Yip3 catalyses the dissociation of endosomal Rab–GDI complexes
- 1 October 2003
- journal article
- letter
- Published by Springer Nature in Nature
- Vol. 425 (6960), 856-859
- https://doi.org/10.1038/nature02057
Abstract
Human cells contain more than 60 small G proteins of the Rab family, which are localized to the surfaces of distinct membrane compartments and regulate transport vesicle formation, motility, docking and fusion1,2,3. Prenylated Rabs also occur in the cytosol bound to GDI4,5 (guanine nucleotide dissociation inhibitor), which binds to Rabs in their inactive state. Prenyl Rab–GDI complexes contain all of the information necessary to direct Rab delivery onto distinct membrane compartments6,7,8. The late endosomal, prenyl Rab9 binds GDI with very high affinity9, which led us to propose that there might be a ‘GDI-displacement factor’ to catalyse dissociation of Rab–GDI complexes and to enable transfer of Rabs from GDI onto membranes6,10. Indeed, we have previously shown that endosomal membranes contain a proteinaceous factor that can act in this manner10. Here we show that the integral membrane protein, Yip3, acts catalytically to dissociate complexes of endosomal Rabs bound to GDI, and to deliver them onto membranes. We propose that the conserved Yip proteins serve as GDI-displacement factors for the targeting of Rab GTPases in eukaryotic cells.Keywords
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