内质网
细胞器
细胞生物学
生物发生
细胞器生物发生
过氧化物酶体
膜接触部位
脂滴
生物
萌芽
复印机
复印件
小泡
膜蛋白
化学
高尔基体
生物化学
分泌途径
整体膜蛋白
膜
基因
作者
Li Wang,Fátima-Zahra Idrissi,Martin Hermansson,Alexandra Grippa,Christer S. Ejsing,Pedro Carvalho
标识
DOI:10.1038/s41467-018-05278-2
摘要
Abstract Lipid droplets (LDs) and peroxisomes are ubiquitous organelles with central roles in eukaryotic cells. Although the mechanisms involved in biogenesis of these organelles remain elusive, both seem to require the endoplasmic reticulum (ER). Here we show that in yeast the ER budding of these structurally unrelated organelles has remarkably similar requirements and involves cooperation between Pex30 and the seipin complex. In the absence of these components, budding of both LDs and peroxisomes is inhibited, leading to the ER accumulation of their respective constituent molecules, such as triacylglycerols and peroxisomal membrane proteins, whereas COPII vesicle formation remains unaffected. This phenotype can be reversed by remodeling ER phospholipid composition highlighting a key function of these lipids in organelle biogenesis. We propose that seipin and Pex30 act in concert to organize membrane domains permissive for organelle budding, and that may have a lipid composition distinct from the bulk ER.
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