Medical School of Nankai University, Tianjin 300071, People's Republic of China.
J Cancer Res Clin Oncol. 2010 Nov;136(11):1745-54. doi: 10.1007/s00432-010-0833-8. Epub 2010 Mar 10.
Few detailed studies about the correlations among the expanded prevalence, elevated function of Treg cells in tumor microenvironment of hepatocellular carcinoma (HCC), and different clinical tumor stage were reported. The purpose of the present study was to examine the presence and functions of CD4(+)CD25(high) regulatory T cell (Treg cell) in tumor microenvironment from early and late stages and reveal the potential underlying mechanisms that may be responsible.
The prevalence of Treg in peripheral blood and fresh tissue samples from 31 patients with HCC after radical hepatectomy and 9 controls was detected. CD127 was selected as a Treg cell maker to test the cell populations and compared its expressions with ICOS. The expressions of FOXP3 mRNA were analyzed. The migration, proliferation, and suppression functions of Treg cell were observed. IFN-γ., IL-10, TGF-ß, CCL-17, CCL-22, and SDF-1 in cell supernatant were detected. Among all of the tests, the relations among the different TNM tumor stages, populations, and functions of Treg cells were evaluated.
The prevalence of Treg cell was significantly higher in the peripheral blood and in tumor tissue compared with those in normal donors. Increased numbers of Treg cell were showed in peripheral blood as well as in tumor tissue. High levels of IL-10 and TGF-ß, but little IFN-γ, were detected in the tumor microenvironment. Treg cells potently suppressed the functions and proliferation of CD4(+)CD25(-) T cells. High levels of SDF-1 were detected in malignant biopsies compared with those in benign regions, significantly increased in stage III. Plasma from the same patient was able to chemoattract Treg cell but that was lesser extent than those in tumor supernatant. Also, supernatant in advanced stage tumors exhibited powerful chemoattractic activity. SDF-1 played an important role in the recruited functions of Treg cell into tumor microenvironment of early and advanced stages. The expressions of Foxp3 mRNA increased in different TNM stages. The increased prevalence and expanded function of Treg cells in the tumor microenvironment of HCC were correlated with the cancer stage.
The increase in frequency of Treg cells might play a role in modulation of the immune response against HCC in different TNM stages. The substance secreted in tumor microenvironment recruited CD4(+)CD25(+) Treg cells to tumor sites to contribute to the prosperity and growth of the tumors. The performance of Treg cells in different TNM stages of tumor microenvironment might be acted as the route to evaluate the immunotherapy-based methods, promote therapy effect, and consequently to increase the survival rate in HCC.
关于肝癌肿瘤微环境中调节性 T 细胞(Treg 细胞)的扩展患病率、功能升高与不同临床肿瘤分期之间的相关性,鲜有详细研究报道。本研究旨在检测早期和晚期肝癌患者肿瘤微环境中 CD4+CD25high 调节性 T 细胞(Treg 细胞)的存在和功能,并揭示可能的潜在机制。
检测 31 例根治性肝切除术后 HCC 患者和 9 例对照者外周血和新鲜组织样本中 Treg 细胞的患病率。选择 CD127 作为 Treg 细胞标志物,检测细胞群,并与 ICOSl 进行比较。分析 FOXP3 mRNA 的表达。观察 Treg 细胞的迁移、增殖和抑制功能。检测细胞上清液中的 IFN-γ、IL-10、TGF-β、CCL-17、CCL-22 和 SDF-1。在所有检测中,评估不同 TNM 肿瘤分期、Treg 细胞群和功能之间的关系。
与正常供体相比,外周血和肿瘤组织中 Treg 细胞的患病率明显升高。外周血和肿瘤组织中 Treg 细胞数量增加。肿瘤微环境中检测到高水平的 IL-10 和 TGF-β,但 IFN-γ 水平较低。Treg 细胞强烈抑制 CD4+CD25-T 细胞的功能和增殖。与良性区域相比,恶性活检中 SDF-1 水平明显升高,III 期时显著升高。同一患者的血浆能够趋化 Treg 细胞,但趋化程度低于肿瘤上清液。此外,晚期肿瘤上清液表现出强大的趋化活性。SDF-1 在早期和晚期肿瘤微环境中 Treg 细胞的募集功能中发挥重要作用。Foxp3 mRNA 的表达随不同 TNM 分期而增加。肝癌肿瘤微环境中 Treg 细胞的患病率增加和功能扩展与癌症分期相关。
Treg 细胞频率的增加可能在不同 TNM 分期的 HCC 免疫反应调节中发挥作用。肿瘤微环境中分泌的物质募集 CD4+CD25+Treg 细胞到肿瘤部位,有助于肿瘤的生长和发展。Treg 细胞在肿瘤微环境的不同 TNM 分期中的表现可作为评估基于免疫疗法的方法的途径,促进治疗效果,从而提高 HCC 的生存率。
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