The Dishevelled-associating protein Daple controls the non-canonical Wnt/Rac pathway and cell motility

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Maki Ishida-Takagishi
Atsushi Enomoto
Naoya Asai
Kaori Ushida
Takashi Watanabe
Takahiko Hashimoto
Takuya Kato
Liang Weng
Shinji Matsumoto
Masato Asai
Yoshiki Murakumo
Kozo Kaibuchi
Akira Kikuchi
Masahide Takahashi
机构
[1] Nagoya University Graduate School of Medicine,Department of Pathology
[2] Center for Neurological Disease and Cancer,Division of Molecular Pathology
[3] Nagoya University Graduate School of Medicine,Department of Cell Pharmacology
[4] Nagoya University Graduate School of Medicine,Department of Molecular Biology and Biochemistry
[5] Osaka University Graduate School of Medicine,undefined
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Dishevelled is the common mediator of canonical and non-canonical Wnt signalling pathways, which are important for embryonic development, tissue maintenance and cancer progression. In the non-canonical Wnt signalling pathway, the Rho family of small GTPases acting downstream of Dishevelled has essential roles in cell migration. The mechanisms by which the non-canonical Wnt signalling pathway regulates Rac activation remain unknown. Here we show that Daple (Dishevelled-associating protein with a high frequency of leucine residues) regulates Wnt5a-mediated activation of Rac and formation of lamellipodia through interaction with Dishevelled. Daple increases the association of Dishevelled with an isoform of atypical protein kinase C, consequently promoting Rac activation. Accordingly, Daple deficiency impairs migration of fibroblasts and epithelial cells during wound healing in vivo. These findings indicate that Daple interacts with Dishevelled to direct the Dishevelled/protein kinase λ protein complex to activate Rac, which in turn mediates the non-canonical Wnt signalling pathway required for cell migration.
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