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单核吞噬细胞激活的细胞内代谢调节:冰山一角的发现。

Cell-intrinsic metabolic regulation of mononuclear phagocyte activation: Findings from the tip of the iceberg.

机构信息

Department of Immunometabolism, Max Planck Institute of Epigenetics and Immunobiology, Freiburg im Breisgau, Germany.

Faculty of Biology, University of Freiburg, Freiburg im Breisgau, Germany.

出版信息

Immunol Rev. 2020 May;295(1):54-67. doi: 10.1111/imr.12848. Epub 2020 Apr 3.

Abstract

We have only recently started to appreciate the extent to which immune cell activation involves significant changes in cellular metabolism. We are now beginning to understand how commitment to specific metabolic pathways influences aspects of cellular biology that are the more usual focus of immunological studies, such as activation-induced changes in gene transcription, post-transcriptional regulation of transcription, post-translational modifications of proteins, cytokine secretion, etc. Here, we focus on metabolic reprogramming in mononuclear phagocytes downstream of stimulation with inflammatory signals (such as LPS and IFNγ) vs alternative activation signals (IL-4), with an emphasis on work on dendritic cells and macrophages from our laboratory, and related studies from others. We cover aspects of glycolysis and its branching pathways (glycogen synthesis, pentose phosphate, serine synthesis, hexose synthesis, and glycerol 3 phosphate shuttle), the tricarboxylic acid pathway, fatty acid synthesis and oxidation, and mitochondrial biology. Although our understanding of the metabolism of mononuclear phagocytes has progressed significantly over the last 10 years, major challenges remain, including understanding the effects of tissue residence on metabolic programming related to cellular activation, and the translatability of findings from mouse to human biology.

摘要

我们最近才开始意识到,免疫细胞的激活涉及到细胞代谢的重大变化。我们现在开始了解到,特定代谢途径的选择如何影响细胞生物学的各个方面,这些方面通常是免疫学研究的焦点,例如激活诱导的基因转录变化、转录后的转录调控、蛋白质的翻译后修饰、细胞因子的分泌等。在这里,我们专注于单核吞噬细胞在受到炎症信号(如 LPS 和 IFNγ)刺激与替代激活信号(IL-4)刺激后的代谢重编程,重点介绍我们实验室关于树突状细胞和巨噬细胞的工作,以及其他相关研究。我们涵盖了糖酵解及其分支途径(糖原合成、戊糖磷酸途径、丝氨酸合成、己糖合成和甘油 3 磷酸穿梭)、三羧酸循环、脂肪酸合成和氧化以及线粒体生物学的各个方面。尽管我们对单核吞噬细胞代谢的理解在过去 10 年中取得了重大进展,但仍存在重大挑战,包括了解组织驻留对与细胞激活相关的代谢编程的影响,以及从小鼠到人类生物学的研究结果的可转化性。

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