KIF3A binds to beta-arrestin for suppressing Wnt/beta-catenin signalling independently of primary cilia in lung cancer
Aberrant Wnt/beta-catenin signalling is implicated in the progression of several human cancers, including non-small cell lung cancer (NSCLC). However, mutations in Wnt/beta-catenin pathway components are uncommon in NSCLC, and their epigenetic control remains unclear. Here, we show that KIF3A, a member of the kinesin-2 family, plays a role in suppressing Wnt/beta-catenin signalling in NSCLC cells. KIF3A knockdown increases both beta-catenin levels and transcriptional activity with concomitant promotion of malignant potential, such as increased proliferation and migration and upregulation of stemness markers. Because KIF3A binds beta-arrestin, KIF3A depletion allows beta-arrestin to form a complex with DVL2 and axin, stabilizing beta-catenin. Although primary cilia, whose biogenesis requires KIF3A, are thought to restrain the Wnt response, pharmacological inhibition of ciliogenesis failed to increase beta-catenin activity in NSCLC cells. A correlation between KIF3A loss and a poorer NSCLC prognosis as well as beta-catenin and cyclin D1 upregulation further suggests that KIF3A suppresses Wnt/beta-catenin signalling and tumourigenesis in NSCLC
- Publisher
- NATURE PUBLISHING GROUP
- Issue Date
- 2016-09
- Language
- English
- Article Type
- Article
- Keywords
STEM-CELLS; KINESIN SUPERFAMILY; TUMOR INITIATION; TUMORIGENESIS; PATHWAYS; CILIOGENESIS; DISEASE; MEDULLOBLASTOMA; PROGRESSION; MECHANISMS
- Citation
SCIENTIFIC REPORTS, v.6
- ISSN
- 2045-2322
- Appears in Collection
- MSE-Journal Papers(저널논문)
- Files in This Item
- 97035.pdf(2.35 MB)Download
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