The role of the Hes1 crosstalk hub in Notch-Wnt interactions of the intestinal crypt

The Notch pathway plays a vital role in determining whether cells in the intestinal epithelium adopt a secretory or an absorptive phenotype. Cell fate specification is coordinated via Notch’s interaction with the canonical Wnt pathway. Here, we propose a new mathematical model of the Notch and Wnt p...

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Autores principales: Kay, Sophie K., Harrington, Heather A., Shepherd, Sarah, Brennan, Keith, Dale, Trevor, Osborne, James M., Gavaghan, David J., Byrne, Helen M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5363986/
https://www.ncbi.nlm.nih.gov/pubmed/28245235
http://dx.doi.org/10.1371/journal.pcbi.1005400
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author Kay, Sophie K.
Harrington, Heather A.
Shepherd, Sarah
Brennan, Keith
Dale, Trevor
Osborne, James M.
Gavaghan, David J.
Byrne, Helen M.
author_facet Kay, Sophie K.
Harrington, Heather A.
Shepherd, Sarah
Brennan, Keith
Dale, Trevor
Osborne, James M.
Gavaghan, David J.
Byrne, Helen M.
author_sort Kay, Sophie K.
collection PubMed
description The Notch pathway plays a vital role in determining whether cells in the intestinal epithelium adopt a secretory or an absorptive phenotype. Cell fate specification is coordinated via Notch’s interaction with the canonical Wnt pathway. Here, we propose a new mathematical model of the Notch and Wnt pathways, in which the Hes1 promoter acts as a hub for pathway crosstalk. Computational simulations of the model can assist in understanding how healthy intestinal tissue is maintained, and predict the likely consequences of biochemical knockouts upon cell fate selection processes. Chemical reaction network theory (CRNT) is a powerful, generalised framework which assesses the capacity of our model for monostability or multistability, by analysing properties of the underlying network structure without recourse to specific parameter values or functional forms for reaction rates. CRNT highlights the role of β-catenin in stabilising the Notch pathway and damping oscillations, demonstrating that Wnt-mediated actions on the Hes1 promoter can induce dynamic transitions in the Notch system, from multistability to monostability. Time-dependent model simulations of cell pairs reveal the stabilising influence of Wnt upon the Notch pathway, in which β-catenin- and Dsh-mediated action on the Hes1 promoter are key in shaping the subcellular dynamics. Where Notch-mediated transcription of Hes1 dominates, there is Notch oscillation and maintenance of fate flexibility; Wnt-mediated transcription of Hes1 favours bistability akin to cell fate selection. Cells could therefore regulate the proportion of Wnt- and Notch-mediated control of the Hes1 promoter to coordinate the timing of cell fate selection as they migrate through the intestinal epithelium and are subject to reduced Wnt stimuli. Furthermore, mutant cells characterised by hyperstimulation of the Wnt pathway may, through coupling with Notch, invert cell fate in neighbouring healthy cells, enabling an aberrant cell to maintain its neighbours in mitotically active states.
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spelling pubmed-53639862017-04-06 The role of the Hes1 crosstalk hub in Notch-Wnt interactions of the intestinal crypt Kay, Sophie K. Harrington, Heather A. Shepherd, Sarah Brennan, Keith Dale, Trevor Osborne, James M. Gavaghan, David J. Byrne, Helen M. PLoS Comput Biol Research Article The Notch pathway plays a vital role in determining whether cells in the intestinal epithelium adopt a secretory or an absorptive phenotype. Cell fate specification is coordinated via Notch’s interaction with the canonical Wnt pathway. Here, we propose a new mathematical model of the Notch and Wnt pathways, in which the Hes1 promoter acts as a hub for pathway crosstalk. Computational simulations of the model can assist in understanding how healthy intestinal tissue is maintained, and predict the likely consequences of biochemical knockouts upon cell fate selection processes. Chemical reaction network theory (CRNT) is a powerful, generalised framework which assesses the capacity of our model for monostability or multistability, by analysing properties of the underlying network structure without recourse to specific parameter values or functional forms for reaction rates. CRNT highlights the role of β-catenin in stabilising the Notch pathway and damping oscillations, demonstrating that Wnt-mediated actions on the Hes1 promoter can induce dynamic transitions in the Notch system, from multistability to monostability. Time-dependent model simulations of cell pairs reveal the stabilising influence of Wnt upon the Notch pathway, in which β-catenin- and Dsh-mediated action on the Hes1 promoter are key in shaping the subcellular dynamics. Where Notch-mediated transcription of Hes1 dominates, there is Notch oscillation and maintenance of fate flexibility; Wnt-mediated transcription of Hes1 favours bistability akin to cell fate selection. Cells could therefore regulate the proportion of Wnt- and Notch-mediated control of the Hes1 promoter to coordinate the timing of cell fate selection as they migrate through the intestinal epithelium and are subject to reduced Wnt stimuli. Furthermore, mutant cells characterised by hyperstimulation of the Wnt pathway may, through coupling with Notch, invert cell fate in neighbouring healthy cells, enabling an aberrant cell to maintain its neighbours in mitotically active states. Public Library of Science 2017-02-28 /pmc/articles/PMC5363986/ /pubmed/28245235 http://dx.doi.org/10.1371/journal.pcbi.1005400 Text en © 2017 Kay et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Kay, Sophie K.
Harrington, Heather A.
Shepherd, Sarah
Brennan, Keith
Dale, Trevor
Osborne, James M.
Gavaghan, David J.
Byrne, Helen M.
The role of the Hes1 crosstalk hub in Notch-Wnt interactions of the intestinal crypt
title The role of the Hes1 crosstalk hub in Notch-Wnt interactions of the intestinal crypt
title_full The role of the Hes1 crosstalk hub in Notch-Wnt interactions of the intestinal crypt
title_fullStr The role of the Hes1 crosstalk hub in Notch-Wnt interactions of the intestinal crypt
title_full_unstemmed The role of the Hes1 crosstalk hub in Notch-Wnt interactions of the intestinal crypt
title_short The role of the Hes1 crosstalk hub in Notch-Wnt interactions of the intestinal crypt
title_sort role of the hes1 crosstalk hub in notch-wnt interactions of the intestinal crypt
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5363986/
https://www.ncbi.nlm.nih.gov/pubmed/28245235
http://dx.doi.org/10.1371/journal.pcbi.1005400
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