| Literature DB >> 36097223 |
Zinaida Good1,2,3, Jay Y Spiegel1,4,5, Bita Sahaf1, Meena B Malipatlolla1, Zach J Ehlinger1, Sreevidya Kurra1,6, Moksha H Desai1, Warren D Reynolds1, Anita Wong Lin1,7, Panayiotis Vandris1, Fang Wu1, Snehit Prabhu1, Mark P Hamilton1,4, John S Tamaresis2, Paul J Hanson1,4, Shabnum Patel1,8,9, Steven A Feldman1,8, Matthew J Frank1,4, John H Baird1,4,10, Lori Muffly1,4, Gursharan K Claire1,4, Juliana Craig1,4,11, Katherine A Kong1, Dhananjay Wagh12, John Coller12, Sean C Bendall1,3,13, Robert J Tibshirani2,14, Sylvia K Plevritis2,15, David B Miklos16,17, Crystal L Mackall18,19,20,21.
Abstract
Approximately 60% of patients with large B cell lymphoma treated with chimeric antigen receptor (CAR) T cell therapies targeting CD19 experience disease progression, and neurotoxicity remains a challenge. Biomarkers associated with resistance and toxicity are limited. In this study, single-cell proteomic profiling of circulating CAR T cells in 32 patients treated with CD19-CAR identified that CD4+Helios+ CAR T cells on day 7 after infusion are associated with progressive disease and less severe neurotoxicity. Deep profiling demonstrated that this population is non-clonal and manifests hallmark features of T regulatory (TReg) cells. Validation cohort analysis upheld the link between higher CAR TReg cells with clinical progression and less severe neurotoxicity. A model combining expansion of this subset with lactate dehydrogenase levels, as a surrogate for tumor burden, was superior for predicting durable clinical response compared to models relying on each feature alone. These data credential CAR TReg cell expansion as a novel biomarker of response and toxicity after CAR T cell therapy and raise the prospect that this subset may regulate CAR T cell responses in humans.Entities:
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Year: 2022 PMID: 36097223 DOI: 10.1038/s41591-022-01960-7
Source DB: PubMed Journal: Nat Med ISSN: 1078-8956 Impact factor: 87.241