A Comprehensive Analysis of Adverse Events in the First 30 days of Phase 1 Pediatric CAR T-cell Trials

Overview

Journal Blood Adv

Specialty Hematology

Date 2023 Jul 24

PMID 37486616

Authors

Sara K Silbert

Sanna Madan

Elizabeth M Holland

Seth M Steinberg

Lauren Little

Toni Foley

Monica Epstein

Angela Sarkisian

Daniel W Lee

Ekaterina Nikitina

Showri Kakumanu

Eytan Ruppin

Haneen Shalabi

Bonnie Yates

Nirali N Shah

Affiliations

Soon will be listed here.

Abstract

The tremendous success of chimeric antigen receptor (CAR) T cells in children and young adults (CAYAs) with relapsed/refractory B-cell acute lymphoblastic leukemia is tempered by toxicities such as cytokine release syndrome (CRS). Despite expansive information about CRS, profiling of specific end-organ toxicities secondary to CAR T-cell therapy in CAYAs is limited. This retrospective, single-center study sought to characterize end-organ specific adverse events (AEs) experienced by CAYAs during the first 30 days after CAR T-cell infusion. AEs graded using Common Terminology Criteria for Adverse Events were retrospectively analyzed for 134 patients enrolled in 1 of 3 phase 1 CAR T-cell trials (NCT01593696, NCT02315612, and NCT03448393), targeting CD19 and/or CD22. A total of 133 patients (99.3%) experienced at least 1 grade ≥3 (≥Gr3) AE across 17 organ systems, of which 75 (4.4%) were considered dose- or treatment-limiting toxicities. Excluding cytopenias, 109 patients (81.3%) experienced a median of 3 ≥Gr3 noncytopenia (NC) AEs. The incidence of ≥Gr3 NC AEs was associated with the development and severity of CRS as well as preinfusion disease burden (≥ 25% marrow blasts). Although those with complete remission trended toward experiencing more ≥Gr3 NC AEs than nonresponders (median, 4 vs 3), nonresponders experiencing CRS (n = 17; 37.8%) had the highest degree of NC AEs across all patients (median, 7 vs 4 in responders experiencing CRS). Greater understanding of these toxicities and the ability to predict which patients may experience more toxicities is critical as the array of CAR T-cell therapies expand. This retrospective study was registered at www.clinicaltrials.gov as NCT03827343.

Citing Articles

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PMID: 39674824 PMC: 11646216. DOI: 10.1007/s10555-024-10227-1.

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