KYMRIAH (tisagenlecleucel), anti-CD19 CAR T
Reason for request
High clinical benefit in the third-line or later treatment of refractory or recurrent diffuse large B-cell lymphoma and minor clinical added value in terms of efficacy compared to current management.
- KYMRIAH has been granted a marketing authorisation for the third-line or later treatment of refractory or recurrent diffuse large B-cell lymphoma (DLBCL).
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CAR T cells are a gene therapy consisting of autologous T lymphocytes harvested by leukapheresis, then genetically modified ex vivo to express a chimeric receptor antigen targeting protein CD19 found on the B cell line. The re-injected anti-CD19 CAR T cells then multiply and activate in vivo after binding to target cells expressing CD19, thus inducing their apoptosis.
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Precise quantification of the clinical effect was difficult, failing any comparative studies with usual management, even though direct comparison was possible.
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In intention-to-treat (ITT) population, the data showed a complete response rate of circa 24.2%, along with an estimated 12-month survival rate of approximately 40%, with a median follow-up period limited to 7 months and adverse events of grade ≥3 in 90% of cases, occasionally requiring hospitalisation in intensive care.
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Further data are awaited, considering the uncertainties concerning the efficacy, tolerance and complexity of the treatment process.
- The use of anti-CD19 CAR T is limited to a small number of specifically qualified centres.
Clinical Benefit
Substantial |
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Clinical Added Value
minor |
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