When Can We Define Cure after CAR-T Therapy in LBCL? Insights from Serial Landmark Analyses

Background: While response rates to CD19-targeted CAR T cell therapies in large B cell lymphoma (LBCL) are high, up to 60% of patients ultimately relapse or progress. Consequently, determining the optimal time point to define a cure following CAR-T therapy remains challenging. To address this, we pe...

Full description

Saved in:
Bibliographic Details
Published in:Blood 2024-11, Vol.144, p.2369-2369
Main Authors: Gomez-Llobell, Marina, Shouval, Roni, Brown, Samantha, Golan Accav, Noa, Devlin, Sean M., Corona, Magdalena, Rejeski, Kai, Rivas-Delgado, Alfredo, Luna, Alejandro, Luttwak, Efrat, Raj, Sandeep S., Alhomoud, Mohammad, Marcus, Ronit, Shimoni, Avichai, Ringelstein-Harlev, Shimrit, Boardman, Alexander P., Dahi, Parastoo B, Lin, Richard J., Scordo, Michael, Falchi, Lorenzo, Shah, Gunjan L., Palomba, Maria Lia, Salles, Gilles, Park, Jae H., Beyar-Katz, Ofrat, Avigdor, Abraham, Perales, Miguel Angel
Format: Article
Language:English
Online Access:Get full text
Tags: Add Tag
No Tags, Be the first to tag this record!
Description
Summary:Background: While response rates to CD19-targeted CAR T cell therapies in large B cell lymphoma (LBCL) are high, up to 60% of patients ultimately relapse or progress. Consequently, determining the optimal time point to define a cure following CAR-T therapy remains challenging. To address this, we performed serial evaluations of the risk of relapse after CAR-T, contingent on patients remaining disease-free at specific time points. Methods: This retrospective multicenter study includes patients with LBCL treated with commercially available CD19 CAR-T products between April 2018 and June 2023. Primary endpoints were progression-free survival (PFS) and overall survival (OS) measured in patients who maintained a response from various landmarks after CAR-T infusion (Day 28, 3, 6, 12, 18, and 24 months). Response rate transitions were visualized using Sankey diagrams. Cox regression models were adjusted for age, NHL transformation, elevated vs. normal LDH, response at corresponding landmark time, CAR-T product, and bridging therapy to determine associations with PFS. Results: We included 477 patients treated with Axi-cel (n=260, 55%), Tisa-cel (n=130, 27%), and Liso-cel (n=87, 18%). Patients were heavily pre-treated, with 79% having received >3 lines of therapy. Overall response rate (ORR) at Day 28 was 78%, with 50% achieving complete response (CR) and 28% partial response (PR). With a median follow-up of 18 months for Axi-cel, 34 months for Tisa-cel, and 12 months for Liso-cel, median PFS was 12 months for Axi-cel, 3.2 months for Tisa-cel, and not reached for Liso-cel. Among patients in CR on day 28 (n=195), 1 and 2-year PFS from day 28 landmark was 64% and 53%, corresponding OS probability was 90% and 74%. Patients with a PR on day 28 (n=194) had lower PFS (1-year: 43%, 2-year: 40%) and OS (1-year 65%, 2-year 50%). Probabilities of 1 and 2-year PFS also varied by product in patients achieving response: Axi-cel (58%/52%), Tisa-cel (46%/35%), and Liso-cel (62%/57%). For patients in CR at 3 months (n=173), PFS from the 3-month landmark was 76% at one year and 66% at two years, while the corresponding OS probability was 92% and 81%. By product, PFS probabilities at one year and two years were, respectively, Axi-cel (83% /74%), Tisa-cel (66% /46%), and Liso-cel (75%/69%). For patients in CR at 6 months (n=148), the PFS from the 6-month landmark was 77% at one year and 64% at two years, while the corresponding OS probability was 89% and 81%. By product, PFS probabil
ISSN:0006-4971
DOI:10.1182/blood-2024-201029