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首页> 外文期刊>Journal of immunotherapy >CD8 + T-cell clones specific for the 5T4 antigen target renal cell carcinoma tumor-initiating cells in a murine xenograft model
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CD8 + T-cell clones specific for the 5T4 antigen target renal cell carcinoma tumor-initiating cells in a murine xenograft model

机译:鼠异种移植模型中对5T4抗原特异性靶向肾细胞癌肿瘤起始细胞的CD8 + T细胞克隆

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摘要

The tumor antigen 5T4 is frequently expressed at high levels on renal cell carcinoma (RCC) and other epithelial carcinomas. Surveys of normal tissues demonstrate abundant 5T4 expression on placental trophoblast cells with limited expression elsewhere. 5T4 is the target for a therapeutic cancer vaccine (MVA-5T4) that elicits 5T4-specific serological, proliferative, and cytotoxic T lymphocyte (CTL) responses. However, the antitumor activity of 5T4-specific CTL has not been extensively characterized. CD8 + T cells from HLA-A2 healthy donors (n=4) or RCC patients (n=2) were stimulated in vitro with the HLA-A2-binding nonamer peptides 5T4 17-25 or 5T4 97-105 and screened by flow cytometry with specific tetramers (TET). CD8 +/TET + T-cell clones specific for 5T417-25 or 5T4 97-105 peptide were isolated from 4/6 and 1/4 donors, respectively. A subset of clones specific for 5T 417-25 was cytolytic for MVA-5T4-infected HLA-A2 + EBV-transformed lymphoblastoid cell line target cells and for constitutively HLA-A2-expressing and 5T4-expressing RCC tumor cell lines (including A498 RCC). In a xenoengraftment assay, the coinoculation of a representative 5T4 17-25-specific CTL clone with A498 RCC tumors cells into immune-deficient mice completely prevented growth of A498 tumors. Taken together, these data demonstrate high-avidity CD8 CTL able to recognize the naturally processed 5T4 17-25 epitope on RCC tumor cells including putative tumor-initiating cells are present in peripheral blood of both healthy donors and RCC patients. CD8T-cell immunity targeting 5T 417-25 is therefore of substantial interest both as a potential target for further development of vaccination or adoptive cellular immunotherapy and for immune monitoring studies in association with nonspecific immunotherapies.
机译:肿瘤抗原5T4经常在肾细胞癌(RCC)和其他上皮癌中高水平表达。正常组织的调查显示,胎盘滋养层细胞上5T4的表达丰富,而其他地方的表达却有限。 5T4是治疗性癌症疫苗(MVA-5T4)的靶标,该疫苗可引发5T4特异性的血清学,增殖性和细胞毒性T淋巴细胞(CTL)反应。但是,尚未广泛表征5T4特异性CTL的抗肿瘤活性。用HLA-A2结合的九聚体肽5T4 17-25或5T4 97-105体外刺激HLA-A2健康供体(n = 4)或RCC患者(n = 2)的CD8 + T细胞,并通过流式细胞仪进行筛选与特定的四聚体(TET)。对5T417-25或5T4 97-105肽具有特异性的CD8 + / TET + T细胞克隆分别从4/6和1/4供体中分离出来。对5T 417-25特异的一部分克隆对MVA-5T4感染的HLA-A2 + EBV转化的淋巴母细胞样细胞系靶细胞以及组成型HLA-A2和5T4表达的RCC肿瘤细胞系(包括A498 RCC)进行细胞溶解)。在异种移植测定中,将具有代表性的5T4 17-25特异的CTL克隆与A498 RCC肿瘤细胞共接种到免疫缺陷小鼠中完全阻止了A498肿瘤的生长。综上所述,这些数据表明,高健康度的CD8 CTL能够识别RCC肿瘤细胞上自然加工的5T4 17-25表位,包括假定的肿瘤引发细胞都存在于健康供体和RCC患者的外周血中。因此,靶向5T 417-25的CD8T细胞免疫力作为进一步开发疫苗接种或过继细胞免疫疗法以及与非特异性免疫疗法相关的免疫监测研究的潜在靶标,引起了广泛关注。

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