线粒体
细胞生物学
化学
脂滴
磷脂酰丝氨酸
脂肪酸
脂质代谢
生物化学
细胞
受体
生物物理学
基因亚型
脂质信号
分泌物
脂毒性
能量转移
HEK 293细胞
细胞器
脂肪酸代谢
新陈代谢
作者
Hanbing Xue,Xingwen Hu,Zhenni Yang,Yiqing Cao,Qi Zhu,Hongyun Zhao,X C,Tianxin Lei,Dian Zhuang,Jing Zheng,Siqi Guo,Xiaochuan Fu,Ka Kit Chung,Pingsheng Liu,Xiaohong Zhuang,Zhengyu Liang,Sicong He,Hui Jiang,Yan Zhao
标识
DOI:10.1083/jcb.202605090
摘要
Fatty acids (FAs) are transported from lipid droplets (LDs) to mitochondria for β-oxidation during cell starvation. Starvation also triggers engulfment of LDs by autophagosomes and their subsequent degradation by lysosomes (lipophagy). The mechanisms coordinating these pathways remain unclear. Here, we demonstrate that PISD-LD, an LD-localized isoform of phosphatidylserine decarboxylase, facilitates FA transfer while inhibiting lipophagy. PISD-LD mediates LD-mitochondrion (LD-mito) contacts via interaction with mitochondrial PISD. In PISD-LD KD cells, LDs are larger, and FA trafficking and mitochondrial FA β-oxidation are suppressed. The lipid transfer proteins ATG2A/B are recruited by PISDs to mediate FA transfer from LDs to mitochondria. Disruption of PISD-LD-mediated LD-mito contacts activates lipophagy, aiding LD degradation. PISD-LD binds the lipophagy receptor Spartin and inhibits lipophagy by impeding Spartin-LC3 interaction. PISD-LD also regulates LD-mito contacts and lipid metabolism in mouse liver. Thus, PISD-LD serves as a switch between LD-to-mitochondrion FA transfer and lipophagy, ensuring efficient energy production.
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