免疫再生:对癌症免疫治疗及其他方面的影响。

Steven L Reiner
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引用次数: 0

摘要

利用T淋巴细胞攻击肿瘤细胞的疗法正在改变癌症治疗。与此同时,最近的基本发现已经汇集成一个框架,即淋巴细胞依赖性免疫是一种再生过程,有时被高水平的参与所超越。像干细胞一样,选择的T细胞必须平衡分化和自我更新的相互对立的需求。激活和抑制T细胞的信号指示相反的细胞代谢,通过不平衡的信息传递与兄弟细胞中出现的细胞命运相关联。新出现的研究表明,持久的免疫治疗反应可能受到自我更新T细胞丰度的限制。利用再生信号的基本发现来支持持续的、干细胞样的新分化T细胞输出,为克服癌症免疫治疗耐药性提供了新的策略。淋巴细胞再生也可能维持有害的自身免疫攻击。因此,削弱致病克隆的自我更新可能成为自身免疫性疾病的一种治疗策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Immune regeneration: implications for cancer immunotherapy and beyond.
Cancer care is being transformed by therapies leveraging T lymphocytes to attack tumor cells. In parallel, recent basic discoveries have converged into a framework of lymphocyte-dependent immunity as a regenerative process that is sometimes outstripped by high-level engagement. In a stem cell-like fashion, selected T cells must balance mutually opposing demands of differentiation and self-renewal. Activating versus inhibitory signals to T cells instruct opposing cell metabolism, linked to alternative cell fates that arise in sibling cells through lopsided information transfer. Emerging studies indicate that durable immunotherapy response may be limited by the abundance of self-renewing T cells. Leveraging of basic discoveries of regenerative signaling to bolster sustained, stem-like output of freshly differentiated T cells is offering new strategies to overcome cancer immunotherapy resistance. Lymphocyte regeneration may also sustain harmful autoimmune attack. Undercutting the self-renewal of pathogenic clones may thus emerge as a therapeutic strategy for autoimmune diseases.
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