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Astrocytoma infiltrating lymphocytes include major T cell clonal expansions confined to the CD8 subset

机译:星形细胞瘤浸润淋巴细胞包括主要的T细胞克隆性扩增,局限于CD8亚群

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摘要

Anaplastic astrocytoma and glioblastoma are frequent and malignant brain tumors that are infiltrated by T lymphocytes. Whether these cells result from non-specific inflammation following blood-brain barrier disruption or an antigen-driven specific immune response is unknown. In this study, an in-depth characterization of TCR diversity in tumor and blood RNA biopsies was performed in a series of 16 patients with malignant astrocytoma. Whilst there was no obvious restriction of the AV and BV gene segment usage, complementarity-determining region 3 size analysis and sequencing of amplified TCR transcripts revealed multiple T cell oligoclonal expansions in all astrocytomas analyzed. Unique T cell clones were present in different adjacent areas of a given tumor, but never detected in the blood. Quantification of the number of TCR clonal transcripts per μg of tumor RNA indicated that certain T cell clonal expansions may represent at least 300 cells/106 tumor cells. Furthermore, we demonstrated that the in vivo expanded clones were almost exclusively confined to the CD8+ subset. Overall, these data suggest that spontaneous antigen-driven immune responses may be elicited against human astrocytoma despite the immunosuppressive microenvironment generated by the brain and the tumor itself. However, the ultimate failure of the immune system to control tumor growth could be the consequence of a deficient CD4 Th component of the response. This observation could have important consequences for the development of immunotherapies for astrocytoma patients
机译:间变性星形细胞瘤和胶质母细胞瘤是常见的恶性脑肿瘤,可通过T淋巴细胞浸润。这些细胞是否是由血脑屏障破坏后的非特异性炎症或抗原驱动的特异性免疫应答引起的。在这项研究中,对16例恶性星形细胞瘤患者进行了肿瘤和血液RNA活检中TCR多样性的深入表征。虽然没有明显限制AV和BV基因片段的使用,但互补决定区3大小分析和扩增的TCR转录本的测序揭示了在所有星形细胞瘤中多个T细胞寡克隆扩增。独特的T细胞克隆存在于给定肿瘤的不同相邻区域,但从未在血液中检测到。每μg肿瘤RNA的TCR克隆转录物数量的定量表明,某些T细胞克隆扩增可能代表至少300个细胞/ 106个肿瘤细胞。此外,我们证明了体内扩增的克隆几乎完全局限于CD8 +亚群。总体而言,这些数据表明,尽管大脑和肿瘤本身产生了免疫抑制性微环境,但仍可引发针对人星形细胞瘤的自发性抗原驱动的免疫反应。但是,免疫系统控制肿瘤生长的最终失败可能是反应中CD4 Th成分不足的结果。该观察结果可能对星形细胞瘤患者免疫疗法的发展产生重要影响

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