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Regulation of lipid stores and metabolism by lipophagy

机译:脂质吞噬对脂质存储和代谢的调节

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Intracellular lipids are stored in lipid droplets (LDs) and metabolized by cytoplasmic neutral hydrolases to supply lipids for cell use. Recently, an alternative pathway of lipid metabolism through the lysosomal degradative pathway of autophagy has been described and termed lipophagy. In this form of lipid metabolism, LD triglycerides (TGs) and cholesterol are taken up by autophagosomes and delivered to lysosomes for degradation by acidic hydrolases. Free fatty acids generated by lipophagy from the breakdown of TGs fuel cellular rates of mitochondrial β-oxidation. Lipophagy therefore functions to regulate intracellular lipid stores, cellular levels of free lipids such as fatty acids and energy homeostasis. The amount of lipid metabolized by lipophagy varies in response to the extracellular supply of nutrients. The ability of the cell to alter the amount of lipid targeted for autophagic degradation depending on nutritional status demonstrates that this process is selective. Intracellular lipids themselves regulate levels of autophagy by unclear mechanisms. Impaired lipophagy can lead to excessive tissue lipid accumulation such as hepatic steatosis, alter hypothalamic neuropeptide release to affect body mass, block cellular transdifferentiation and sensitize cells to death stimuli. Future studies will likely identify additional mechanisms by which lipophagy regulates cellular physiology, making this pathway a potential therapeutic target in a variety of diseases.
机译:细胞内脂质存储在脂质滴(LDs)中,并被细胞质中性水解酶代谢,以提供脂质供细胞使用。最近,已经描述了通过自噬的溶酶体降解途径的脂质代谢的另一种途径,并称为脂质吞噬。在这种形式的脂质代谢中,LD3甘油酯(TGs)和胆固醇被自噬体吸收,并被运送至溶酶体,以通过酸性水解酶降解。 TG分解导致的脂肪吞噬产生的游离脂肪酸促进了线粒体β-氧化的细胞速率。因此,脂蛋白的功能是调节细胞内脂质的储存,游离脂质(如脂肪酸)的细胞水平和能量稳态。通过脂肪吞噬代谢的脂质的量随营养素的细胞外供应而变化。细胞根据营养状况改变靶向自噬降解的脂质量的能力证明该过程是选择性的。细胞内脂质本身通过不清楚的机制调节自噬水平。脂肪吞噬障碍可导致过多的组织脂质蓄积,例如肝脂肪变性,改变下丘脑神经肽释放以影响体重,阻止细胞转分化并使细胞对死亡刺激敏感。未来的研究可能会发现脂肪吞噬调节细胞生理的其他机制,从而使该途径成为多种疾病的潜在治疗靶标。

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