CAR-T Cell Therapy vs Stem Cell Transplant — Clinical Trial Comparison

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CAR-T Cell Therapy

Engineered T-cells targeting specific cancer antigens

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Stem Cell Transplant

Replace diseased bone marrow with healthy stem cells

CAR-T cell therapy and stem cell transplant are two of the most advanced treatments for blood cancers, and both are areas of intense clinical research in the UK. While stem cell transplantation has been a curative approach for decades, CAR-T represents a revolutionary form of personalised immunotherapy. Many patients facing relapsed or refractory blood cancers will encounter both options — understanding the trial landscape can help guide your decisions.

Key Differences at a Glance

FeatureCAR-T Cell TherapyStem Cell Transplant
MechanismPatient's T-cells are genetically engineered to express chimeric antigen receptors (CARs) that recognise cancer cellsHealthy stem cells (from patient or donor) replace diseased bone marrow after high-dose chemotherapy/radiation
Autologous vs allogeneicCurrently only autologous (patient's own T-cells) approved; allogeneic CAR-T in trialsBoth autologous (self) and allogeneic (donor) transplants are standard
Treatment processLeukapheresis → manufacturing (2–4 weeks) → lymphodepletion → CAR-T infusionStem cell harvest → conditioning chemotherapy → stem cell infusion → engraftment
Typical cancers treatedDLBCL, ALL, mantle cell lymphoma, follicular lymphoma, multiple myelomaAML, ALL, lymphoma, myeloma, MDS, CML, aplastic anaemia
Hospital stayUsually 2–4 weeks for monitoring (cytokine release syndrome risk)4–8 weeks for allogeneic; shorter for autologous
Long-term risksB-cell aplasia, hypogammaglobulinaemia, secondary malignancies (rare)Graft-vs-host disease (allogeneic), infections, organ toxicity, secondary malignancies

Clinical Trial Availability

Trial AspectCAR-T Cell TherapyStem Cell Transplant
UK trials actively recruiting30–60 studies50–80 studies
Most common phasesPhase 1–2 (rapidly expanding to Phase 3)Phase 2–3
Top conditions studiedDLBCL, ALL, multiple myeloma, mantle cell lymphoma, follicular lymphomaAML, myelodysplastic syndromes, ALL, lymphoma, myeloma, aplastic anaemia
Novel approaches in trialsDual-target CAR-T, allogeneic "off-the-shelf" CAR-T, CAR-NK, logic-gated CARsHaploidentical transplants, reduced-intensity conditioning, post-transplant maintenance, cord blood
Combination trialsCAR-T + checkpoint inhibitors, CAR-T + bispecific antibodiesTransplant + maintenance therapy, transplant + targeted therapy
Age focusExpanding from paediatric/young adult to older patientsBoth paediatric and adult; age limits vary by protocol

Exciting Emerging Treatments

CAR-T Cell Therapy Trials

Stem Cell Transplant Trials

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Eligibility Differences

CAR-T Cell Therapy Trial Criteria

Stem Cell Transplant Trial Criteria

CAR-T Cell Therapy Trials

Find actively recruiting CAR-T clinical trials across the UK

CAR-T Cell Therapy Trials

Stem Cell Transplant Trials

Find actively recruiting stem cell transplant trials across the UK

Stem Cell Transplant Trials

Frequently Asked Questions

Can I have CAR-T after a stem cell transplant?
Yes — CAR-T is increasingly used as salvage therapy after transplant relapse. In fact, many CAR-T trials specifically enrol patients who have relapsed after autologous or allogeneic stem cell transplant. Your haematologist can advise on sequencing.
Is CAR-T replacing stem cell transplant?
Not entirely. CAR-T is expanding into earlier lines of therapy, but stem cell transplant remains the standard curative approach for many blood cancers, particularly AML and MDS. They are complementary rather than competing approaches, and combination strategies are being actively studied.
Which treatment has a faster recovery?
CAR-T typically has a shorter hospital stay (2–4 weeks) compared to allogeneic transplant (4–8 weeks), but recovery is highly individual. CAR-T recovery focuses on managing cytokine release syndrome and neurological side effects, while transplant recovery centres on engraftment and preventing graft-versus-host disease.

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