Fatty acid metabolism in the regulation of T cell function

分解代谢 细胞代谢 效应器 免疫系统 细胞生物学 生物 脂质代谢 细胞生长 T细胞 细胞分化 信号转导 细胞 脂肪酸代谢 代谢途径 CD8型 新陈代谢 生物化学 功能(生物学) 免疫学 基因
作者
Matthias Lochner,Luciana Berod,Tim Sparwasser
出处
期刊:Trends in Immunology [Elsevier]
卷期号:36 (2): 81-91 被引量:394
标识
DOI:10.1016/j.it.2014.12.005
摘要

•T effector cell differentiation depends on de novo fatty acid (FA) synthesis. •CD8+ T memory cell development and function depend on both FA synthesis and oxidation. •FA synthesis and oxidation are determinants for CD4+ T effector versus Treg cell development. •These pathways may present therapeutic targets for modulating T cell responses in vivo. The specific regulation of cellular metabolic processes is of major importance for directing immune cell differentiation and function. We review recent evidence indicating that changes in basic cellular lipid metabolism have critical effects on T cell proliferation and cell fate decisions. While induction of de novo fatty acid (FA) synthesis is essential for activation-induced proliferation and differentiation of effector T cells, FA catabolism via β-oxidation is important for the development of CD8+ T cell memory as well as for the differentiation of CD4+ regulatory T cells. We consider the influence of lipid metabolism and metabolic intermediates on the regulation of signaling and transcriptional pathways via post-translational modifications, and discuss how an improved understanding of FA metabolism may reveal strategies for manipulating immune responses towards therapeutic outcomes. The specific regulation of cellular metabolic processes is of major importance for directing immune cell differentiation and function. We review recent evidence indicating that changes in basic cellular lipid metabolism have critical effects on T cell proliferation and cell fate decisions. While induction of de novo fatty acid (FA) synthesis is essential for activation-induced proliferation and differentiation of effector T cells, FA catabolism via β-oxidation is important for the development of CD8+ T cell memory as well as for the differentiation of CD4+ regulatory T cells. We consider the influence of lipid metabolism and metabolic intermediates on the regulation of signaling and transcriptional pathways via post-translational modifications, and discuss how an improved understanding of FA metabolism may reveal strategies for manipulating immune responses towards therapeutic outcomes.
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