Triacylglycerols sequester monotopic membrane proteins to lipid droplets

Caillon, Lucie; Nieto, Vincent; Gehan, Pauline; Omrane, Mohyeddine; Rodriguez, Nicolas; Monticelli, Luca; Thiam, Abdou Rachid

doi:10.1038/s41467-020-17585-8

Cited by 61 publications

(63 citation statements)

References 70 publications

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“…Additionally, in yeast genetic backgrounds that support the formation of supersized LDs (such as ∆sei1 ∆pln1), the absence of ER-localized Psd1 may reduce the PE levels on the LD surface monolayer, attenuating the ability of small LDs to fuse with one another and generate supersized LDs (Fei et al, 2011). A non-mutually exclusive possibility is that altered PC/PE ratios at the ER in PSD-deficient cells influences LD protein targeting, which feeds back into influencing LD biogenesis or expansion (Caillon et al, 2020).…”

Section: Discussionmentioning

confidence: 99%

ER-localized phosphatidylethanolamine synthase plays a conserved role in lipid droplet formation

Gok

Speer

Friedman

2022

MBoC

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The asymmetric distribution of phospholipids in membranes is a fundamental principle of cellular compartmentalization and organization. Phosphatidylethanolamine (PE), a nonbilayer phospholipid that contributes to organelle shape and function, is synthesized at several subcellular localizations via semi-redundant pathways. Previously, we demonstrated in budding yeast that the PE synthase Psd1, which primarily operates on the mitochondrial inner membrane, is additionally targeted to the ER. While ER-localized Psd1 is required to support cellular growth in the absence of redundant pathways, its physiological function is unclear. We now demonstrate that ER-localized Psd1 sub-localizes on the ER to lipid droplet (LD) attachment sites and show it is specifically required for normal LD formation. We also find that the role of phosphatidylserine decarboxylase (PSD) enzymes in LD formation is conserved in other organisms. Thus, we have identified PSD enzymes as novel regulators of LDs and demonstrate that both mitochondria and LDs in yeast are organized and shaped by the spatial positioning of a single PE synthesis enzyme.

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Section: Discussionmentioning

confidence: 99%

ER-localized phosphatidylethanolamine synthase plays a conserved role in lipid droplet formation

Gok

Speer

Friedman

2022

MBoC

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“…Hence, LD biogenesis at the ER results in the formation of a hydrophobic oil phase surrounded by a phospholipid monolayer derived from the cytosolic leaflet of the ER. Such an architecture distinguishes LDs from other intracellular membrane-enveloped organelles, which are surrounded by phospholipid bilayers, and has profound consequences for phospholipid packing and protein localisation to LDs ( Caillon et al, 2020 ; Dhiman et al, 2020 ; Kory et al, 2015 ; Krahmer et al, 2011 ; Olarte et al, 2020 ).…”

Section: Introductionmentioning

confidence: 99%

Co-translational biogenesis of lipid droplet integral membrane proteins

Leznicki

Schneider

Harvey

et al. 2021

Journal of Cell Science

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Membrane proteins destined for lipid droplets (LDs), a major intracellular storage site for neutral lipids, are inserted into the endoplasmic reticulum (ER) and then trafficked to LDs where they reside in a hairpin loop conformation. Here, we show that LD membrane proteins can be delivered to the ER either co- or post-translationally and that their membrane-embedded region specifies pathway selection. The co-translational route for LD membrane protein biogenesis is insensitive to a small molecule inhibitor of the Sec61 translocon, Ipomoeassin F, and instead relies on the ER membrane protein complex (EMC) for membrane insertion. This route may even result in a transient exposure of the short N-termini of some LD membrane proteins to the ER lumen, followed by putative topological rearrangements that would enable their transmembrane segment to form a hairpin loop and N-termini to face the cytosol. Our study reveals an unexpected complexity to LD membrane protein biogenesis and identifies a role for the EMC during their co-translational insertion into the ER.

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“…As such, Type I LD proteins can translocate between the ER and LD monolayer via lipidic bridges connecting the two organelles (Wilfling et al, 2013). Elegant in vitro studies have suggested that LD localization promotes energetically favorable conformational changes within some proteins, and the movement of proteins to LDs from the ER network can even influence their enzymatic activities, or modulate their degradation (Caillon et al, 2020), (Chorlay and Thiam, 2020), (Leber et al, 1998), (Schmidt et al, 2013), (Ohsaki et al, 2006). A second mechanism of LD targeting occurs from the cytoplasm, where soluble proteins insert into the LD monolayer via a hydrophobic region, amphipathic helix, or lipid moiety.…”

Section: Introductionmentioning

confidence: 99%

Liquid-crystalline lipid phase transitions in lipid droplets selectively remodel the LD proteome

Rogers

Gui

Kovalenko

et al. 2021

Preprint

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Lipid droplets (LDs) are reservoirs for triglycerides (TGs) and sterol-esters (SEs). How lipids are organized within LDs and influence the LD proteome remains unclear. Using in situ cryo-electron tomography, we show that glucose restriction triggers lipid phase transitions within LDs generating liquid-crystalline lattices inside them. Mechanistically, this requires TG lipolysis, which alters LD neutral lipid composition and promotes SE transition to a liquid-crystalline phase. Fluorescence imaging and proteomics further reveal that LD liquid-crystalline lattices selectively remodel the LD proteome. Some canonical LD proteins including Erg6 re-localize to the ER network, whereas others remain on LDs. Model peptide LiveDrop also redistributes from LDs to the ER, suggesting liquid-crystalline-phases influence ER-LD inter-organelle transport. Proteomics also indicates glucose restriction elevates peroxisome lipid oxidation, suggesting TG mobilization provides fatty acids for cellular energetics. This suggests glucose restriction drives TG mobilization, which alters the phase properties of LD lipids and selectively remodels the LD proteome.

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Triacylglycerols sequester monotopic membrane proteins to lipid droplets

Cited by 61 publications

References 70 publications

ER-localized phosphatidylethanolamine synthase plays a conserved role in lipid droplet formation

ER-localized phosphatidylethanolamine synthase plays a conserved role in lipid droplet formation

Co-translational biogenesis of lipid droplet integral membrane proteins

Liquid-crystalline lipid phase transitions in lipid droplets selectively remodel the LD proteome

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