Abstract 802MO
Background
The therapeutic landscape for multiple myeloma (MM) has expanded in the last few decades. For relapsed/refractory MM, teclistamab and two CAR-T therapies, idecabtagene vicleucel (ide-cel) and ciltacabtagene autoleucel (cilta-cel), are approved by the FDA after four or more lines of therapy. There is limited data comparing B-cell maturation antigen (BCMA) CAR-T and bispecifics. We report the largest real-world comparison of survival outcomes in patients who received teclistamab versus cilta-cel or ide-cel.
Methods
We used the TriNetX Global Collaborative Network, a de-identified real-world database, to study patients with multiple myeloma who received CAR-T or teclistamab from 2021 to 2023. Cohort 1 received CAR-T without teclistamab, while Cohort 2 received teclistamab without CAR-T. After matching the cohorts, we calculated hazard ratios for 2-year overall survival (OS), CRS, and ICANS and conducted subgroup analyses.
Results
391 CAR-T patients (ide-cel: 277, cilta-cel: 114) and 458 teclistamab patients were included (mean age 66, 54% male). CAR-T showed better OS compared to teclistamab, especially for the cilta-cel group. More CRS was reported with CAR-T, but the incidence of ICANS was similar in both groups. In subgroup analyses, older (age ≥ 70) (OS: HR 0.197, 95% CI: 0.066-0.587; CRS: HR 1.631 95% CI: 1.003-2.651) and those who did not undergo bone marrow transplantation (OS: HR 0.302, 95% CI: 0.163-0.559) especially benefited. Table: 802MO
| Outcomes | CAR-T (Ide-cel + Cilta-cel) | Teclistamab | HR (95% CI) | ||
| Patients at risk | Cases | Patients at risk | Cases | ||
| All-cause mortality | 270 | 30 | 270 | 54 | 0.409 (0.259-0.645) |
| CRS | 270 | 102 | 270 | 74 | 1.394 (1.032-1.883) |
| ICANS | 270 | 40 | 270 | 37 | 1.007 (0.642-1.581) |
| Ide-cel | Teclistamab | HR (95% CI) | |||
| All-cause mortality | 214 | 23 | 214 | 48 | 0.329 (0.197-0.550) |
| CRS | 214 | 74 | 214 | 59 | 1.204 (0.853-1.701) |
| ICANS | 214 | 24 | 214 | 27 | 0.758 (0.432-1.330) |
| Cilta-cel | Teclistamab | HR (95% CI) | |||
| All-cause mortality | 100 | 4 | 100 | 19 | 0.157 (0.053-0.464) |
| CRS | 100 | 42 | 100 | 26 | 1.618 (0.991-2.643) |
| ICANS | 100 | 21 | 100 | 9 | 2.109 (0.993-4.478) |
CRS, cytokine release syndrome; ICANS, immune effector cell-associated neurotoxicity syndrome; HR, hazard ratio; CI, confidence interval
Conclusions
This is the first report comparing survival in a real-world setting between BCMA CAR-Ts and bispecifics. We found that CAR-T improved survival over patients receiving only bispecifics. Older patients and those who did not receive transplants particularly had better OS with CAR-T. Based on our study, we hypothesize that upfront BCMA CAR-T therapy in older transplant-ineligible individuals can improve survival over BCMA bispecifics like teclistamab. Hence, these patients should be especially considered for early BCMA CAR-T.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
Has not received any funding.
Disclosure
All authors have declared no conflicts of interest.
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