Single-Cell Multi-Tissue T Cell Clonal Dynamics Reveal Distinct Immune Coercion Landscapes in MSI and MSS Colorectal Cancer
Qianhe Zhan, Siwen Zhang, Bofu Cao, Lanming Chen, Lu Xie

TL;DR
This study uses single-cell sequencing to uncover how T cell clonality differs between MSI and MSS colorectal cancer, revealing distinct immune dynamics that affect immunotherapy response.
Contribution
The study introduces a TCR reconstruction pipeline and identifies two distinct immune coercion patterns in MSI and MSS tumors.
Findings
MSI tumors show a 'high-fluctuation, deep-exhaustion' T cell clonal pattern.
MSS tumors exhibit a 'high-baseline, strong-suppression' immune coercion mode.
T cell clonal dynamics, not just MSI status, influence immunotherapy response.
Abstract
The efficacy of immunotherapy in colorectal cancer (CRC) has long been considered to be closely associated with microsatellite instability (MSI) status. Patients with microsatellite stable (MSS) tumors typically exhibit poor responses to PD-1/PD-L1 inhibitors and a poor prognosis, often being categorized as immunologically ‘cold’ tumors. However, some MSS patients can still achieve favorable therapeutic responses, sometimes even surpassing those of certain MSI patients. Immune-cold and immune-hot tumor phenotypes are largely determined by the abundance, clonal expansion, and functional states of tumor-infiltrating T cells. This suggests that immunotherapy responses are driven by dynamic remodeling of T-cell clonality rather than by MSI status alone. To elucidate the underlying T cell clonal dynamics, integrated single-cell transcriptome (scRNA-seq) and T cell receptor sequencing…
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Taxonomy
TopicsCancer Immunotherapy and Biomarkers · Single-cell and spatial transcriptomics · CAR-T cell therapy research
