Tumour cell-derived Wnt7a recruits and activates fibroblasts to promote tumour aggressiveness.
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Date
2016-01-18Author
Avgustinova, A
Iravani, M
Robertson, D
Fearns, A
Gao, Q
Klingbeil, P
Hanby, AM
Speirs, V
Sahai, E
Calvo, F
Isacke, CM
Type
Journal Article
Metadata
Show full item recordAbstract
Stromal fibroblast recruitment to tumours and activation to a cancer-associated fibroblast (CAF) phenotype has been implicated in promoting primary tumour growth and progression to metastatic disease. However, the mechanisms underlying the tumour:fibroblast crosstalk that drive the intertumoural stromal heterogeneity remain poorly understood. Using in vivo models we identify Wnt7a as a key factor secreted exclusively by aggressive breast tumour cells, which induces CAF conversion. Functionally, this results in extracellular matrix remodelling to create a permissive environment for tumour cell invasion and promotion of distant metastasis. Mechanistically, Wnt7a-mediated fibroblast activation is not dependent on classical Wnt signalling. Instead, we demonstrate that Wnt7a potentiates TGFβ receptor signalling both in 3D in vitro and in vivo models, thus highlighting the interaction between two of the key signalling pathways in development and disease. Importantly, in clinical breast cancer cohorts, tumour cell Wnt7a expression correlates with a desmoplastic, poor-prognosis stroma and poor patient outcome.
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Subject
NIH 3T3 Cells
Fibroblasts
Animals
Mice, Inbred BALB C
Humans
Mice
Breast Neoplasms
Gene Expression Regulation, Neoplastic
Female
Wnt Proteins
Research team
Molecular Cell Biology
Tumour Microenvironment
Language
eng
Date accepted
2015-11-27
License start date
2016-01-18
Citation
Nature communications, 2016, 7 pp. 10305 - ?
Publisher
NATURE PUBLISHING GROUP