Migrating into the tumor: a roadmap for T cells

LL van der Woude, MAJ Gorris, A Halilovic, CG Figdor… - Trends in cancer, 2017 - cell.com
LL van der Woude, MAJ Gorris, A Halilovic, CG Figdor, IJM de Vries
Trends in cancer, 2017cell.com
Tumors can be divided into 'hot'(T cell inflamed) or 'cold'(T cell noninflamed) according to the
presence of immune cells. In this review, we discuss variables that influence T cell migration
into the tumor microenvironment. Chemokines can attract T cells to the tumor site and tumor
intrinsic pathways can influence the composition of local chemokines. Tumor-induced
vasculature can hamper T cell migration. Other immune cells and tumor-derived molecules
can block T cell proliferation and survival. It is important to better understand these …
Tumors can be divided into ‘hot' (T cell inflamed) or ‘cold' (T cell noninflamed) according to the presence of immune cells. In this review, we discuss variables that influence T cell migration into the tumor microenvironment. Chemokines can attract T cells to the tumor site and tumor intrinsic pathways can influence the composition of local chemokines. Tumor-induced vasculature can hamper T cell migration. Other immune cells and tumor-derived molecules can block T cell proliferation and survival. It is important to better understand these mechanisms in order to target them therapeutically. Enhancing T cell infiltration may increase response rates to immunotherapy and increase survival.
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