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Active surveillance characterizes human intratumoral T cell exhaustion

机译:主动监测表征人类瘤内 T 细胞耗竭

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摘要

Intratumoral T cells that might otherwise control tumors are often identified in an "exhausted" state, defined by specific epigenetic modifications and upregulation of genes such as CD38, cytotoxic T-lymphocyte-associated protein 4 (CTLA4), and programmed cell death 1 (PD1). Although the term might imply inactivity, there has been little study of this state at the phenotypic level in tumors to understand the extent of their incapacitation. Starting with the observation that T cells move more quickly through mouse tumors the longer they reside there and progress toward exhaustion, we developed a nonstimulatory, live-biopsy method for the real-time study of T cell behavior within individual patient tumors. Using 2-photon microscopy, we studied native CD8(+) T cell interaction with antigen-presenting cells (APCs) and cancer cells in different microniches of human tumors and found that T cell speed was variable by region and by patient and was inversely correlated with local tumor density. Across a range of tumor types, we found a strong relationship between CD8(+) T cell motility and the exhausted T cell state that corresponded with our observations made in mouse models in which exhausted T cells moved faster. Our study demonstrates T cell dynamic states in individual human tumors and supports the existence of an active program in "exhausted" T cells that extends beyond incapacitating them.
机译:可能控制肿瘤的瘤内 T 细胞通常处于“耗尽”状态,定义为 CD38、细胞毒性 T 淋巴细胞相关蛋白 4 (CTLA4) 和程序性细胞死亡 1 (PD1) 等基因的特异性表观遗传修饰和上调。尽管该术语可能意味着不活动,但在肿瘤的表型水平上对这种状态的研究很少,以了解其失能的程度。从观察到 T 细胞在小鼠肿瘤中停留的时间越长并逐渐耗尽,它们通过小鼠肿瘤移动得越快,我们开发了一种非刺激活体活检方法,用于实时研究个体患者肿瘤内的 T 细胞行为。使用双光子显微镜,我们研究了天然CD8(+)T细胞与人类肿瘤不同微生态位中抗原呈递细胞(APC)和癌细胞的相互作用,发现T细胞速度因区域和患者而异,并且与局部肿瘤密度呈负相关。在一系列肿瘤类型中,我们发现CD8(+)T细胞运动与耗竭的T细胞状态之间存在很强的关系,这与我们在小鼠模型中观察到的T细胞移动得更快。我们的研究证明了个体人类肿瘤中的T细胞动态状态,并支持在“耗尽”的T细胞中存在一种活跃的程序,这种程序超出了使它们丧失能力的范围。

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