Bulletin of the American Physical Society
APS March Meeting 2020
Volume 65, Number 1
Monday–Friday, March 2–6, 2020; Denver, Colorado
Session U31: Emergent Collective Dynamics in Biology: from Microbes to Organs II
2:30 PM–5:18 PM,
Thursday, March 5, 2020
Room: 503
Sponsoring
Units:
DSOFT DBIO GSNP
Chair: Sujit Datta, Princeton University
Abstract: U31.00006 : Control of patterning in human pluripotent stem cell colonies via a Turing system with reactive boundaries
Presenter:
Daniel Aguilar-Hidalgo
(School of Biomedical Engineering, University of British Columbia)
Authors:
Benjamin McMaster
(School of Biomedical Engineering, University of British Columbia)
Himanshu Kaul
(School of Biomedical Engineering, University of British Columbia)
Daniel Aguilar-Hidalgo
(School of Biomedical Engineering, University of British Columbia)
Peter Zandstra
(School of Biomedical Engineering, University of British Columbia)
Recently, in-vitro studies using human pluripotent stem cells (hPSC) in confined environments have shown the emergence of spatially organized markers of an early gastrulation-like state following induction by the bone morphogenetic protein 4 (BMP4), thus providing a framework to understand, and ultimately control, collective self-organization and pattern formation in hPSC.
We present minimal Turing system that is consistent with hPSC patterns observed in 2- and 3-D structures. Our approach considers that the morphogen flux at the colony boundaries is morphogen-concentration dependent (a so-called reactive boundary). Using this framework, we have quantified the effective transport dynamics of the morphogen BMP4 in hPSC colonies, and defined conditions that predict pattern properties such as marker spatial order, domain size and thresholds for symmetry-breaking events. This work presents a general framework for self-organized pattern formation that explain observed patterns in hPSC colonies, leading to a design-based specification of collective cell behavior.
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