Is CAR-T therapy available on the NHS?

Yes, several CAR-T products are approved by NICE for specific blood cancers, including ALL and DLBCL. However, access is limited to approved indications and specific treatment lines. Clinical trials offer access to newer CAR-T constructs and for conditions where CAR-T is not yet approved.

How long does CAR-T treatment take from start to finish?

The entire process takes 4-8 weeks: 1-2 weeks for assessment, 2-4 weeks for cell manufacturing, a few days of lymphodepleting chemotherapy, and 2-4 weeks of inpatient monitoring after infusion. Some trials have "off-the-shelf" (allogeneic) CAR-T that can be given immediately.

What happens if CAR-T doesn't work?

If CAR-T therapy doesn't achieve remission, options include other CAR-T products (targeting different antigens), bispecific antibodies, stem cell transplant, or other clinical trials. Your haematologist will discuss next steps based on your specific situation.

Can CAR-T cure cancer?

CAR-T has produced long-term remissions in some patients with otherwise incurable blood cancers, particularly in ALL and lymphoma. For some patients, these remissions have lasted 5+ years. However, it doesn't work for everyone, and "cure" is a complex term in oncology.

Treatment Guide

CAR-T Cell Therapy Clinical Trials in the UK 2026 — Find Active Studies

26 May 2026 12 min read

80+

UK CAR-T trials

30+

NHS centres

15+

Target conditions

CAR-T cell therapy (Chimeric Antigen Receptor T-cell therapy) represents one of the most exciting advances in modern medicine. By genetically engineering your own immune cells to recognise and destroy cancer, CAR-T has achieved remarkable results in blood cancers that were previously untreatable. The UK is a major hub for CAR-T research, with trials now expanding from blood cancers into solid tumours and autoimmune diseases.

How CAR-T Cell Therapy Works

1. Collection (Leukapheresis)

Your white blood cells are collected via an IV line. This takes 2-4 hours and is similar to donating blood. The T-cells are separated out and the rest of your blood is returned to you.

2. Engineering

Your T-cells are sent to a specialised lab where a viral vector (usually a lentivirus or retrovirus) inserts the chimeric antigen receptor (CAR) gene. This reprogrammes them to target a specific protein on cancer cells. This takes 2-4 weeks.

3. Expansion

The engineered CAR-T cells are multiplied in the lab to reach the therapeutic dose — typically millions to billions of cells. Quality control checks ensure the cells are safe and effective.

4. Infusion

Before receiving your CAR-T cells, you'll typically have a short course of lymphodepleting chemotherapy to make space for the new cells. The CAR-T infusion itself takes just minutes, but you'll be monitored in hospital for 2-4 weeks.

CAR-T Trials by Condition

Acute Lymphoblastic Leukaemia (ALL) — CD19-targeted CAR-T (tisagenlecleucel, brexucabtagene) is approved; trials focus on earlier lines and new constructs
Diffuse Large B-Cell Lymphoma (DLBCL) — Multiple approved CAR-T products; trials testing in 2nd line and combinations
Multiple Myeloma — BCMA-targeted CAR-T (ide-cel, cilta-cel) showing dramatic responses; next-gen dual-target CAR-T in trials
Acute Myeloid Leukaemia (AML) — Early-phase trials targeting CD33, CD123, and other AML antigens
Follicular Lymphoma & Mantle Cell — Expanding CAR-T into indolent lymphomas with promising results
Solid Tumours — Early trials targeting GD2 (neuroblastoma), HER2, mesothelin, and other solid tumour antigens

Eligibility and Assessment

CAR-T trial eligibility is more complex than standard drug trials:

Performance status — You need to be well enough to withstand the treatment process (typically ECOG 0-2)
Organ function — Adequate heart, lung, liver, and kidney function required
Disease-specific criteria — Specific markers like CD19 expression, BCMA expression, or disease refractory status
Prior treatments — Most trials require failure of at least 2 prior lines of therapy
No active infections — Including HIV, hepatitis B/C (some trials allow controlled HIV)
T-cell fitness — Your collected T-cells must be healthy enough to be engineered

Important: CAR-T therapy requires specialised centres with expertise in cell therapy. UK CAR-T centres include The Christie (Manchester), UCLH (London), Birmingham, Glasgow, and others. Your referral pathway may depend on your nearest centre.

Side Effects and Monitoring

Cytokine Release Syndrome (CRS) — The most significant side effect. Fever, low blood pressure, and difficulty breathing occur as CAR-T cells multiply and release inflammatory cytokones. Occurs in 30-90% of patients (most are mild). Treated with tocilizumab.
Immune Effector Cell-Associated Neurotoxicity (ICANS) — Confusion, tremor, or difficulty speaking. Usually resolves within days. Close neurological monitoring is standard.
Long-term B-cell aplasia — CD19-targeted CAR-T destroys normal B-cells too, requiring immunoglobulin replacement therapy.
Infection risk — You'll be immunosuppressed for months. Prophylactic antibiotics and antivirals are standard.

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