Legend Biotech Unveils Promising Clinical Data for LB2501 CAR‑T Therapy in B-Cell Non‑Hodgkin Lymphoma

June 14, 2026
Legend Biotech Unveils Promising Clinical Data for LB2501 CAR‑T Therapy in B-Cell Non‑Hodgkin Lymphoma
  • Legend Biotech reports first clinical proof‑of‑concept data for LB2501, an in vivo CD19/CD20 dual‑targeting CAR‑T, in relapsed/refractory B‑cell non‑Hodgkin lymphoma, presented in a late‑breaking session at EHA 2026.

  • The late‑breaking EHA 2026 presentation (Abstract LB5006) underscores Legend Biotech’s leadership in next‑generation cell therapies beyond CARVYKTI.

  • In the Phase 1 dose‑escalation, a single LB2501 infusion at the higher DL2 achieved a 100% objective response rate (6/6) and 83.3% complete responses (5/6), with all responses ongoing at data cutoff.

  • LB2501 showed dose‑dependent in vivo CAR‑T expansion without lymphodepletion, and safety was favorable with no dose‑limiting toxicities, serious adverse events, ICANS, or deaths; any infusion reactions and CRS were Grade 1–2 and did not require steroids.

  • Translational analyses demonstrated polyclonal, diverse vector integrations and no evidence of non‑specific transduction in off‑target populations, supporting feasibility of in vivo T‑cell engineering.

  • A senior researcher emphasized in vivo CAR‑T as a frontier in cell therapy, with LB2501 potentially simplifying treatment and expanding access, building on CARVYKTI’s foundation.

  • Pharmacokinetics showed detectable CAR‑T cells for up to about four months, with 100% expansion at DL2 and 83% at DL1; vector clearance was rapid, with viral copies peaking immediately after infusion and becoming undetectable within 24 hours.

  • The study enrolled 12 patients across two dose levels (6 per level), with a median of three prior therapies and 58.3% refractory to the most recent treatment, aiming to assess safety, determine a recommended Phase 2 dose, pharmacokinetics, and preliminary efficacy in adults with R/R B‑NHL.

  • Across both dose levels, the overall ORR was 50% and the CR rate was 41.7%, with all DL2 responses ongoing at data cutoff and including DLBCL, MCL, and FL patients.

  • Additional translational data highlighted rapid vector clearance and non‑specific transduction absence, reinforcing the feasibility of in vivo CAR‑T strategies.

Summary based on 2 sources


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