V-ATPase interacts with ARNO and Arf6 in early endosomes and regulates the protein degradative pathw

Author:  ["Andrés Hurtado-Lorenzo","Mhairi Skinner","Jaafar El Annan","Masamitsu Futai","Ge-Hong Sun-Wada","Sylvain Bourgoin","James Casanova","Alan Wildeman","Shaliha Bechoua","Dennis A. Ausiello","Dennis Brown","Vladimir Marshansky"]

Publication:  Nature Cell Biology

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Tags:  general   CellBiology   CancerResearch   DevelopmentalBiology   StemCells   Biological

Abstract

The recruitment of the small GTPase Arf6 and ARNO from cytosol to endosomal membranes is driven by V-ATPase-dependent intra-endosomal acidification. The molecular mechanism that mediates this pH-sensitive recruitment and its role are unknown. Here, we demonstrate that Arf6 interacts with the c-subunit, and ARNO with the a2-isoform of V-ATPase. The a2-isoform is targeted to early endosomes, interacts with ARNO in an intra-endosomal acidification-dependent manner, and disruption of this interaction results in reversible inhibition of endocytosis. Inhibition of endosomal acidification abrogates protein trafficking between early and late endosomal compartments. These data demonstrate the crucial role of early endosomal acidification and V-ATPase/ARNO/Arf6 interactions in the regulation of the endocytic degradative pathway. They also indicate that V-ATPase could modulate membrane trafficking by recruiting and interacting with ARNO and Arf6; characteristics that are consistent with the role of V-ATPase as an essential component of the endosomal pH-sensing machinery.

Cite this article

Hurtado-Lorenzo, A., Skinner, M., Annan, J. et al. V-ATPase interacts with ARNO and Arf6 in early endosomes and regulates the protein degradative pathway. Nat Cell Biol 8, 124–136 (2006). https://doi.org/10.1038/ncb1348

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