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Background: Ide-cel received regulatory approval for the treatment of patients with RRMM after ≥4 prior lines of therapy based on the results of the pivotal KarMMa trial in which patients achieved an overall response rate (ORR) of 73%, ≥ complete response (CR) in 33%, and median progression free survival (PFS) of 8.8 months (Munshi et al. N Engl J Med 2021). Patients who had previously received a BCMA-targeted therapy (BCMA-TT) were excluded from the KarMMa trial. We evaluated the real-world outcomes for patients treated with standard of care ide-cel after having previously received a BCMA-TT. Methods: Eleven US academic centers contributed data to this effort which included patients who had undergone apheresis up until 5/1/2022, and who were infused with ide-cel with sufficient follow-up duration for at least a day 30 response assessment. Patients who died from an infection or ide-cel related toxicity prior to response assessment were included in the safety and survival analyses, but were not considered evaluable for response. Results: A total of 50 patients who had received a prior BCMA-TT and were later infused with ide-cel were evaluable for safety and survival analyses, of which 49 were evaluable for response. The specific type of prior BCMA-TT with respective ORR to the prior BCMA-TT were antibody-drug conjugates (n=38, ORR 17%), bispecifics (n=7, ORR 0%), and CAR T (n=5, ORR 80%). This cohort consisted of 56% patients aged ≥ 65 years, 66% male, and 19% with ECOG performance status ≥ 2. Disease characteristics were notable for 36% with high-risk FISH findings as defined by del(17p), t(4;14), and t(14;16), 50% extramedullary disease, 27% R-ISS stage III disease, and 30% with high bone marrow plasma cell burden (≥50%) prior to ide-cel infusion. Patients were heavily pre-treated with a median of 9 prior lines of therapy, 88% received prior autologous stem cell transplant, 62% were penta-refractory, and 86% required bridging therapy (68% with ≥SD on bridging therapy). Compared to the cohort of patients who had not received a prior BCMA-TT (n=153), patients who received prior BCMA-TT were more likely to have t(4;14) as a high-risk feature (23% v 8%; p=0.005), had a higher median number of prior lines of therapy (9 v 6; p 6 months prior to ide-cel, those with treatment < 6 months prior to ide-cel had lower rates of overall response (60% v 83%; p=0.076), CR (20% v 34.5%; p=0.22), and median PFS (3.0 v 5.3 months; p=0.39), though these differences did not reach statistical significance. Treatment with a prior BCMA-TT was associated with an inferior median PFS compared to those without prior BCMA-TT (3.2 v 9.0 months; log-rank p=0.0002). The 3-month PFS rates amongst those with prior ADC, prior bispecific, prior CAR T, and without prior BCMA-TT were 57.2%, 41.5%, 77.8%, and 85% respectively. On univariate analysis amongst patients treated with a prior BCMA-TT, having penta-refractory disease reached borderline significance for association with response of < PR (p=0.053), and treatment with a prior ADC trended for association with a response of < CR compared to other modalities of BCMA-TT (p=0.076). The toxicity profile for patients receiving a prior BCMA-TT was similar to those in our cohort who had not received a prior BCMA-TT and to that described in KarMMa. Grade ≥ 3 CRS and ICANS were 2.0% and 8.5% respectively. Patients in the prior BCMA-TT cohort were more likely to have grade 4 thrombocytopenia in the first 30 days after ide-cel infusion (46% v 31.5%; p=0.064) and were more likely to receive a thrombopoietin (TPO) agonist (27% v 12%; p=0.017). Conclusions: This multicenter retrospective study characterizes a large cohort of patients who received a prior BCMA-TT before treatment with ide-cel, which is associated with inferior PFS and less likelihood of attaining both an overall response and best response of ≥CR. There was a trend towards worse efficacy outcomes for patients who received ide-cel < 6 months after their prior BCMA-TT, and the timing of ide-cel infusion after prior BCMA-TT warrants further investigation. Figure 1View largeDownload PPTFigure 1View largeDownload PPT Close modal
Ferreri et al. (Tue,) studied this question.