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从神经细胞和组织到成纤维细胞的甘油磷脂代谢的昼夜节律调节和生物钟控制机制

Circadian Regulation and Clock-Controlled Mechanisms of Glycerophospholipid Metabolism from Neuronal Cells and Tissues to Fibroblasts.

作者信息

Guido Mario E, Monjes Natalia M, Wagner Paula M, Salvador Gabriela A

机构信息

CIQUIBIC-CONICET, Facultad de Ciencias Químicas, Universidad Nacional de Córdoba, Córdoba, 5000, Argentina.

Departamento de Química Biológica "Ranwel Caputto", Facultad de Ciencias Químicas, Universidad Nacional de Córdoba, Córdoba, 5000, Argentina.

出版信息

Mol Neurobiol. 2022 Jan;59(1):326-353. doi: 10.1007/s12035-021-02595-4. Epub 2021 Oct 26.

Abstract

Along evolution, living organisms developed a precise timekeeping system, circadian clocks, to adapt life to the 24-h light/dark cycle and temporally regulate physiology and behavior. The transcriptional molecular circadian clock and metabolic/redox oscillator conforming these clocks are present in organs, tissues, and even in individual cells, where they exert circadian control over cellular metabolism. Disruption of the molecular clock may cause metabolic disorders and higher cancer risk. The synthesis and degradation of glycerophospholipids (GPLs) is one of the most highly regulated metabolisms across the 24-h cycle in terms of total lipid content and enzyme expression and activity in the nervous system and individual cells. Lipids play a plethora of roles (membrane biogenesis, energy sourcing, signaling, and the regulation of protein-chromatin interaction, among others), making control of their metabolism a vital checkpoint in the cellular organization of physiology. An increasing body of evidence clearly demonstrates an orchestrated and sequential series of events occurring in GPL metabolism across the 24-h day in diverse retinal cell layers, immortalized fibroblasts, and glioma cells. Moreover, the clock gene Per1 and other circadian-related genes are tightly involved in the regulation of GPL synthesis in quiescent cells. However, under proliferation, the metabolic oscillator continues to control GPL metabolism of brain cancer cells even after molecular circadian clock disruption, reflecting the crucial role of the temporal metabolism organization in cell preservation. The aim of this review is to examine the control exerted by circadian clocks over GPL metabolism, their synthesizing enzyme expression and activities in normal and tumorous cells of the nervous system and in immortalized fibroblasts.

摘要

在进化过程中,生物体发展出了精确的计时系统——生物钟,以使生命适应24小时的光/暗周期,并在时间上调节生理和行为。符合这些生物钟的转录分子生物钟以及代谢/氧化还原振荡器存在于器官、组织甚至单个细胞中,在这些地方它们对细胞代谢进行昼夜节律控制。分子生物钟的破坏可能导致代谢紊乱和更高的癌症风险。甘油磷脂(GPLs)的合成和降解是整个24小时周期中,在神经系统和单个细胞的总脂质含量、酶表达及活性方面,调控最为严格的代谢过程之一。脂质发挥着众多作用(如膜生物合成、能量供应、信号传导以及蛋白质 - 染色质相互作用的调节等),因此对其代谢的控制是细胞生理组织中的一个关键检查点。越来越多的证据清楚地表明,在不同的视网膜细胞层、永生化成纤维细胞和胶质瘤细胞中,GPL代谢在24小时内会发生一系列精心编排且有序的事件。此外,生物钟基因Per1和其他与昼夜节律相关的基因紧密参与静止细胞中GPL合成的调节。然而,在细胞增殖状态下,即使分子生物钟被破坏,代谢振荡器仍继续控制着脑癌细胞的GPL代谢,这反映了时间代谢组织在细胞维持中的关键作用。本综述的目的是研究生物钟对GPL代谢的控制,以及它们在神经系统的正常和肿瘤细胞以及永生化成纤维细胞中的合成酶表达和活性。

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