| Literature DB >> 31178403 |
Veijo T Salo1, Shiqian Li1, Helena Vihinen2, Maarit Hölttä-Vuori1, Abel Szkalisity3, Peter Horvath3, Ilya Belevich2, Johan Peränen1, Christoph Thiele4, Pentti Somerharju5, Hongxia Zhao2, Alexandre Santinho6, Abdou Rachid Thiam7, Eija Jokitalo8, Elina Ikonen9.
Abstract
Seipin is an oligomeric integral endoplasmic reticulum (ER) protein involved in lipid droplet (LD) biogenesis. To study the role of seipin in LD formation, we relocalized it to the nuclear envelope and found that LDs formed at these new seipin-defined sites. The sites were characterized by uniform seipin-mediated ER-LD necks. At low seipin content, LDs only grew at seipin sites, and tiny, growth-incompetent LDs appeared in a Rab18-dependent manner. When seipin was removed from ER-LD contacts within 1 h, no lipid metabolic defects were observed, but LDs became heterogeneous in size. Studies in seipin-ablated cells and model membranes revealed that this heterogeneity arises via a biophysical ripening process, with triglycerides partitioning from smaller to larger LDs through droplet-bilayer contacts. These results suggest that seipin supports the formation of structurally uniform ER-LD contacts and facilitates the delivery of triglycerides from ER to LDs. This counteracts ripening-induced shrinkage of small LDs.Entities:
Keywords: auxin-induced degradation; correlative light electron microscopy; electron tomography; lipid trafficking; lipogenesis; membrane contacts; model membranes; neutral lipid; organelle biogenesis; triglyceride
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Year: 2019 PMID: 31178403 DOI: 10.1016/j.devcel.2019.05.016
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 12.270