An alternative membrane topology permits lipid droplet localization of peroxisomal fatty acyl-CoA reductase 1

Author:

Exner Tarik,Romero-Brey Inés,Yifrach Eden,Rivera-Monroy Jhon,Schrul Bianca,Zouboulis Christos C.,Stremmel Wolfgang,Honsho Masanori,Bartenschlager Ralf,Zalckvar Einat,Poppelreuther Margarete,Füllekrug JoachimORCID

Abstract

AbstractFatty acyl-CoA reductase 1 (Far1) is an ubiquitously expressed peroxisomal membrane protein generating fatty alcohols required for the biosynthesis of ether lipids.Lipid droplet localization of human Far1 was observed by fluorescence microscopy under conditions of increased triglyceride synthesis in tissue culture cells. This unexpected finding was supported further by correlative light electron microscopy and subcellular fractionation. Selective permeabilization and N-glycosylation tagging suggest that Far1 is able to assume two different membrane topologies, differing in the orientation of the short hydrophilic C-terminus towards the lumen or the cytosol, respectively. Two closely spaced hydrophobic domains are contained within the C-terminal region. When analyzed separately, the second domain was sufficient for the localization of a fluorescent reporter to lipid droplets. Targeting of Far1 to lipid droplets was not impaired in either pex19 or TRC40/ASNA1 CRISPR/Cas9 knockout cells.In conclusion, our data suggest that Far1 is a novel member of the rather exclusive group of dual topology membrane proteins. At the same time, Far1 shows lipid metabolism-dependent differential subcellular localizations to peroxisomes and lipid droplets.

Publisher

Cold Spring Harbor Laboratory

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