The influence of chimeric antigen receptor structural domains on clinical outcomes and associated toxicities
Details
Publication Year 2020-12-25,Volume 13,Issue #1,Page 38
Journal Title
Cancers
Abstract
Chimeric antigen receptor (CAR)-T cell therapy has transformed the treatment of B cell malignancies, improving patient survival and long-term remission. Nonetheless, over 50% of patients experience severe treatment-related toxicities including cytokine release syndrome (CRS) and neurotoxicity. Differences in severity of toxic side-effects among anti-CD19 CARs suggest that the choice of costimulatory domain makes a significant contribution to toxicity, but comparisons are complicated by additional differences in the hinge and transmembrane (TM) domains of the most commonly used CARs in the clinic, segments that have long been considered to perform purely structural roles. In this perspective, we examine clinical and preclinical data for anti-CD19 CARs with identical antigen-binding (FMC63) and signalling (CD3ζ) domains to unravel the contributions of different hinge-TM and costimulatory domains. Analysis of clinical trials highlights an association of the CD28 hinge-TM with higher incidence of CRS and neurotoxicity than the corresponding sequences from CD8, regardless of whether the CD28 or the 4-1BB costimulatory domain is used. The few preclinical studies that have systematically varied these domains similarly support a strong and independent role for the CD28 hinge-TM sequence in high cytokine production. These observations highlight the value that a comprehensive and systematic interrogation of each of these structural domains could provide toward developing fundamental principles for rational design of safer CAR-T cell therapies.
Publisher
MDPI
Keywords
CAR-T cell therapy; Cd19; Crs; clinical trials; toxicity; modifications.
Research Division(s)
Structural Biology
PubMed ID
33375550
Open Access at Publisher's Site
https://doi.org/10.3390/cancers13010038
Terms of Use/Rights Notice
Refer to copyright notice on published article.


Creation Date: 2021-03-03 09:20:34
Last Modified: 2021-03-03 09:23:29
An error has occurred. This application may no longer respond until reloaded. Reload 🗙