PLoS ONE (Jan 2009)

A-RAF kinase functions in ARF6 regulated endocytic membrane traffic.

  • Elena Nekhoroshkova,
  • Stefan Albert,
  • Matthias Becker,
  • Ulf R Rapp

DOI
https://doi.org/10.1371/journal.pone.0004647
Journal volume & issue
Vol. 4, no. 2
p. e4647

Abstract

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BackgroundRAF kinases direct ERK MAPK signaling to distinct subcellular compartments in response to growth factor stimulation.Methodology/principal findingsOf the three mammalian isoforms A-RAF is special in that one of its two lipid binding domains mediates a unique pattern of membrane localization. Specific membrane binding is retained by an N-terminal fragment (AR149) that corresponds to a naturally occurring splice variant termed DA-RAF2. AR149 colocalizes with ARF6 on tubular endosomes and has a dominant negative effect on endocytic trafficking. Moreover actin polymerization of yeast and mammalian cells is abolished. AR149/DA-RAF2 does not affect the internalization step of endocytosis, but trafficking to the recycling compartment.Conclusions/significanceA-RAF induced ERK activation is required for this step by activating ARF6, as A-RAF depletion or inhibition of the A-RAF controlled MEK-ERK cascade blocks recycling. These data led to a new model for A-RAF function in endocytic trafficking.