Wnt signalling pathway parameters for mammalian cells

C.W. Tan; B.S. Gardiner; Y. Hirokawa; M.J. Layton; D.W. Smith; A.W. Burgess

doi:10.1371/journal.pone.0031882

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Wnt signalling pathway parameters for mammalian cells

Journal article

Open access

Peer reviewed

Wnt signalling pathway parameters for mammalian cells

C.W. Tan, B.S. Gardiner, Y. Hirokawa, M.J. Layton, D.W. Smith and A.W. Burgess

PloS one, Vol.7(2)

2012

DOI: https://doi.org/10.1371/journal.pone.0031882

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Abstract

Wnt/β-catenin signalling regulates cell fate, survival, proliferation and differentiation at many stages of mammalian development and pathology. Mutations of two key proteins in the pathway, APC and β-catenin, have been implicated in a range of cancers, including colorectal cancer. Activation of Wnt signalling has been associated with the stabilization and nuclear accumulation of β-catenin and consequential up-regulation of β-catenin/TCF gene transcription. In 2003, Lee et al. constructed a computational model of Wnt signalling supported by experimental data from analysis of time-dependent concentration of Wnt signalling proteins in Xenopus egg extracts. Subsequent studies have used the Xenopus quantitative data to infer Wnt pathway dynamics in other systems. As a basis for understanding Wnt signalling in mammalian cells, a confocal live cell imaging measurement technique is developed to measure the cell and nuclear volumes of MDCK, HEK293T cells and 3 human colorectal cancer cell lines and the concentrations of Wnt signalling proteins β-catenin, Axin, APC, GSK3β and E-cadherin. These parameters provide the basis for formulating Wnt signalling models for kidney/intestinal epithelial mammalian cells. There are significant differences in concentrations of key proteins between Xenopus extracts and mammalian whole cell lysates. Higher concentrations of Axin and lower concentrations of APC are present in mammalian cells. Axin concentrations are greater than APC in kidney epithelial cells, whereas in intestinal epithelial cells the APC concentration is higher than Axin. Computational simulations based on Lee's model, with this new data, suggest a need for a recalibration of the model. A quantitative understanding of Wnt signalling in mammalian cells, in particular human colorectal cancers requires a detailed understanding of the concentrations of key protein complexes over time. Simulations of Wnt signalling in mammalian cells can be initiated with the parameters measured in this report.

Details

Title: Wnt signalling pathway parameters for mammalian cells
Authors/Creators: C.W. Tan (Author/Creator) - Ludwig Cancer Research
B.S. Gardiner (Author/Creator) - The University of Western Australia
Y. Hirokawa (Author/Creator) - Ludwig Cancer Research
M.J. Layton (Author/Creator) - Ludwig Institute for Cancer Research, Melbourne-Parkville Branch, Parkville, Victoria, Australia
D.W. Smith (Author/Creator) - The University of Western Australia
A.W. Burgess (Author/Creator) - Ludwig Cancer Research
Publication Details: PloS one, Vol.7(2)
Publisher: Public Library of Science
Identifiers: 991005540255007891
Copyright: © 2012 Tan et al.
Murdoch Affiliation: Murdoch University
Language: English
Resource Type: Journal article

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Collaboration types: Domestic collaboration
Citation topics: 1 Clinical & Life Sciences; 1.108 Molecular & Cell Biology - Cancer & Development; 1.108.757 Wnt-Cadherin Interactions
Web Of Science research areas: Cell Biology
ESI research areas: Molecular Biology & Genetics