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Literature DB >> 26126266

Daple is a novel non-receptor GEF required for trimeric G protein activation in Wnt signaling.

Nicolas Aznar¹, Krishna K Midde¹, Ying Dunkel¹, Inmaculada Lopez-Sanchez¹, Yelena Pavlova¹, Arthur Marivin², Jorge Barbazán³, Fiona Murray¹, Ulrich Nitsche⁴, Klaus-Peter Janssen⁴, Karl Willert⁵, Ajay Goel⁶, Miguel Abal³, Mikel Garcia-Marcos², Pradipta Ghosh¹.

Abstract

Wnt signaling is essential for tissue homeostasis and its dysregulation causes cancer. Wnt ligands trigger signaling by activating Frizzled receptors (FZDRs), which belong to the G-protein coupled receptor superfamily. However, the mechanisms of G protein activation in Wnt signaling remain controversial. In this study, we demonstrate that FZDRs activate G proteins and trigger non-canonical Wnt signaling via the Dishevelled-binding protein, Daple. Daple contains a Gα-binding and activating (GBA) motif, which activates Gαi proteins and an adjacent domain that directly binds FZDRs, thereby linking Wnt stimulation to G protein activation. This triggers non-canonical Wnt responses, that is, suppresses the β-catenin/TCF/LEF pathway and tumorigenesis, but enhances PI3K-Akt and Rac1 signals and tumor cell invasiveness. In colorectal cancers, Daple is suppressed during adenoma-to-carcinoma transformation and expressed later in metastasized tumor cells. Thus, Daple activates Gαi and enhances non-canonical Wnt signaling by FZDRs, and its dysregulation can impact both tumor initiation and progression to metastasis.

Entities: Disease Gene

Keywords: G proteins; GEF; PI3K/Akt; Rac1; biophysics; cell biology; human; structural biology; tumor suppressor

Mesh：

Substances：

Year: 2015 PMID： 26126266 PMCID： PMC4484057 DOI： 10.7554/eLife.07091

Source DB: PubMed Journal: Elife ISSN： 2050-084X Impact factor: 8.140

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