Transport of LDL-derived cholesterol from the NPC1 compartment to the ER involves the trans-Golgi network and the SNARE protein complex

Urano, Yasuomi; Watanabe, Hiroshi; Murphy, Stephanie R; Shibuya, Yohei; Geng, Yong; Peden, Andrew A.; Chang, Catherine C.Y.; Chang, Ta Yuan

doi:10.1073/pnas.0807450105

Cited by 105 publications

(136 citation statements)

References 51 publications

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“…ORP9L depletion did not affect ER cholesterol homeostatic responses, potentially indicating no change in ER cholesterol content, but significantly increased cholesterol deposition in the endosomal/lysosomal compartment, as measure by filipin binding (Figure 8). The TGN is an important delivery site for endocytosed cholesterol (Urano et al, 2008) that, in the absence of ORP9L, appeared to backup into the endosomes and lysosomes. This suggests that ORP9L maintains cholesterol flux from the endosomal pathway to the transGolgi/TGN by transferring cholesterol to the ER or other organelles.…”

Section: Discussionmentioning

confidence: 99%

Oxysterol Binding Protein–related Protein 9 (ORP9) Is a Cholesterol Transfer Protein That Regulates Golgi Structure and Function

Ngo

Ridgway

2009

MBoC

157

193

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Oxysterol-binding protein (OSBP) and OSBP-related proteins (ORPs) constitute a large gene family that differentially localize to organellar membranes, reflecting a functional role in sterol signaling and/or transport. OSBP partitions between the endoplasmic reticulum (ER) and Golgi apparatus where it imparts sterol-dependent regulation of ceramide transport and sphingomyelin synthesis. ORP9L also is localized to the ER-Golgi, but its role in secretion and lipid transport is unknown. Here we demonstrate that ORP9L partitioning between the trans-Golgi/trans-Golgi network (TGN), and the ER is mediated by a phosphatidylinositol 4-phosphate (PI-4P)-specific PH domain and VAMP-associated protein (VAP), respectively. In vitro, both OSBP and ORP9L mediated PI-4P-dependent cholesterol transport between liposomes, suggesting their primary in vivo function is sterol transfer between the Golgi and ER. Depletion of ORP9L by RNAi caused Golgi fragmentation, inhibition of vesicular somatitus virus glycoprotein transport from the ER and accumulation of cholesterol in endosomes/lysosomes. Complete cessation of protein transport and cell growth inhibition was achieved by inducible overexpression of ORP9S, a dominant negative variant lacking the PH domain. We conclude that ORP9 maintains the integrity of the early secretory pathway by mediating transport of sterols between the ER and trans-Golgi/TGN. INTRODUCTIONThe Golgi apparatus is a highly compartmentalized organelle that serves as a nexus for the processing, sorting, and vesicular transport of protein and lipid cargo between organelles. Regulation of vesicular transport is dependent on coat proteins and factors that control coat assembly/disassembly, as well as membrane dynamics and individual lipid regulators. A continuing challenge is the identification of the proteins responsible for spatial generation of Golgi lipid regulators by localized synthesis and/or transport (Huijbregts et al., 2000;De Matteis et al., 2007). In this study we investigated one such lipid-binding protein, oxysterol-binding protein (OSBP)-related protein 9 (ORP9), and its role in endoplasmic reticulum (ER)-to-Golgi transport.Lipid synthesis and transport to the Golgi apparatus regulates local and distal cellular functions. For example, synthesis of sphingomyelin (SM) and glycosphingolipids (Huitema et al., 2004) in combination with cholesterol is required for raft assembly in the Golgi and cargo delivery to the apical surface of polarized cells (Hoekstra et al., 2003). SM synthesis in the Golgi apparatus is dependent on delivery of ceramide from the ER by the ceramide transfer protein (CERT; Hanada et al., 2003). Ceramide transport by CERT involves binding of a phosphatidylinositol 4-phosphate (PI-4P)-specific pleckstrin homology (PH) domain to the Golgi apparatus and interaction with vesicle-associated membrane protein (VAMP)-associated-protein (VAP) by the "two phenylalanines in an acidic tract" (FFAT) motif (Hanada et al., 2003). In addition, CERT activates protein kinase D activity and secretory t...

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Section: Discussionmentioning

confidence: 99%

Oxysterol Binding Protein–related Protein 9 (ORP9) Is a Cholesterol Transfer Protein That Regulates Golgi Structure and Function

Ngo

Ridgway

2009

MBoC

157

193

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“…The majority of late-endosome-derived cholesterol is then delivered to the plasma membrane, while some of it is transported to the ER to enable feedback control or undergoes esterification for storage in lipid droplets in the form of cholesteryl esters. The routes and mechanisms by which late endosome-originating cholesterol reaches the plasma membrane are not clear, but as shown by our laboratory (Cubells et al, 2007;Reverter et al, 2014) and others (Kanerva et al, 2013;Urano et al, 2008), might involve transport through the ER, the transGolgi network (TGN) and recycling endosomes (Fig. 1A).…”

Section: Intracellular Trafficking Of Cholesterolmentioning

confidence: 99%

“…Niemann Pick C1 protein (NPC1) and Niemann Pick type C2 protein homolog (NPC2) bind to late-endosome-associated cholesterol and facilitate its export from late endosomes (Ikonen, 2006;Vance and Karten, 2014). Mutations in the genes encoding NPC1 or NPC2 inhibit the egress of cholesterol from late endosomes (Klein et al, 2006) and reduce its delivery to the Golgi, plasma membrane and recycling endosomes (Cubells et al, 2007;Kanerva et al, 2013;Reverter et al, 2014;Urano et al, 2008). Together, this triggers a dysfunction of membrane trafficking, which is associated with cardiovascular, neurological and lysosomal storage diseases (Cortes et al, 2013;De Matteis and Luini, 2011;Ikonen, 2006;Maxfield and Tabas, 2005).…”

Section: Intracellular Trafficking Of Cholesterolmentioning

confidence: 99%

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Role of cholesterol in SNARE-mediated trafficking on intracellular membranes

Enrich

Rentero

Hierro

et al. 2015

Journal of Cell Science

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The cell surface delivery of extracellular matrix (ECM) and integrins is fundamental for cell migration in wound healing and during cancer cell metastasis. This process is not only driven by several soluble NSF attachment protein (SNAP) receptor (SNARE) proteins, which are key players in vesicle transport at the cell surface and intracellular compartments, but is also tightly modulated by cholesterol. Cholesterol-sensitive SNAREs at the cell surface are relatively well characterized, but it is less well understood how altered cholesterol levels in intracellular compartments impact on SNARE localization and function. Recent insights from structural biology, protein chemistry and cell microscopy have suggested that a subset of the SNAREs engaged in exocytic and retrograde pathways dynamically 'sense' cholesterol levels in the Golgi and endosomal membranes. Hence, the transport routes that modulate cellular cholesterol distribution appear to trigger not only a change in the location and functioning of SNAREs at the cell surface but also in endomembranes. In this Commentary, we will discuss how disrupted cholesterol transport through the Golgi and endosomal compartments ultimately controls SNARE-mediated delivery of ECM and integrins to the cell surface and, consequently, cell migration.

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“…Next, we asked whether endosome-to-mitochondria movement of cholesterol required additional, cytosolic carrier proteins and/ or passage through other subcellular membranes, such as ER or plasma membrane. To address these questions, we used CHO-F2 cells that were semi-permeabilized to remove cytosolic proteins following a protocol that was used previously to investigate endosome-to-trans Golgi cholesterol traffi cking ( 34 ). Treatment with 20 µg/ml digitonin permeabilized the plasma membrane of 90% of cells, as shown by the uptake of Trypan blue ( Fig.…”

Section: Endosomal Cholesterol Reaches the Mitochondrial Inner Membramentioning

confidence: 99%

Niemann-Pick Type C2 protein contributes to the transport of endosomal cholesterol to mitochondria without interacting with NPC1

Kennedy

Charman

Karten

2012

Journal of Lipid Research

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Transport of LDL-derived cholesterol from the NPC1 compartment to the ER involves the trans-Golgi network and the SNARE protein complex

Cited by 105 publications

References 51 publications

Oxysterol Binding Protein–related Protein 9 (ORP9) Is a Cholesterol Transfer Protein That Regulates Golgi Structure and Function

Oxysterol Binding Protein–related Protein 9 (ORP9) Is a Cholesterol Transfer Protein That Regulates Golgi Structure and Function

Role of cholesterol in SNARE-mediated trafficking on intracellular membranes

Niemann-Pick Type C2 protein contributes to the transport of endosomal cholesterol to mitochondria without interacting with NPC1

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