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胆碱介导的黄颡鱼肝脂代谢稳态:揭示胆碱的脂肪作用和甲基供体功能,以及信号通路的意义。

Choline-mediated hepatic lipid homoeostasis in yellow catfish: unravelling choline's lipotropic and methyl donor functions and significance of signalling pathway.

机构信息

Key Laboratory of Freshwater Animal Breeding, Ministry of Agriculture, Fishery College, Huazhong Agricultural University, Wuhan430070, People's Republic of China.

Laboratory for Marine Fisheries Science and Food Production Processes, Qingdao National Laboratory for Marine Science and Technology, Qingdao266237, People's Republic of China.

出版信息

Br J Nutr. 2024 Jan 28;131(2):202-213. doi: 10.1017/S000711452300185X. Epub 2023 Aug 29.

Abstract

Choline plays a crucial role in hepatic lipid homeostasis by acting as a major methyl-group donor. However, despite this well-accepted fact, no study has yet explored how choline's methyl-donor function contributes to preventing hepatic lipid dysregulation. Moreover, the potential regulatory role of Ire-1, an ER-transmembrane transducer for the unfolded protein response (UPRer), in choline-mediated hepatic lipid homeostasis remains unexplored. Thus, this study investigated the mechanism by which choline prevents hepatic lipid dysregulation, focusing on its role as a methyl-donor and the involvement of Ire-1 in this process. To this end, a model animal for lipid metabolism, yellow catfish () were fed two different diets (adequate or deficient choline diets) for 10 weeks. The key findings of studies are as follows: 1. Dietary choline, upregulated selected lipolytic and fatty acid -oxidation transcripts promoting hepatic lipid homeostasis. 2. Dietary choline ameliorated UPRer and prevented hepatic lipid dysregulation mainly through signalling, not perk or signalling. 3. Choline inhibited the transcriptional expression level of ire-1 by activating site-specific DNA methylations in the promoter of . 4. Choline-mediated methylations reduced Ire-1/Fas interactions, thereby further inhibiting Fas activity and reducing lipid droplet deposition. These results offer a novel insight into the direct and indirect regulation of choline on lipid metabolism genes and suggests a potential crosstalk between signalling and choline-deficiency-induced hepatic lipid dysregulation, highlighting the critical contribution of choline as a methyl-donor in maintaining hepatic lipid homeostasis.

摘要

胆碱作为主要的甲基供体,在肝脏脂质动态平衡中起着至关重要的作用。然而,尽管这是一个公认的事实,但迄今为止,尚无研究探讨胆碱的甲基供体功能如何有助于防止肝脏脂质失调。此外,IRE-1 在胆碱介导的肝脏脂质动态平衡中的作用也尚未被探索,IRE-1 是未折叠蛋白反应(UPRer)的内质网跨膜转导物。因此,本研究探讨了胆碱防止肝脏脂质失调的机制,重点研究了其作为甲基供体的作用以及 IRE-1 在该过程中的参与。为此,采用黄色鲶鱼()作为脂质代谢模型动物,用两种不同的饮食(胆碱充足或缺乏的饮食)喂养 10 周。研究的主要发现如下:1. 饮食中的胆碱上调了选定的脂肪分解和脂肪酸氧化转录本,促进了肝脏脂质动态平衡。2. 饮食中的胆碱通过 信号改善 UPRer 并预防肝脏脂质失调,而不是 perk 或 信号。3. 胆碱通过激活 启动子中的特定位点 DNA 甲基化抑制 ire-1 的转录表达水平。4. 胆碱介导的甲基化减少了 ire-1/Fas 的相互作用,从而进一步抑制 Fas 活性并减少脂质滴沉积。这些结果为胆碱对脂质代谢基因的直接和间接调控提供了新的见解,并提示了 信号和胆碱缺乏诱导的肝脏脂质失调之间的潜在串扰,突出了胆碱作为甲基供体在维持肝脏脂质动态平衡中的关键作用。

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