细胞器
细胞生物学
转运蛋白
内体
脂滴
膜接触部位
生物
膜蛋白
脂质代谢
化学
生物化学
膜
整体膜蛋白
细胞内
作者
Nikit Kumar,Marianna Leonzino,William Hancock‐Cerutti,Florian A. Horenkamp,Peiqi Li,Joshua A. Lees,Heather Wheeler,Karin M. Reinisch,Pietro De Camilli
标识
DOI:10.1083/jcb.201807019
摘要
Mutations in the human VPS13 genes are responsible for neurodevelopmental and neurodegenerative disorders including chorea acanthocytosis (VPS13A) and Parkinson’s disease (VPS13C). The mechanisms of these diseases are unknown. Genetic studies in yeast hinted that Vps13 may have a role in lipid exchange between organelles. In this study, we show that the N-terminal portion of VPS13 is tubular, with a hydrophobic cavity that can solubilize and transport glycerolipids between membranes. We also show that human VPS13A and VPS13C bind to the ER, tethering it to mitochondria (VPS13A), to late endosome/lysosomes (VPS13C), and to lipid droplets (both VPS13A and VPS13C). These findings identify VPS13 as a lipid transporter between the ER and other organelles, implicating defects in membrane lipid homeostasis in neurological disorders resulting from their mutations. Sequence and secondary structure similarity between the N-terminal portions of Vps13 and other proteins such as the autophagy protein ATG2 suggest lipid transport roles for these proteins as well.
科研通智能强力驱动
Strongly Powered by AbleSci AI