Article

  • The EMBO Journal (2008) 27, 956 - 969
  • doi:10.1038/emboj.2008.38

Published online: 6 March 2008

Subversion of CtBP1-controlled macropinocytosis by human adenovirus serotype 3

Beat Amstutz1, Michele Gastaldelli1, Stefan Kälin1, Nicola Imelli1, Karin Boucke1, Eliane Wandeler1, Jason Mercer2, Silvio Hemmi3 and Urs F Greber1

  1. Institute of Zoology, University of Zürich, Zürich, Switzerland
  2. Institute of Biochemistry, ETH Zürich, Zürich, Switzerland
  3. Institute of Molecular Biology, University of Zürich, Zürich, Switzerland

Correspondence to:

Urs F Greber, Institute of Zoology, University of Zuerich, Winterthurerstrasse 190, CH-8057 Zurich, Switzerland. Tel.: +41 44 635 4841; Fax: +41 44 635 6822; E-mail: ufgreber@zool.unizh.ch

Received 22 August 2007; Accepted 13 February 2008


Endocytosis supports cell communication, growth, and pathogen infection. The species B human adenovirus serotype 3 (Ad3) is associated with epidemic conjunctivitis, and fatal respiratory and systemic disease. Here we show that Ad3 uses dynamin-independent endocytosis for rapid infectious entry into epithelial and haematopoietic cells. Unlike Ad5, which uses dynamin-dependent endocytosis, Ad3 endocytosis spatially and temporally coincided with enhanced fluid-phase uptake. It was sensitive to macropinocytosis inhibitors targeting F-actin, protein kinase C, the sodium–proton exchanger, and Rac1 but not Cdc42. Infectious Ad3 macropinocytosis required viral activation of p21-activated kinase 1 (PAK1) and the C-terminal binding protein 1 of E1A (CtBP1), recruited to macropinosomes. These macropinosomes also contained the Ad3 receptors CD46 and alphav integrins. CtBP1 is a phosphorylation target of PAK1, and is bifunctionally involved in membrane traffic and transcriptional repression of cell cycle, cancer, and innate immunity pathways. Phosphorylation-defective S147A-CtBP1 blocked Ad3 but not Ad5 infection, providing a direct link between PAK1 and CtBP1. The data show that viruses induce macropinocytosis for infectious entry, a pathway used in antigen presentation and cell migration.

  • Keywords:

    • cell defence,
    • endocytosis,
    • infectious disease,
    • innate immunity,
    • transcription
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