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KMID : 0923620200200010005
Immune Network
2020 Volume.20 No. 1 p.5 ~ p.5
Heterogeneity of Human ¥ã¥ä T Cells and Their Role in Cancer Immunity
Lee Hye-Won

Chung Yun-Shin
Kim Tae-Jin
Abstract
The ¥ã¥ä T cells are unconventional lymphocytes that function in both innate and adaptive immune responses against various intracellular and infectious stresses. The ¥ã¥ä T cells can be exploited as cancer-killing effector cells since ¥ã¥ä TCRs recognize MHC-like molecules and growth factor receptors that are upregulated in cancer cells, and ¥ã¥ä T cells can differentiate into cytotoxic effector cells. However, ¥ã¥ä T cells may also promote tumor progression by secreting IL-17 or other cytokines. Therefore, it is essential to understand how the differentiation and homeostasis of ¥ã¥ä T cells are regulated and whether distinct ¥ã¥ä T cell subsets have different functions. Human ¥ã¥ä T cells are classified into V¥ä2 and non-V¥ä2 ¥ã¥ä T cells. The majority of V¥ä2 ¥ã¥ä T cells are V¥ã9¥ä2 T cells that recognize pyrophosphorylated isoprenoids generated by the dysregulated mevalonate pathway. In contrast, V¥ä1 T cells expand from initially diverse TCR repertoire in patients with infectious diseases and cancers. The ligands of V¥ä1 T cells are diverse and include the growth factor receptors such as endothelial protein C receptor. Both V¥ä1 and V¥ä2 ¥ã¥ä T cells are implicated to have immunotherapeutic potentials for cancers, but the detailed elucidation of the distinct characteristics of 2 populations will be required to enhance the immunotherapeutic potential of ¥ã¥ä T cells. Here, we summarize recent progress regarding cancer immunology of human ¥ã¥ä T cells, including their development, heterogeneity, and plasticity, the putative mechanisms underlying ligand recognition and activation, and their dual effects on tumor progression in the tumor microenvironment.
KEYWORD
T-lymphocyte subsets, ¥ã¥ä T cell, T Cell Receptors, gamma delta, Tumor microenvironment
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