Radiotherapy enhances CXCR3highCD8+ T cell activation through inducing IFNγ-mediated CXCL10 and ICAM-1 expression in lung cancer cells

被引：16

作者：

Wang, Chih-Liang ^{[1
]}

Ho, Ai-Sheng ^{[2
]}

Chang, Chun-Chao ^{[3
,4
,5
]}

Sie, Zong-Lin ^{[6
]}

Peng, Cheng-Liang ^{[7
]}

Chang, Jungshan ^{[8
]}

Cheng, Chun-Chia ^{[1
,6
]}

机构：

[1] Chang Gung Mem Hosp, Dept Thorac Med, Div Pulm Oncol & Intervent Bronchoscopy, Taoyuan 333, Taiwan

[2] Cheng Hsin Gen Hosp, Div Gastroenterol, Taipei 112, Taiwan

[3] Taipei Med Univ Hosp, Dept Internal Med, Div Gastroenterol & Hepatol, Taipei 110, Taiwan

[4] Taipei Med Univ, Coll Med, Sch Med, Div Gastroenterol & Hepatol,Dept Internal Med, Taipei 110, Taiwan

[5] Taipei Med Univ, TMU Res Ctr Digest Med, Taipei 110, Taiwan

[6] Chang Gung Univ, Inst Radiol Res, Radiat Biol Res Ctr, Taoyuan 333, Taiwan

[7] Atom Energy Council, Inst Nucl Energy Res, Taoyuan 325, Taiwan

[8] Taipei Med Univ, Grad Inst Med Sci, Coll Med, Sch Med, Taipei 110, Taiwan

来源：

CANCER IMMUNOLOGY IMMUNOTHERAPY | 2023年 / 72卷 / 06期

关键词：

CD8(+) T cells; CXCR3; CXCL10; IFN gamma; ICAM-1; Lung cancer; PD-L1; STAT3; Radiotherapy; INTERFERON-GAMMA; IMMUNOTHERAPY; THERAPY; BINDING; PD-L1; EFFECTOR; RECEPTOR;

D O I：

10.1007/s00262-023-03379-6

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Radiotherapy (RT) not only damages tumors but also induces interferon (IFN) expression in tumors. IFNs mediate PD-L1 to exhaust CD8(+) T cells, but which also directly impact tumor cells and potentially activate anti-tumor immune surveillance. Little is known about the contradictory mechanism of IFNs in regulating CD8(+) T-mediated anti-tumor activity in lung cancer. This study found that RT induced IFNs and CXCL9/10 expression in the RT-treated lung cancer cells. Specifically, RT- and IFN gamma-pretreated A549 significantly activated CD8(+) T cells, resulting in significant inhibition of A549 colony formation. RNAseq and consequent qPCR results revealed that IFN gamma induced PD-L1, CXCL10, and ICAM-1, whereas PD-L1 knockdown activated CD8(+) T cells, but ICAM-1 knockdown diminished CD8(+) T cell activation. We further demonstrated that CXCR3 and CXCL10 decreased in the CD8(+) T cells and nonCD8(+) PBMCs, respectively, in the patients with lung cancer that expressed lower reactivation as co-cultured with A549 cells. In addition, inhibitors targeting CXCR3 and LFA-1 in CD8(+) T cells significantly diminished CD8(+) T cell activation and splenocytes-mediated anti-LL/2shPdl1. In conclusion, we validated that RT suppressed lung cancer and overexpress PD-L1, CXCL10, and ICAM-1, which exhibited different roles in regulating CD8(+) T cell activity. We propose that CXCR3(high)CD8(+) T cells stimulated by CXCL10 exhibit anti-tumor immunity, possibly by enhancing T cells-tumor cells adhesion through CXCL10/CXCR3-activated LFA-1-ICAM-1 interaction, but CXCR3(low)CD8(+) T cells with low CXCL10 in patients with lung cancer were exhausted by PD-L1 dominantly. Therefore, RT potentially activates CD8(+) T cells by inducing IFNs-mediated CXCL10 and ICAM-1 expression in tumors to enhance CD8(+) T-tumor adhesion and recognition. This study clarified the possible mechanisms of RT and IFNs in regulating CD8(+) T cell activation in lung cancer.

引用

页码：1865 / 1880

页数：16

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