7058 Background: cBTKis have become standard therapy for relapsed/refractory MCL and are rapidly advancing to the first-line setting. However, real-world evidence on clinical and economic outcomes following cBTKi therapy is limited. Treatment patterns, time to treatment discontinuation (TTD), and HCRU were evaluated among patients (pts) with MCL previously treated with cBTKis. Methods: This retrospective observational study used claims data from the Symphony Integrated Dataverse (Jan 2020-Aug 2025) to identify adults with MCL who received a cBTKi in any line of therapy (LOT) and, following discontinuation, initiated another treatment. Post-cBTKi regimens were categorized as B-cell lymphoma 2 inhibitor (BCL2i), cBTKi, noncovalent BTKi (ncBTKi), chimeric antigen receptor T-cell therapy (CAR-T), chemo±immunotherapy (C±IT), and other. TTD and HCRU (outpatient/inpatient/other medical, reported per-patient-per-month PPPM), were assessed for regimens received post cBTKi. Results: Of 10,519 total US pts with MCL, 571 were previously treated with cBTKis and received a subsequent therapy (median age, 72.0 years; ≥65 years, 77%; male, 74%; White non-Hispanic, 67%; Medicare, 62%). Regimens received in a subsequent LOT after cBTKi included cBTKis (38%), ncBTKis (32%), C±IT (11%), BCL2is (9%; monotherapy 7%), CAR-T (2%), and other (8%). Median TTD was longest with cBTKis (365 days), followed by ncBTKis (206 days), and shortest with BCL2is (140 days). Mean HCRU PPPM was lowest with cBTKis (outpatient, 1.21; inpatient, 0.20; other medical, 1.07) and highest with CAR-T (outpatient, 10.63; inpatient, 1.89; other medical, 1.55). Conclusions: In this real-world analysis, pts with MCL who previously received cBTKis were most frequently re-treated with cBTKis, highlighting the need for novel treatment options in the post-cBTKi setting. TTD was greatest in pts who received cBTKis or ncBTKis and shortest in those treated with BCL2is. HCRU burden was lowest for pts who received cBTKis and highest for those treated with CAR-T. Further research, including an understanding of the reasons for re-exposure to cBTKis, is warranted to confirm these findings. TTD and HCRU by MCL treatment regimens received post cBTKi. Outcomes AllN=571 cBTKin=215 ncBTKin=182 C±ITn=62 BCL2in=53 CAR-Tn=12 Follow-up, median (IQR), days 294(118-628) 414(206-762) 189(89-453) 330(116-727) 256(70-844) 412(216-912) TTD, median (95% CI), days 222(181-281) 365(278-460) 206(173-304) 169(112-183) 140(100-315) NA HCRU, mean (SD), PPPM Outpatient 1.95 (2.82) 1.21 (1.61) 1.48 (2.19) 2.19 (2.65) 2.34 (2.70) 10.63 (5.05) Inpatient 0.34 (0.91) 0.20 (0.67) 0.33 (0.75) 0.29 (0.82) 0.43 (1.22) 1.89 (1.89) Other medical services 1.47 (2.62) 1.07 (1.93) 1.35 (2.54) 2.54 (3.59) 1.64 (2.82) 1.55 (1.70)
Alencar et al. (Wed,) studied this question.