Division of Gastroenterology, Department of Medicine, Showa University School of Medicine, 1-5-8 Hatanodai, Shinagawa-ku, Tokyo 142-8666, Japan.
J Gastroenterol. 2010 Apr;45(4):451-8. doi: 10.1007/s00535-009-0155-2. Epub 2009 Nov 20.
We investigated whether tumor-specific CD8(+) T-cell responses affect tumor-free survival as well as the relationship between CD8(+) T-cell responses against tumor-associated antigens (TAAs) and the clinical course after tumor treatment in patients with hepatocellular carcinoma (HCC).
Twenty patients with HCC that were treated by radiofrequency ablation or trans-catheter chemo-embolization (TACE) and in whom HCC was undetectable by ultrasonography, CT, and/or MRI 1 month after treatment were enrolled in the study. Before and after treatment for HCC, analyses of TAA (glypican-3, NY-ESO-1, and MAGE-1)-specific CD8(+) T-cell responses were evaluated with an interferon-gamma enzyme-linked immunospot (ELISpot) assay using peripheral CD8(+) T-cells, monocytes, and 104 types of 20-mer synthetic peptide overlapping by 10 residues and spanning the entirety of the 3 TAAs.
Sixteen out of 20 patients (80%) showed a positive response (> or = 10 TAA-specific cells/10(5) CD8(+) T-cells) before or after treatment. When we performed univariate analysis of prognostic factors for the tumor-free period in the 20 patients, platelet count, prothrombin time, and the number of TAA-specific CD8(+) T-cells after treatment were significant factors (P = 0.027, 0.030, and 0.004, respectively). In multivariate analysis, the magnitude of the TAA-specific CD8(+) T-cell response (> or = 40 TAA-specific cells/10(5) CD8(+) T-cells) was the only significant prognostic factor for a prolonged tumor-free interval (hazard ratio 0.342, P = 0.022).
Our results suggest that strong TAA-specific CD8(+) T-cell responses suppress the recurrence of HCC. Immunotherapy to induce TAA-specific cytotoxic T lymphocytes by means such as the use of peptide vaccines should be considered for clinical application in patients with HCC after local therapy.
我们研究了肿瘤特异性 CD8(+) T 细胞应答是否影响无肿瘤存活期,以及 HCC 患者肿瘤治疗后 CD8(+) T 细胞应答与肿瘤相关抗原 (TAA) 的关系以及临床病程之间的关系。
本研究纳入了 20 例接受射频消融或经导管化疗栓塞 (TACE) 治疗且治疗后 1 个月超声、CT 和/或 MRI 均无法检测到 HCC 的 HCC 患者。在 HCC 治疗前后,使用干扰素-γ酶联免疫斑点(ELISpot)分析评估了外周血 CD8(+) T 细胞、单核细胞和 104 种 20 个氨基酸重叠 10 个氨基酸残基并覆盖 3 个 TAA 全长的肽段的糖蛋白 3 (glypican-3)、NY-ESO-1 和 MAGE-1 特异性 CD8(+) T 细胞应答。
20 例患者中有 16 例(80%)在治疗前后表现出阳性反应(>或= 10 个 TAA 特异性细胞/10(5) CD8(+) T 细胞)。在对 20 例患者无肿瘤期的预后因素进行单因素分析时,血小板计数、凝血酶原时间和治疗后 TAA 特异性 CD8(+) T 细胞数是显著因素(P = 0.027、0.030 和 0.004)。在多因素分析中,TAA 特异性 CD8(+) T 细胞应答的大小(>或= 40 个 TAA 特异性细胞/10(5) CD8(+) T 细胞)是无肿瘤间期延长的唯一显著预后因素(风险比 0.342,P = 0.022)。
我们的结果表明,强烈的 TAA 特异性 CD8(+) T 细胞应答抑制 HCC 的复发。免疫疗法通过使用肽疫苗诱导 TAA 特异性细胞毒性 T 淋巴细胞,应考虑在 HCC 患者局部治疗后用于临床应用。
