酸性物质通过扰乱 IL-2、mTORC1 和 c-Myc 信号转导抑制 CD8 + T 细胞功能。

Romain Vuillefroy de Silly,Laetitia Pericou,Bili Seijo,Isaac Crespo,Melita Irving
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引用次数: 0

摘要

CD8 + T细胞在肿瘤控制中起着至关重要的作用,但其微环境中的一系列因素(如低pH值)会抑制其功能。在这里,我们证明了酸性主要通过损害 IL-2 反应性、降低细胞因子再激活时的分泌以及降低表达低亲和性 TCR 的 CD8 + T 细胞的细胞溶解能力来限制 T 细胞的扩增。我们还发现,在低 pH 值条件下,mTORC1 信号活性和 c-Myc 水平都会下降。从机理上讲,核/细胞质酸化与 mTORC1 的抑制有关,这种抑制与 Rheb、Akt/TSC2/PRAS40、GATOR1 和 Lkb1/AMPK 无关。此外,细胞内谷氨酰胺、谷氨酸和天冬氨酸水平降低,脯氨酸水平升高,但对 mTORC1 信号转导或 c-Myc 水平无明显影响。总之,我们认为,由于酸性对 CD8 + T 细胞的广泛影响,除非细胞内 pH 值得到有效控制,否则需要采取多种干预措施才能恢复 T 细胞的功能。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Acidity suppresses CD8 + T-cell function by perturbing IL-2, mTORC1, and c-Myc signaling.
CD8 + T cells have critical roles in tumor control, but a range of factors in their microenvironment such as low pH can suppress their function. Here, we demonstrate that acidity restricts T-cell expansion mainly through impairing IL-2 responsiveness, lowers cytokine secretion upon re-activation, and reduces the cytolytic capacity of CD8 + T cells expressing low-affinity TCR. We further find decreased mTORC1 signaling activity and c-Myc levels at low pH. Mechanistically, nuclear/cytoplasmic acidification is linked to mTORC1 suppression in a Rheb-, Akt/TSC2/PRAS40-, GATOR1- and Lkb1/AMPK-independent manner, while c-Myc levels drop due to both decreased transcription and higher levels of proteasome-mediated degradation. In addition, lower intracellular levels of glutamine, glutamate, and aspartate, as well as elevated proline levels are observed with no apparent impact on mTORC1 signaling or c-Myc levels. Overall, we suggest that, due to the broad impact of acidity on CD8 + T cells, multiple interventions will be required to restore T-cell function unless intracellular pH is effectively controlled.
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