1. Rigorous benchmarking of T-cell receptor repertoire profiling methods for cancer RNA sequencing.
- Author
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Peng, Kerui, Nowicki, Theodore S, Campbell, Katie, Vahed, Mohammad, Peng, Dandan, Meng, Yiting, Nagareddy, Anish, Huang, Yu-Ning, Karlsberg, Aaron, Miller, Zachary, Brito, Jaqueline, Nadel, Brian, Pak, Victoria M, Abedalthagafi, Malak S, Burkhardt, Amanda M, Alachkar, Houda, Ribas, Antoni, and Mangul, Serghei
- Subjects
RNA sequencing ,T cells ,TUMOR antigens ,T cell receptors ,EARLY detection of cancer ,CANCER research - Abstract
The ability to identify and track T-cell receptor (TCR) sequences from patient samples is becoming central to the field of cancer research and immunotherapy. Tracking genetically engineered T cells expressing TCRs that target specific tumor antigens is important to determine the persistence of these cells and quantify tumor responses. The available high-throughput method to profile TCR repertoires is generally referred to as TCR sequencing (TCR-Seq). However, the available TCR-Seq data are limited compared with RNA sequencing (RNA-Seq). In this paper, we have benchmarked the ability of RNA-Seq-based methods to profile TCR repertoires by examining 19 bulk RNA-Seq samples across 4 cancer cohorts including both T-cell-rich and T-cell-poor tissue types. We have performed a comprehensive evaluation of the existing RNA-Seq-based repertoire profiling methods using targeted TCR-Seq as the gold standard. We also highlighted scenarios under which the RNA-Seq approach is suitable and can provide comparable accuracy to the TCR-Seq approach. Our results show that RNA-Seq-based methods are able to effectively capture the clonotypes and estimate the diversity of TCR repertoires, as well as provide relative frequencies of clonotypes in T-cell-rich tissues and low-diversity repertoires. However, RNA-Seq-based TCR profiling methods have limited power in T-cell-poor tissues, especially in highly diverse repertoires of T-cell-poor tissues. The results of our benchmarking provide an additional appealing argument to incorporate RNA-Seq into the immune repertoire screening of cancer patients as it offers broader knowledge into the transcriptomic changes that exceed the limited information provided by TCR-Seq. [ABSTRACT FROM AUTHOR]
- Published
- 2023
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