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The lysosomal lipid transporter LIMP-2 is part of lysosome-ER STARD3-VAPB-dependent contact sites

  • Sönke Rudnik
  • , Saskia Heybrock
  • , Etienne Coyaud
  • , Zizhen Xu
  • , Dante Neculai
  • , Brian Raught
  • , Viola Oorschot
  • , Cecilia Heus
  • , Judith Klumperman
  • , Paul Saftig*
  • *Corresponding author for this work

Research output: Contribution to journalArticleAcademicpeer-review

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Abstract

LIMP-2 (also known as SCARB2) is an abundant lysosomalmembrane protein. Previous studies have shown that LIMP-2 functions as a virus receptor, a chaperone for lysosomal enzyme targeting and a lipid transporter. The large luminal domain of LIMP-2 contains a hydrophobic tunnel that enables transport of phospholipids, sphingosine and cholesterol from the lysosomal lumen to the membrane. The question about the fate of the lipids after LIMP-2- mediated transport is largely unexplored. To elucidate whether LIMP-2 is present at contact sites between lysosomes and the endoplasmic reticulum (ER), we performed a proximity-based interaction screen. This revealed that LIMP-2 interacts with the endosomal protein STARD3 and the ER-resident protein VAPB. Using imaging and co-immunoprecipitation, we demonstrated colocalization and physical interaction between LIMP-2 and these proteins. Moreover, we found that interaction of LIMP-2 with VAPB required the presence of STARD3. Our findings suggest that LIMP-2 is present at ER-lysosome contact sites, possibly facilitating cholesterol transport from the lysosomal to the ER membrane. This suggests a novel mechanism for inter-organelle communication and lipid trafficking mediated by LIMP-2.

Original languageEnglish
Article numberjcs261810
JournalJournal of cell science
Volume137
Issue number22
Early online date7 Oct 2024
DOIs
Publication statusPublished - 15 Nov 2024

Keywords

  • ER-lysosome contact sites
  • Endoplasmic reticulum
  • LIMP-2
  • Lipid transport
  • Lysosome
  • Membrane contact sites
  • SCARB2
  • STARD3
  • VAPB

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