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Fueling the flame: bioenergy couples metabolism and inflammation

机译:助燃火焰:生物能耦合新陈代谢和炎症

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摘要

We review the emerging concept that changes in cellular bioenergetics concomitantly reprogram inflammatory and metabolic responses. The molecular pathways of this integrative process modify innate and adaptive immune reactions associated with inflammation, as well as influencing the physiology of adjacent tissue and organs. The initiating proinflammatory phase of inflammation is anabolic and requires glucose as the primary fuel, whereas the opposing adaptation phase is catabolic and requires fatty acid oxidation. The fuel switch to fatty acid oxidation depends on the sensing of AMP and NAD+ by AMPK and the SirT family of deacetylases (e.g., SirT1, -6, and -3), respectively, which couple inflammation and metabolism by chromatin and protein reprogramming. The AMP-AMPK/NAD+-SirT axis proceeds sequentially during acute systemic inflammation associated with sepsis but ceases during chronic inflammation associated with diabetes, obesity, and atherosclerosis. Rebalancing bioenergetics resolves inflammation. Manipulating cellular bioenergetics is identifying new ways to treat inflammatory and immune diseases.
机译:我们审查了新兴的概念,即细胞生物能学的变化会同时重新编程炎症和代谢反应。这种整合过程的分子途径改变了与炎症相关的先天性和适应性免疫反应,并影响了邻近组织和器官的生理。炎症的起始促炎期是合成代谢的,需要葡萄糖作为主要燃料,而相反的适应期是分解代谢的,需要脂肪酸氧化。燃料转换为脂肪酸氧化取决于AMPK和脱乙酰基酶SirT家族(例如SirT1,-6和-3)对AMP和NAD + 的检测,它们分别与炎症和通过染色质和蛋白质重编程进行新陈代谢。 AMP-AMPK / NAD + -SirT轴在与败血症相关的急性全身性炎症期间依次进行,但在与糖尿病,肥胖和动脉粥样硬化相关的慢性炎症期间停止进行。重新平衡生物能学可以解决炎症。操纵细胞生物能学正在寻找治疗炎症和免疫疾病的新方法。

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