Proteomics

Dataset Information

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A trimeric Rab7 GEF controls NPC1-dependent lysosomal cholesterol export


ABSTRACT: Cholesterol import in mammalian cells is mediated by the LDL receptor pathway. Here, we perform a genome-wide CRISPR screen using an endogenous cholesterol reporter and identify >100 genes involved in LDL-cholesterol import. We characterise C18orf8 as a core subunit of the mammalian Mon1-Ccz1 guanidine exchange factor (GEF) for Rab7, required for complex stability and function. C18orf8-deficient cells lack Rab7 activation and show severe defects in late endosome morphology and endosomal LDL trafficking, resulting in cellular cholesterol deficiency. Unexpectedly, free cholesterol accumulates within swollen lysosomes, suggesting a critical defect in lysosomal cholesterol export. We find that active Rab7 interacts with the NPC1 cholesterol transporter and licenses lysosomal cholesterol export. This process is abolished in C18orf8-, Ccz1- and Mon1A/B-deficient cells and restored by a constitutively active Rab7. The trimeric Mon1-Ccz1-C18orf8 (MCC) GEF therefore plays a central role in cellular cholesterol homeostasis coordinating Rab7 activation, endosomal LDL trafficking and NPC1-dependent lysosomal cholesterol export.

INSTRUMENT(S): Orbitrap Fusion

ORGANISM(S): Homo Sapiens (human)

TISSUE(S): Epithelial Cell

DISEASE(S): Niemann-pick Disease

SUBMITTER: James Williamson  

LAB HEAD: Paul Lehner

PROVIDER: PXD021444 | Pride | 2020-10-29

REPOSITORIES: Pride

Dataset's files

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Action DRS
PJL-DVB_1705_C18orf8-HA_IP-1.mzML Mzml
PJL-DVB_1705_C18orf8-HA_IP-1.mzid.gz Mzid
PJL-DVB_1705_C18orf8-HA_IP.raw Raw
PJL-DVB_1705_HA-C18orf8_IP-1.mzML Mzml
PJL-DVB_1705_HA-C18orf8_IP-1.mzid.gz Mzid
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Publications

A trimeric Rab7 GEF controls NPC1-dependent lysosomal cholesterol export.

van den Boomen Dick J H DJH   Sienkiewicz Agata A   Berlin Ilana I   Jongsma Marlieke L M MLM   van Elsland Daphne M DM   Luzio J Paul JP   Neefjes Jacques J C JJC   Lehner Paul J PJ  

Nature communications 20201103 1


Cholesterol import in mammalian cells is mediated by the LDL receptor pathway. Here, we perform a genome-wide CRISPR screen using an endogenous cholesterol reporter and identify >100 genes involved in LDL-cholesterol import. We characterise C18orf8 as a core subunit of the mammalian Mon1-Ccz1 guanidine exchange factor (GEF) for Rab7, required for complex stability and function. C18orf8-deficient cells lack Rab7 activation and show severe defects in late endosome morphology and endosomal LDL traf  ...[more]

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