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  • Resident memory T cells in tumor-distant tissues fortify against metastasis formation.

Resident memory T cells in tumor-distant tissues fortify against metastasis formation.

Cell reports (2021-05-13)
Laura S Christian, Liuyang Wang, Bryan Lim, Dachuan Deng, Haiyang Wu, Xiao-Fan Wang, Qi-Jing Li
ABSTRACT

As a critical machinery for rapid pathogen removal, resident memory T cells (TRMs) are locally generated after the initial encounter. However, their development accompanying tumorigenesis remains elusive. Using a murine breast cancer model, we show that TRMs develop in the tumor, the contralateral mammary mucosa, and the pre-metastatic lung. Single-cell RNA sequencing of TRMs reveals two phenotypically distinct populations representing their active versus quiescent phases. These TRMs in different tissue compartments share the same TCR clonotypes and transcriptomes with a subset of intratumoral effector/effector memory T cells (TEff/EMs), indicating their developmental ontogeny. Furthermore, CXCL16 is highly produced by tumor cells and CXCR6- TEff/EMs are the major subset preferentially egressing the tumor to form distant TRMs. Functionally, releasing CXCR6 retention in the primary tumor amplifies tumor-derived TRMs in the lung and leads to superior protection against metastases. This immunologic fortification suggests a potential strategy to prevent metastasis in clinical oncology.

MATERIALS
Product Number
Brand
Product Description

Sigma-Aldrich
GI254023X, ≥98% (HPLC)
Sigma-Aldrich
TRI Reagent®, for DNA, RNA and protein isolation
Sigma-Aldrich
Bouin′s solution, histological fixative