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Idecabtagene Vicleucel (Ide-cel) Chimeric Antigen Receptor (CAR) T-Cell Therapy in Patients with Relapsed/Refractory Multiple Myeloma (RRMM) Who Have Received a Prior BCMA-Targeted Therapy: Real World, Multi-Institutional Experience

Christopher J. Ferreri, Michelle A.T. Hildebrandt, Hamza Hashmi, Leyla Shune, Joseph P. McGuirk, Douglas W. Sborov, Charlotte B Wagner, Mehmet H. Kocoglu, Shebli Atrash, Peter M. Voorhees, Jack Khouri, Danai Dima, Aimaz Afrough, Aishwarya Sannareddy, Gary Simmons, James A. Davis, Nilesh Kalariya, Lauren C. Peres, Melissa Alsina, Frederick L. Locke, Surbhi Sidana, Doris K. Hansen, Krina K. Patel, Omar Castañeda Puglianini

2022Blood18 citationsDOI

Abstract

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<0.0001), and were more likely to have penta-refractory disease (62% v 37%; p=0.002). Response outcomes stratified by the specific type of prior BCMA-TT and by timing of prior BCMA-TT are summarized in Table 1. Patients receiving prior BCMA-TT had a lower ORR (74% v 88%; p=0.021) and lower best response of ≥ CR (29% v 48%; p=0.018) compared to those without prior BCMA-TT. Compared to patients who were treated with a BCMA-TT > 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

Topics & Concepts

MedicineChimeric antigen receptorMultiple myelomaOncologyRefractory (planetary science)Internal medicineCancer researchImmunotherapyCancerBiologyAstrobiologyCAR-T cell therapy researchMultiple Myeloma Research and Treatments