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L-Arginine Modulates T Cell Metabolism and Enhances Survival and Anti-tumor Activity

机译:L-精氨酸调节T细胞代谢并增强生存和抗肿瘤活性。

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摘要

Metabolic activity is intimately linked to T cell fate and function. Using high-resolution mass spectrometry, we generated dynamic metabolome and proteome profiles of human primary naive T cells following activation. We discovered critical changes in the arginine metabolism that led to a drop in intracellular L-arginine concentration. Elevating L-arginine levels induced global metabolic changes including a shift from glycolysis to oxidative phosphorylation in activated T cells and promoted the generation of central memory-like cells endowed with higher survival capacity and, in a mouse model, anti-tumor activity. Proteome-wide probing of structural alterations, validated by the analysis of knockout T cell clones, identified three transcriptional regulators (BAZ1B, PSIP1, and TSN) that sensed L-arginine levels and promoted T cell survival. Thus, intracellular L-arginine concentrations directly impact the metabolic fitness and survival capacity of T cells that are crucial for antitumor responses.
机译:代谢活性与T细胞的命运和功能密切相关。使用高分辨率质谱,我们在激活后生成了人类原代幼稚T细胞的动态代谢组和蛋白质组图谱。我们发现精氨酸代谢的关键变化导致细胞内L-精氨酸浓度下降。升高的L-精氨酸水平诱导了整体代谢变化,包括活化T细胞从糖酵解转变为氧化磷酸化,并促进了中央记忆样细胞的产生,这些细胞具有更高的生存能力,并且在小鼠模型中具有抗肿瘤活性。通过对敲除的T细胞克隆进行分析验证了蛋白质组学上的结构改变,发现了三个转录调节因子(BAZ1B,PSIP1和TSN),它们可以检测L-精氨酸水平并促进T细胞存活。因此,细胞内L-精氨酸浓度直接影响T细胞的代谢适应性和存活能力,这对于抗肿瘤反应至关重要。

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