Centre for Translational Medicine and Therapeutics, William Harvey Research Institute, Queen Mary University of London, London, United Kingdom.
Institute of Immunology and Immunotherapy, College of Medical and Dental Sciences, University of Birmingham, Birmingham, United Kingdom.
Front Immunol. 2022 Oct 14;13:990794. doi: 10.3389/fimmu.2022.990794. eCollection 2022.
The immune system protects from infections and cancer through complex cellular networks. For this purpose, immune cells require well-developed mechanisms of energy generation. However, the immune system itself can also cause diseases when defective regulation results in the emergence of autoreactive lymphocytes. Recent studies provide insights into how differential patterns of immune cell responses are associated with selective metabolic pathways. This review will examine the changing metabolic requirements of Th17 cells and of B cells at different stages of their development and activation. Both cells provide protection but can also mediate diseases through the production of autoantibodies and the production of proinflammatory mediators. In health, B cells produce antibodies and cytokines and present antigens to T cells to mount specific immunity. Th17 cells, on the other hand, provide protection against extra cellular pathogens at mucosal surfaces but can also drive chronic inflammation. The latter cells can also promote the differentiation of B cells to plasma cells to produce more autoantibodies. Metabolism-regulated checkpoints at different stages of their development ensure the that self-reactive B cells clones and needless production of interleukin (IL-)17 are limited. The metabolic regulation of the two cell types has some similarities, e.g. the utility of hypoxia induced factor (HIF)1α during low oxygen tension, to prevent autoimmunity and regulate inflammation. There are also clear differences, as Th17 cells only are vulnerable to the lack of certain amino acids. B cells, unlike Th17 cells, are also dependent of mechanistic target of rapamycin 2 (mTORC2) to function. Significant knowledge has recently been gained, particularly on Th17 cells, on how metabolism regulates these cells through influencing their epigenome. Metabolic dysregulation of Th17 cells and B cells can lead to chronic inflammation. Disease associated alterations in the genome can, in addition, cause dysregulation to metabolism and, thereby, result in epigenetic alterations in these cells. Recent studies highlight how pathology can result from the cooperation between the two cell types but only few have so far addressed the key metabolic alterations in such settings. Knowledge of the impact of metabolic dysfunction on chronic inflammation and pathology can reveal novel therapeutic targets to treat such diseases.
免疫系统通过复杂的细胞网络来保护身体免受感染和癌症的侵害。为此,免疫细胞需要发达的能量生成机制。然而,当缺陷调节导致自身反应性淋巴细胞出现时,免疫系统本身也会导致疾病。最近的研究提供了关于免疫细胞反应的不同模式如何与选择性代谢途径相关联的见解。这篇综述将探讨 Th17 细胞和 B 细胞在其发育和激活的不同阶段的代谢需求变化。这两种细胞都能提供保护,但也可以通过产生自身抗体和产生促炎介质来介导疾病。在健康状态下,B 细胞产生抗体和细胞因子,并将抗原呈递给 T 细胞以产生特异性免疫。Th17 细胞则在黏膜表面抵御细胞外病原体,但也能引发慢性炎症。后者还可以促进 B 细胞向浆细胞分化,以产生更多的自身抗体。在其发育的不同阶段,受代谢调控的检查点确保了自我反应性 B 细胞克隆和不必要的白细胞介素(IL)-17 的产生受到限制。两种细胞类型的代谢调控有一些相似之处,例如在低氧张力下缺氧诱导因子(HIF)1α的利用,以防止自身免疫和调节炎症。也有明显的差异,因为 Th17 细胞仅易受某些氨基酸缺乏的影响。与 Th17 细胞不同,B 细胞也依赖雷帕霉素靶蛋白(mTORC2)来发挥作用。最近,人们对代谢如何通过影响细胞的表观基因组来调节这些细胞有了更多的了解,特别是在 Th17 细胞方面。Th17 细胞和 B 细胞的代谢失调可导致慢性炎症。与疾病相关的基因组改变除了会导致代谢失调外,还会导致这些细胞的表观遗传改变。最近的研究强调了病理如何可以由两种细胞类型的合作引起,但到目前为止,很少有研究涉及这种情况下的关键代谢改变。了解代谢功能障碍对慢性炎症和病理学的影响可以揭示治疗这些疾病的新治疗靶点。
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