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Lipid packing defects and membrane charge control RAB GTPase recruitment
Authors:Guillaume Kulakowski  Hugo Bousquet  Jean‐Baptiste Manneville  Patricia Bassereau  Bruno Goud  Lena K. Oesterlin
Affiliation:1. Institut Curie, Paris Sciences et Lettres Research University, Sorbonne Université, CNRS UMR144, Paris, France;2. Laboratoire Physico Chimie, Institut Curie, Paris Sciences et Lettres Research University, Sorbonne Université, CNRS UMR168, Paris, France
Abstract:Specific intracellular localization of RAB GTPases has been reported to be dependent on protein factors, but the contribution of the membrane physicochemical properties to this process has been poorly described. Here, we show that three RAB proteins (RAB1/RAB5/RAB6) preferentially bind in vitro to disordered and curved membranes, and that this feature is uniquely dependent on their prenyl group. Our results imply that the addition of a prenyl group confers to RAB proteins, and most probably also to other prenylated proteins, the ability to sense lipid packing defects induced by unsaturated conical‐shaped lipids and curvature. Consistently, RAB recruitment increases with the amount of lipid packing defects, further indicating that these defects drive RAB membrane targeting. Membrane binding of RAB35 is also modulated by lipid packing defects but primarily dependent on negatively charged lipids. Our results suggest that a balance between hydrophobic insertion of the prenyl group into lipid packing defects and electrostatic interactions of the RAB C‐terminal region with charged membranes tunes the specific intracellular localization of RAB proteins. image
Keywords:curvature sensing  geranylgeranyl  lipid packing defects  membrane order  prenylation
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