260 Investigating cancer cell autonomous CAR T cell therapy resistance in DLBCL in vitro [Abstract]

  • Background CD19 CAR T cell therapy has greatly improved the outcome of r/r DLBCL patients, but durable responses are achieved in only 40% of cases. Relapses can be due to declining T cell fitness and/or cancer cells becoming inherently refractory. However, besides antigen loss, cancer cell autonomous resistance mechanisms are poorly understood. Methods We generated DLBCL cell lines that are refractory to CD19 targeting CAR T cells by longterm co-culture in vitro. We assessed response to alternative CAR T cells targeting other antigens and performed RNAseq of resistant cancer cell lines to identify yet unknown resistance mechanisms. Results Our in vitro longterm co-cultures recapitulate common resistance mechanisms observed in the clinics including CD19 loss. Interestingly, we do observe CD19 positive resistance and multiple of our CD19 CAR T cell resistant cell lines had become less sensitive also to alternative CAR T cells. Moreover, our RNAseq data indicate that theBackground CD19 CAR T cell therapy has greatly improved the outcome of r/r DLBCL patients, but durable responses are achieved in only 40% of cases. Relapses can be due to declining T cell fitness and/or cancer cells becoming inherently refractory. However, besides antigen loss, cancer cell autonomous resistance mechanisms are poorly understood. Methods We generated DLBCL cell lines that are refractory to CD19 targeting CAR T cells by longterm co-culture in vitro. We assessed response to alternative CAR T cells targeting other antigens and performed RNAseq of resistant cancer cell lines to identify yet unknown resistance mechanisms. Results Our in vitro longterm co-cultures recapitulate common resistance mechanisms observed in the clinics including CD19 loss. Interestingly, we do observe CD19 positive resistance and multiple of our CD19 CAR T cell resistant cell lines had become less sensitive also to alternative CAR T cells. Moreover, our RNAseq data indicate that the majority of transcriptional changes are associated with a common resistant phenotype rather than a specific resistance mechanism (e.g., antigen loss). Conclusions Our results suggest that besides CD19 loss, DLBCL cells evolve mechanisms to overcome T cell killing which may render them cross-resistant to CAR T cells targeting other antigens. Analysis of our RNAseq data will allow us to characterize these mechanisms.show moreshow less

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Metadaten
Author:Fabiana Lueoend, Youngchul Song, Beverly Nguyen, Xiaoyan Li, Andreas RaueORCiDGND, Jennifer Brogdon, Glenn Dranoff, Matthew Niederst, Louise Treanor
Frontdoor URLhttps://opus.bibliothek.uni-augsburg.de/opus4/112737
ISSN:2051-1426OPAC
Parent Title (English):Journal for ImmunoTherapy of Cancer
Publisher:BioMed Central
Place of publication:London
Type:Article
Language:English
Year of first Publication:2022
Release Date:2024/04/29
Volume:10
Issue:Suppl. 2
First Page:A275
DOI:https://doi.org/10.1136/jitc-2022-sitc2022.0260
Institutes:Fakultät für Angewandte Informatik
Fakultät für Angewandte Informatik / Institut für Informatik
Fakultät für Angewandte Informatik / Institut für Informatik / Lehrstuhl für Modellierung und Simulation biologischer Prozesse
Dewey Decimal Classification:6 Technik, Medizin, angewandte Wissenschaften / 61 Medizin und Gesundheit / 610 Medizin und Gesundheit

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