Mantleโ Cell Lymphoma: Progression Risks โAfter CAR T-Cell Therapy Highlighted in New Study
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A recent, extensive analysis of 384 patients with relapsed or refractoryโค mantle cell lymphoma (MCL) indicatesโค thatโ approximately one-third experience disease progression following โtreatment with chimeric antigen receptor (CAR) T-cellโฃ therapy. The โคfindings, published August โ5 in Bloodโ Advances, underscore theโข complexities of managing thisโฃ aggressive blood cancerโ even with cutting-edge immunotherapies.
Understanding mantle Cell Lymphoma and CAR T-Cell โtherapy
Mantle cell lymphoma is a rare โฃand aggressive type of non-Hodgkin lymphoma.โ CAR T-cell therapy represents a significant advancement in cancer treatment, genetically modifying a patient’s ownโข T โขcellsโฃ to recognize and destroy cancer cells.The Food and Drugโ Managementโข has approvedโ two CAR T-cell therapies for MCL: brexucabtagene autoleucelโ (brexu-cel, Tecartus) in 2020, โขand lisocabtagene maraleucel (liso-cel, Breyanzi) in 2024.
Brexu-cel โคisโ indicated for patientsโค after at least โone prior line โof โคtherapy, โคwhile โliso-cel can be used after at โขleast two prior lines, including a Bruton tyrosine kinase (BTK) inhibitor.Despiteโ the promise of these therapies, the new study reveals โฃaโ significant โrisk of disease โขprogression, prompting researchers to investigate contributing โคfactors.
key Findings from the Multicenter Analysis
Researchersโข from leading cancer centers, โincluding โMemorial Sloanโค Kettering Cancer Center, The University ofโฃ Texas MD Anderson โCancer Center, andโข Mayo Clinic, โcollaborated onโ the study. โขTheir analysis โขfocused onโ the 135 patients who โคexperienced disease progression โคafter CAR T-cell therapy, with a median โtimeโ to progression ofโ six months.โ
The patient cohort experiencing progression was predominantly male, with a median age of 67 years. โข Notably, 98% of theseโ patients hadโ previously received โขa BTK inhibitor, with 63% demonstratingโค a response. The median number of prior therapiesโฃ was three.
Did Youโ know?
Mantle cell โlymphoma accounts for โapproximately 6% ofโค all non-Hodgkinโค lymphomas โฃin the โคUnitedโค States, affecting โฃmore men than women.
Patient Characteristics Associated with Progression
Severalโฃ high-risk features wereโฃ common among patients who progressedโ afterโ CAR T-cell therapy.โ These included a TP53 mutation in 68% of cases,a Ki67 proliferation indexโฃ of โatโ least 50% in 69%,central nervous system (CNS) involvement in 16%,and blastoid/pleomorphic MCL inโค 25%. Most patients (73%) โฃreceived bridging therapy, butโข 60% of those assessed were refractory to it.
The majority of patients receivedโฃ brexu-cel (87%) or liso-cel (13%), with most โundergoing lymphodepletion with fludarabine and cyclophosphamide (87%). Following treatment, 64% achieved aโ complete response, โ27% a partial โresponse, and 16% โstable disease.
| Characteristic | Percentage/Median |
|---|---|
| Male Patients | 74% |
| Median Age โฃ(Years) | 67 |
| Prior BTK Inhibitor Use | 98% |
| TP53 Mutation | 68% |
| Ki67 โฅโ 50% | 69% |
Outcomes Following disease Progression
The median time from CAR T-cell infusion to disease progression was six months, with only โค30 โขpatients experiencing progression after moreโข than 12 months. โคAtโ the time of โprogression,high-riskโฃ features persisted in many patients,including blastoid/pleomorphic morphologyโข (37%),a Ki67 of at leastโ 50% (77%),andโ a โค TP53 mutation (51%). CNS involvement was present in 51% of patients with prior CNS disease.
Analysis of CD19 status โคfollowing progression revealed that 10% of patientsโข had become CD19-negative, possibly contributing toโข treatmentโค resistance. Following disease progression, 17 patients โขreceived no further treatment, 13 โฃreceived local therapy, and 105 received systemic therapy.
Pro Tip:
Understanding the specific genetic mutations and characteristics โof a patient’s MCL is crucial for tailoring treatmentโฃ strategiesโ and predicting response โto therapies.
Responseโ rates โฃto โฃsubsequent therapies were as follows:โ chemoimmunotherapyโค (40%), pirtobrutinib (36%), โฃand bispecific antibodies (67%). The median progression-free survival (PFS) and overall survival (OS) for patients experiencing progression โwere 2.5 months and 5.4 months, respectively. โA lack of initial response to CAR T-cell therapy and rapid progression โ(less than threeโ months) were associated โwith inferior OS.
Future Directionsโค and Clinical Implications
“We confirm the challenging prognosis โfor patients experiencing [disease progression] followingโ CD19 CAR-Tโ for R/R MCL and โestablish a benchmark for โคfuture,” the authors concluded. โ These findings highlight โthe need for โimprovedโ strategies to address disease โprogressionโข after โฃCAR T-cell therapy, including novel therapeutic โapproaches and more refined patient selection criteria. What additional therapies might improveโ outcomes for patients whoโ relapse after โคCAR T-cell โtreatment? How can we betterโ identify patients who โare most likely to benefit fromโ this therapy in the first place?
References
- Epstein-Peterson ZD, Lionel AC, Joseph A, et al. โขTreatment and outcomes of progression ofโ disease post-CAR T-cell therapy inโค mantle cell lymphoma: a multicenter analysis. Blood Advances. Publishedโค August 5, 2025.โ doi.org/10.1182/bloodadvances.2025016315
- Stallard J. FDA approves CAR T cell treatment for resistant mantle cell lymphoma. Memorial Sloan Kettering Cancer Center. July 31, 2024.Accessed August โ15, โฃ2025. https://www.mskcc.org/news/fda-approves-car-t-cell-treatment-for-resistant-mantle-cell-lymphoma
Mantle cell lymphoma research is rapidly evolving, withโ ongoing clinical trials exploring novel combinations โofโ therapies and strategies to overcome treatment resistance. The development of bispecific antibodies and improved CAR โฃT-cell designs โrepresentโ promising avenues for enhancing outcomes โฃin this challenging disease. Long-term follow-up of patientsโค receiving CAR T-cell therapy is crucial to fully โunderstand theโ durability of responses and identify factors associated withโ late relapses.
Frequently Asked Questionsโ About Mantle Cell Lymphoma and CAR T-Cell Therapy
- What is mantle cell lymphoma? Mantle cellโฃ lymphoma is an aggressive type of non-Hodgkin lymphoma that develops in the mantle zone of lymph nodes.
- What is CAR T-cell therapy? CAR T-cellโ therapy is a personalized โขcancer treatment thatโ uses โฃa patient’s ownโ immune cells to fight cancer.
- What areโฃ the common side effects of CAR T-cellโค therapy? Common side effects include cytokine releaseโ syndrome and neurotoxicity.
- What is โthe prognosis for patients with relapsed or refractoryโ mantle cell lymphoma? โค The prognosis โvaries depending onโข individual โfactors,but it is generally considered poor.
- What areโค the current treatment options for mantleโฃ cellโ lymphoma? Treatment options include chemotherapy, radiation therapy, stem cell transplant,โ and CAR T-cellโ therapy.
Disclaimer: This article โขprovides general information and shouldโ not be considered medical advice. Pleaseโ consult โwith a qualifiedโ healthcare professional for anyโฃ health concerns or before making any decisions related to your health or treatment.
We hope โคthis article provided valuableโ insights into the โlatest research on mantle cell lymphoma and CAR T-cell therapy.โค If you found thisโฃ information helpful, please share it withโ yourโค network, leave a comment below, or subscribe to our newsletter for more updates on cutting-edgeโ medical advancements.
