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Emma Maxwell
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Journal Articles
Sophia Semerdjieva, Barry Shortt, Emma Maxwell, Sukhdeep Singh, Paul Fonarev, Jonathan Hansen, Giampietro Schiavo, Barth D. Grant, Elizabeth Smythe
Journal:
Journal of Cell Biology
Journal of Cell Biology (2008) 183 (3): 499–511.
Published: 03 November 2008
Abstract
Here we investigate the role of rab5 and its cognate exchange factors rabex-5 and hRME-6 in the regulation of AP2 uncoating from endocytic clathrin-coated vesicles (CCVs). In vitro, we show that the rate of AP2 uncoating from CCVs is dependent on the level of functional rab5. In vivo, overexpression of dominant-negative rab5 S34N , or small interfering RNA (siRNA)–mediated depletion of hRME-6, but not rabex-5, resulted in increased steady-state levels of AP2 associated with endocytic vesicles, which is consistent with reduced uncoating efficiency. hRME-6 guanine nucleotide exchange factor activity requires hRME-6 binding to α-adaptin ear, which displaces the ear-associated μ2 kinase AAK1. siRNA-mediated depletion of hRME-6 increases phospho-μ2 levels, and expression of a phosphomimetic μ2 mutant increases levels of endocytic vesicle-associated AP2. Depletion of hRME-6 or rab5 S35N expression also increases the levels of phosphoinositide 4,5-bisphosphate (PtdIns(4,5)P 2 ) associated with endocytic vesicles. These data are consistent with a model in which hRME-6 and rab5 regulate AP2 uncoating in vivo by coordinately regulating μ2 dephosphorylation and PtdIns(4,5)P 2 levels in CCVs.
Includes: Supplementary data