EASIX-guided Risk Stratification for Complications and Outcome After CAR T-cell Therapy with Ide-cel in Relapsed/refractory Multiple Myeloma

Overview

Journal J Immunother Cancer

Specialties Allergy & Immunology
Oncology
Pharmacology

Date 2024 Oct 8

PMID 39379098

Authors

Jan H Frenking

Xiang Zhou

Vivien Wagner

Thomas Hielscher

Joseph Kauer

Elias K Mai

Mirco J Friedrich

Christian S Michel

Marina Hajiyianni

Iris Breitkreutz

Patrick Costello

Omar Nadeem

Niels Weinhold

Hartmut Goldschmidt

Anita Schmitt

Thomas Luft

Michael Schmitt

Carsten Muller-Tidow

Max Topp

Hermann Einsele

Peter Dreger

Nikhil C Munshi

Adam S Sperling

Leo Rasche

Sandra Sauer

Marc S Raab

Affiliations

Soon will be listed here.

Abstract

Background: Chimeric antigen receptor (CAR) T-cell therapy has demonstrated significant benefits in the treatment of relapsed/refractory multiple myeloma (RRMM). However, these outcomes can be compromised by severe complications, including cytokine release syndrome, immune effector cell-associated neurotoxicity syndrome (ICANS) and immune effector cell-associated hematotoxicity (ICAHT), predisposing for life-threatening infections.

Methods: This retrospective observational study examined a total of 129 patients with RRMM who had received idecabtagene vicleucel (ide-cel) at two major myeloma centers in Germany and one center in the USA to assess the Endothelial Activation and Stress Index (EASIX) as a risk marker for an unfavorable clinical course and outcome after CAR T-cell therapy. EASIX is calculated by lactate dehydrogenase (U/L) × creatinine (mg/dL) / platelets (10 cells/L) and was determined before lymphodepletion (baseline) and at the day of CAR T-cell infusion (day 0). The analysis was extended to EASIX derivatives and the CAR-HEMATOTOX score.

Results: An elevated baseline EASIX (>median) was identified as a risk marker for severe late ICAHT, manifesting with an impaired hematopoietic reconstitution and pronounced cytopenias during the late post-CAR-T period. Patients with high EASIX levels (>upper quartile) were particularly at risk, as evidenced by an increased rate of an aplastic phenotype of neutrophil recovery, severe late-onset infections and ICANS. Finally, we found associations between baseline EASIX and an inferior progression-free and overall survival. Moreover, the EASIX at day 0 also demonstrated potential to serve as a risk marker for post-CAR-T complications and adverse outcomes.

Conclusions: In conclusion, EASIX aids in risk stratification at clinically relevant time points prior to CAR T-cell therapy with ide-cel. Increased EASIX levels might help clinicians to identify vulnerable patients to adapt peri-CAR-T management at an early stage.

Citing Articles

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