assess neutrophil and platelet trajectory. Blood pressure check. Adverse event review.
Month 2 to 6: Monthly haematology follow-up. Response assessment by imaging or clinical exam.
Month 6 onwards: Every-3-month haematology follow-up for stable responders. Annual dermatology review.
Year 1 onwards: Long-term maintenance for as long as the disease responds and the patient tolerates the drug.
When Calquence is the wrong drug
For a UAE patient with active untreated hepatitis B without antiviral prophylaxis, with severe uncontrolled hypertension, with significant pre-existing atrial fibrillation that has not been optimised by cardiology, during pregnancy when effective contraception cannot be ensured, or where strong CYP3A inhibitor or inducer therapy cannot be modified, the operational pathway shifts:
- Other BTK inhibitors (Imbruvica, Brukinsa, Jaypirca): each has a distinct safety profile. - BCL2 inhibitor combination (venetoclax plus obinutuzumab or rituximab): fixed-duration alternative to indefinite BTK inhibitor therapy in CLL. - Chemo-immunotherapy (bendamustine plus rituximab, FCR, R-CHOP for MCL induction): where targeted therapy is contraindicated or not yet warranted.
Reserve Meds does not promote one BTK inhibitor over another. If the conversation with the treating haematologist points toward a different BTK inhibitor, a BCL2 combination, or chemo-immunotherapy, the operational pathway shifts accordingly.
What Reserve Meds does on this case
We are a US-based concierge coordinator. We are not the prescriber and not the dispensing pharmacy. On a UAE Calquence case we build the documentation pack with the treating haematologist office, confirm UAE EDE registration status per formulation and the appropriate dispensing pathway, run the insurance pre-authorisation conversation alongside the clinical preauthorisation, coordinate the supply logistics for ongoing dispensing, organise baseline screening that the prescribing office requires, and stay with the case through the first year of dosing with handoff to the local prescriber for ongoing surveillance. Clinical decisions remain with your treating haematologist.
Composite case examples; no individual patient is depicted. This content is for general information and does not constitute medical advice. Reserve Meds is a US-based concierge coordinator; we are not the prescriber and not the dispensing pharmacy. Clinical decisions remain with your treating haematologist.
Clinical and regulatory review: Mohammad Ali, MD (US-trained physician, Chief AI Officer, Reserve Meds). Last medically reviewed: 2026-05-20.
Regulatory status of Calquence (acalabrutinib) in UAE, 2026
Calquence (acalabrutinib) is approved by the US Food and Drug Administration for the labelled indication of chronic lymphocytic leukaemia, small lymphocytic lymphoma, and mantle cell lymphoma (see the FDA approval record at accessdata.fda.gov). The European Medicines Agency holds a parallel marketing authorisation where applicable (see the EMA EPAR at ema.europa.eu). For a UAE-based patient, the access pathway runs through the Ministry of Health and Prevention (MOHAP) and Department of Health Abu Dhabi (DoH) framework. The official regulator portal is at www.mohap.gov.ae; the locally registered medicines list is at www.mohap.gov.ae/en/services/drug-registration.
Where Calquence (acalabrutinib) is held on the locally registered list at the time the case opens, standard prescription and in-country dispensing applies and the treating consultant at the prescribing tertiary centre coordinates supply through the institutional pharmacy. Where Calquence (acalabrutinib) is not yet on the locally registered list at the time the case opens, the named-patient and personal-import framework that the Ministry of Health and Prevention (MOHAP) and Department of Health Abu Dhabi (DoH) maintains for reference-authority-approved medicines is the operative route. The qualifying conditions are well established: the medicine is approved by a recognised reference authority (FDA or EMA qualifies), no locally available alternative is clinically equivalent for the specific patient indication, the treating physician of record takes documented clinical responsibility, and chain of custody is preserved end to end from the US source through international transit to the named dispensing facility. Confirm current registration status at intake; the published registration list governs.
Tertiary centers and clinical coordination in UAE
The UAE tertiary referral network for a Calquence (acalabrutinib) case is concentrated at Cleveland Clinic Abu Dhabi (CCAD), Sheikh Shakhbout Medical City (SSMC), Tawam Hospital Al Ain, Mediclinic Parkview Hospital Dubai, and Burjeel Medical City. These centers carry the haematology, oncology, neurology, metabolic, infectious-disease, or rare-disease specialist staffing and the institutional pharmacy and import-license operations that the named-patient pathway requires. For second-generation selective Bruton tyrosine kinase (BTK) inhibitor therapies that require specialised infusion infrastructure, baseline organ-function workup, or post-treatment monitoring of a complexity beyond what a community centre is configured for, the case is routinely referred to one of these tertiary centers from the outset.
For oral, subcutaneous, or in-clinic infusion therapies that can be administered in UAE once imported, the tertiary centres dispense and monitor under their institutional pharmacy operations. Reserve Meds handles US-side sourcing under Drug Supply Chain Security Act (DSCSA) chain-of-custody documentation, international shipment to the named dispensing facility, and re-supply cadence aligned to the dosing schedule. For therapies that require US-certified treatment center administration (some cell, gene, and complex biologics fall in this bucket), the practical access pathway runs through patient travel to a US-certified treatment center rather than import into UAE; the UAE tertiary team continues to handle upstream referral package assembly and the long-term follow-up after the patient returns home.
UAE pricing reference and payer posture, 2026
Reserve Meds publishes a drug-only US cash-pay reference range at intake and issues a delivered, itemised quote within 24 hours once the treating physician's documentation is in. The 2026 reference rate used for AED conversion is 1 USD = 3.673 AED. As an illustrative composite case in the 2026 reference band, the US cash-pay drug-only cost for Calquence (acalabrutinib) reflects the US wholesale acquisition cost published by the manufacturer (AstraZeneca) plus standard specialty pharmacy markup; the precise band is delivered in the case quote because it varies by indication, dosing, and pack size.
Logistics, international shipment, chain-of-custody documentation, cold-chain handling where applicable, Reserve Meds concierge coordination, and any patient and caregiver travel and accommodation are itemised separately. For a complex case the total course cost commonly lands meaningfully above the drug-only band once treatment-centre fees, pre-treatment workup, on-treatment monitoring, complication management, and family logistics are added in.
Payer posture in UAE is overwhelmingly cash-pay for named-patient imports and cross-border specialty cases. The relevant public-payer body is Daman (Abu Dhabi) and Dubai Health Authority (DHA Sehati and Dhamani); the portal is at www.doh.gov.ae. Public coverage generally does not extend to non-locally-registered specialty cases. Private health insurance plans review case-by-case on a pre-authorisation basis when the documentation package is strong, but cash-pay should be assumed as the default at intake.
Access barriers and how Reserve Meds clears them
The five access barriers we see most often for a Calquence (acalabrutinib) case in UAE are: (1) Regulatory documentation complexity. The Ministry of Health and Prevention (MOHAP) and Department of Health Abu Dhabi (DoH) named-patient and personal-import application package requires a specific bundle (physician clinical rationale letter, prescription, patient identifier, product strength and quantity, chain-of-custody plan, evidence of reference-authority approval, and confirmation that no locally available alternative is clinically equivalent for the patient). Reserve Meds provides physician-facing templates that match the format reviewers expect. (2) US-side sourcing and DSCSA chain-of-custody. We coordinate with our US-licensed specialty wholesale partners to secure Calquence (acalabrutinib) from authorised distribution under the US Drug Supply Chain Security Act, logging every transfer point through to international shipment.
(3) Clinical eligibility documentation. The treating consultant at the prescribing tertiary centre defines eligibility against the FDA labelled indication and the relevant clinical-practice guideline; Reserve Meds does not adjudicate the clinical decision. (4) Family logistics. Patient and caregiver travel where applicable, accommodation near the treatment center where applicable, in-country transport, translator support where needed, and post-treatment data flow back to the treating UAE physician are coordinated as a single arc. (5) Insurance and payer posture. Cash-pay is the default. Where private insurance review is contemplated, we supply documentation for the family's submission but we do not bill insurers and we do not adjudicate insurance disputes.
Drug-specific clinical context for Calquence (acalabrutinib): the labelled indication is chronic lymphocytic leukaemia, small lymphocytic lymphoma, and mantle cell lymphoma. The second-generation selective Bruton tyrosine kinase (BTK) inhibitor mechanism shapes both the eligibility workup and the monitoring schedule. The relevant clinical-practice guideline body is National Comprehensive Cancer Network (NCCN) CLL/SLL and B-cell lymphoma guidelines at www.nccn.org/guidelines/category_1. The treating physician of record makes the clinical decision; Reserve Meds is the coordination layer that clears the operational and regulatory barriers between the prescription and the delivered course.
Recent regulatory and access news for Calquence (acalabrutinib) in UAE, 2026
The Ministry of Health and Prevention (MOHAP) and Department of Health Abu Dhabi (DoH) portal at www.mohap.gov.ae and the locally registered medicines list at www.mohap.gov.ae/en/services/drug-registration are the authoritative source for the current UAE listing status of Calquence (acalabrutinib); the snapshot date governs. The FDA Drug Safety Communications feed at fda.gov drug-safety-communications and the FDA Drug Shortages list at accessdata.fda.gov drugshortages are the authoritative sources for any active Calquence (acalabrutinib) safety advisory or shortage signal over the most recent 12-month window. The FDA labelled indication for Calquence (acalabrutinib) remains chronic lymphocytic leukaemia, small lymphocytic lymphoma, and mantle cell lymphoma (see the current FDA approval record at accessdata.fda.gov). AstraZeneca continues commercial supply per the FDA-labelled indication and the EMA marketing authorisation. The National Comprehensive Cancer Network (NCCN) CLL/SLL and B-cell lymphoma guidelines guidance at www.nccn.org/guidelines/category_1 remains the relevant clinical-practice reference. Reserve Meds refreshes this snapshot per case at intake; the snapshot date governs.