大肠癌树突状细胞上的 TIM-3 表达

Cancers Pub Date : 2024-05-15 DOI:10.3390/cancers16101888
Mei Sakuma, Masanori Katagata, H. Okayama, S. Nakajima, Katsuharu Saito, Takahiro Sato, Satoshi Fukai, Hideaki Tsumuraya, H. Onozawa, W. Sakamoto, Motonobu Saito, Z. Saze, T. Momma, Kosaku Mimura, Koji Kono
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摘要

TIM-3 最初被认为是辅助性 T 细胞的负调控因子,在树突状细胞(DC)上表达。由于有人认为抑制 TIM-3 在 DCs 上的表达可增强 T 细胞介导的抗肿瘤免疫力,因此我们利用公共数据库中的转录组数据(n = 592)和我们的 CRC 队列(n = 115)中的免疫组化评估,研究了 TIM-3 在结直肠癌(CRC)肿瘤微环境(TME)中 DCs 上的表达。流式细胞术检测了 TIM-3 在体外直流细胞上的表达,Western 印迹法评估了其相关分子 cGAS 和 STING 在未成熟和成熟直流细胞上的表达。HAVCR2(TIM-3)的表达与CRC TME中DC的浸润密切相关。对临床组织样本进行免疫组化染色后发现,肿瘤浸润的DC表达TIM-3,但它们在肿瘤浸润前沿的数量会随着阶段的进展而显著减少。来自不同供体的未成熟直流细胞(n = 6)的 TIM-3 表达高于成熟直流细胞。Western 印迹分析表明,STING 在成熟 DCs 上的表达高于未成熟 DCs,这与 TIM-3 的表达相反。我们证明了TIM-3在CRC肿瘤浸润DC上的高表达,而且其在未成熟DC上的表达高于在成熟DC上的表达。
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TIM-3 Expression on Dendritic Cells in Colorectal Cancer
TIM-3 was originally identified as a negative regulator of helper T cells and is expressed on dendritic cells (DCs). Since the inhibition of TIM-3 on DCs has been suggested to enhance T cell-mediated anti-tumor immunity, we examined its expression on DCs within the tumor microenvironment (TME) in colorectal cancer (CRC) using transcriptomic data from a public database (n = 592) and immunohistochemical evaluations from our cohorts of CRC (n = 115). The expression of TIM-3 on DCs in vitro was examined by flow cytometry, while the expression of its related molecules, cGAS and STING, on immature and mature DCs was assessed by Western blotting. The expression of HAVCR2 (TIM-3) was strongly associated with the infiltration of DCs within the TME of CRC. Immunohistochemical staining of clinical tissue samples revealed that tumor-infiltrating DCs expressed TIM-3; however, their number at the tumor-invasive front significantly decreased with stage progression. TIM-3 expression was higher on immature DCs than on mature DCs from several different donors (n = 6). Western blot analyses showed that the expression of STING was higher on mature DCs than on immature DCs, which was opposite to that of TIM-3. We demonstrated that TIM-3 was highly expressed on tumor-infiltrating DCs of CRC and that its expression was higher on immature DCs than on mature DCs.
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