Article

  • The EMBO Journal (2009) 28, 1197 - 1207
  • doi:10.1038/emboj.2009.78

Published online: 26 March 2009

CtBP1/BARS is an activator of phospholipase D1 necessary for agonist-induced macropinocytosisEMBO Open

Yuki Haga1,a, Noriko Miwa1,a, Saleem Jahangeer1, Taro Okada1 and Shun-ichi Nakamura1

  1. Division of Biochemistry, Department of Molecular and Cellular Biology, Kobe University Graduate School of Medicine, Kobe, Japan

Correspondence to:

Shun-ichi Nakamura, Division of Biochemistry, Department of Molecular and Cellular Biology, Kobe University Graduate School of Medicine, Kobe 650-0017, Japan. Tel.: +81 78 382 5420; Fax: +81 78 382 5439; E-mail: snakamur@kobe-u.ac.jp

aThese authors contributed equally to this work

Received 17 September 2008; Accepted 26 February 2009


Vesicular trafficking such as macropinocytosis is a dynamic process that requires coordinated interactions between specialized proteins and lipids. A recent report suggests the involvement of CtBP1/BARS in epidermal growth factor (EGF)-induced macropinocytosis. Detailed mechanisms as to how lipid remodelling is regulated during macropinocytosis are still undefined. Here, we show that CtBP1/BARS is a physiological activator of PLD1 required in agonist-induced macropinocytosis. EGF-induced macropinocytosis was specifically blocked by 1-butanol but not by 2-butanol. In addition, stimulation of cells by serum or EGF resulted in the association of CtBP1/BARS with PLD1. Finally, CtBP1/BARS activated PLD1 in a synergistic manner with other PLD activators, including ADP-ribosylation factors as demonstrated by in vitro and intact cell systems. The present results shed light on the molecular basis of how the 'fission protein' CtBP1/BARS controls vesicular trafficking events including macropinocytosis.

  • Keywords:

    • CtBP1/BARS,
    • macropinocytosis,
    • phospholipase D

This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits distribution, and reproduction in any medium, provided the original author and source are credited. This license does not permit commercial exploitation or the creation of derivative works without specific permission.

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