A mathematical model of mechanotransduction reveals how mechanical memory regulates mesenchymal stem cell fate decisions

Tao Peng; Linan Liu; Adam L MacLean; Chi Wut Wong; Weian Zhao; Qing Nie

doi:10.1186/s12918-017-0429-x

A mathematical model of mechanotransduction reveals how mechanical memory regulates mesenchymal stem cell fate decisions

BMC Syst Biol. 2017 May 16;11(1):55. doi: 10.1186/s12918-017-0429-x.

Authors

Tao Peng¹, Linan Liu², Adam L MacLean¹, Chi Wut Wong², Weian Zhao², Qing Nie³

Affiliations

¹ Department of Mathematics, Center for Complex Biological Systems, and Center for Mathematical and Computational Biology, University of California, Irvine, CA, 92697, USA.
² Department of Pharmaceutical Sciences, Department of Biomedical Engineering, Department of Biological Chemistry, Sue and Bill Gross Stem Cell Research Center, Chao Family Comprehensive Cancer Center & Edwards Life sciences Center for Advanced Cardiovascular Technology, University of California, 845 Health Sciences Road, Irvine, CA, 92697, USA.
³ Department of Mathematics, Center for Complex Biological Systems, and Center for Mathematical and Computational Biology, University of California, Irvine, CA, 92697, USA. qnie@uci.edu.

Abstract

Background: Mechanical and biophysical properties of the cellular microenvironment regulate cell fate decisions. Mesenchymal stem cell (MSC) fate is influenced by past mechanical dosing (memory), but the mechanisms underlying this process have not yet been well defined. We have yet to understand how memory affects specific cell fate decisions, such as the differentiation of MSCs into neurons, adipocytes, myocytes, and osteoblasts.

Results: We study a minimal gene regulatory network permissive of multi-lineage MSC differentiation into four cell fates. We present a continuous model that is able to describe the cell fate transitions that occur during differentiation, and analyze its dynamics with tools from multistability, bifurcation, and cell fate landscape analysis, and via stochastic simulation. Whereas experimentally, memory has only been observed during osteogenic differentiation, this model predicts that memory regions can exist for each of the four MSC-derived cell lineages. We can predict the substrate stiffness ranges over which memory drives differentiation; these are directly testable in an experimental setting. Furthermore, we quantitatively predict how substrate stiffness and culture duration co-regulate the fate of a stem cell, and we find that the feedbacks from the differentiating MSC onto its substrate are critical to preserve mechanical memory. Strikingly, we show that re-seeding MSCs onto a sufficiently soft substrate increases the number of cell fates accessible.

Conclusions: Control of MSC differentiation is crucial for the success of much-lauded regenerative therapies based on MSCs. We have predicted new memory regions that will directly impact this control, and have quantified the size of the memory region for osteoblasts, as well as the co-regulatory effects on cell fates of substrate stiffness and culture duration. Taken together, these results can be used to develop novel strategies to better control the fates of MSCs in vitro and following transplantation.

Keywords: Bistability; Cell fate decision; ECM; Mathematical modeling; Memory; Mesenchymal stem cell; Nonlinear dynamics; Stiffness sensing; YAP/TAZ.

MeSH terms

Biomechanical Phenomena
Cell Adhesion
Cell Differentiation
Cell Lineage
Feedback, Physiological
Gene Regulatory Networks
Mechanical Phenomena*
Mechanotransduction, Cellular*
Mesenchymal Stem Cells / cytology*
Mesenchymal Stem Cells / metabolism
Models, Biological*

Abstract

MeSH terms

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