Biomol Ther.  2019 Jan;27(1):63-70. 10.4062/biomolther.2018.201.

Analysis of the Expression and Regulation of PD-1 Protein on the Surface of Myeloid-Derived Suppressor Cells (MDSCs)

Affiliations
  • 1Division of Biological Sciences, Research Institute of Women’s Health and Cellular Heterogeneity Research Center, Sookmyung Women's University, Seoul 04310, Republic of Korea. jslim@sookmyung.ac.kr

Abstract

Myeloid-derived suppressor cells (MDSCs) that are able to suppress T cell function are a heterogeneous cell population frequently observed in cancer, infection, and autoimmune disease. Immune checkpoint molecules, such as programmed death 1 (PD-1) expressed on T cells and its ligand (PD-L1) expressed on tumor cells or antigen-presenting cells, have received extensive attention in the past decade due to the dramatic effects of their inhibitors in patients with various types of cancer. In the present study, we investigated the expression of PD-1 on MDSCs in bone marrow, spleen, and tumor tissue derived from breast tumor-bearing mice. Our studies demonstrate that PD-1 expression is markedly increased in tumor-infiltrating MDSCs compared to expression in bone marrow and spleens and that it can be induced by LPS that is able to mediate NF-κB signaling. Moreover, expression of PD-L1 and CD80 on PD-1+ MDSCs was higher than on PD-1− MDSCs and proliferation of MDSCs in a tumor microenvironment was more strongly induced in PD-1+ MDSCs than in PD-1− MDSCs. Although we could not characterize the inducer of PD-1 expression derived from cancer cells, our findings indicate that the study on the mechanism of PD-1 induction in MDSCs is important and necessary for the control of MDSC activity; our results suggest that PD-1+ MDSCs in a tumor microenvironment may induce tumor development and relapse through the modulation of their proliferation and suppressive molecules.

Keyword

Myeloid-derived suppressor cells; PD-1; PD-L1/L2; Bone marrow cells; Tumor cell-conditioned medium; NF-κB

MeSH Terms

Animals
Antigen-Presenting Cells
Autoimmune Diseases
Bone Marrow
Bone Marrow Cells
Breast
Humans
Mice
Recurrence
Spleen
T-Lymphocytes
Tumor Microenvironment
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