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PD-L1 Overexpression, SWI/SNF Complex Deregulation, and Profound Transcriptomic Changes Characterize Cancer-Dependent Exhaustion of Persistently Activated CD4+ T Cells

Jancewicz, I. and Szarkowska, J. and Konopinski, R. and Stachowiak, M. and Swiatek, M. and Blachnio, K. and Kubala, Szymon and Oksińska, Paulina and Cwiek, P. and Rusetska, N. and Tupalska, Agnieszka and Zeber-Lubecka, N. and Grabowska, Ewa and Świderska, Bianka and Malinowska, Agata and Mikula, Michał and Jagielska, Beata and Walewski, J. and Siedlecki, J.A. and Sarnowski, T.J. and Markowicz, S. and Sarnowska, E.A. (2021) PD-L1 Overexpression, SWI/SNF Complex Deregulation, and Profound Transcriptomic Changes Characterize Cancer-Dependent Exhaustion of Persistently Activated CD4+ T Cells. Cancers, 13 (16). p. 4148. ISSN 2072-6694

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Official URL: https://doi.org/10.3390/cancers13164148

Abstract

Growing tumors avoid recognition and destruction by the immune system. During continuous stimulation of tumor-infiltrating lymphocytes (TILs) by tumors, TILs become functionally exhausted; thus, they become unable to kill tumor cells and to produce certain cytokines and lose their ability to proliferate. This collectively results in the immune escape of cancer cells. Here, we show that breast cancer cells expressing PD-L1 can accelerate exhaustion of persistently activated human effector CD4+ T cells, manifesting in high PD-1 and PD-L1 expression level son T cell surfaces, decreased glucose metabolism genes, strong downregulation of SWI/SNF chromatin remodelingcomplex subunits, and p21 cell cycle inhibitor upregulation. This results in inhibition of T cell proliferation and reduction of T cell numbers. The RNAseq analysis on exhausted CD4+ T cells indicated strong overexpression of IDO1 and genes encoding pro-inflammatory cytokines and chemokines. Some interleukins were also detected in media from CD4+ T cells co-cultured with cancer cells. The PD-L1 overexpression was also observed in CD4+ T cells after co-cultivation with other cell lines overexpressing PD-L1, which suggested the existence of a general mechanism of CD4+ T cell exhaustion induced by cancer cells. The ChIP analysis on the PD-L1 promoter region indicated that the BRM recruitment in control CD4+ T cells was replaced by BRG1 and EZH2 in CD4+ T cells strongly exhausted by cancer cells. These findings suggest that epi-drugs such as EZH2 inhibitors may be used as immunomodulators in cancer treatment.

Item Type:Article
Subjects:R Medicine > R Medicine (General)
Divisions:Department of Protein Biosynthesis
ID Code:2086
Deposited By: dr hab Tomasz/T.J. Sarnowski
Deposited On:22 Sep 2021 07:28
Last Modified:22 Sep 2021 07:28

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