Bulletin of the American Physical Society
APS March Meeting 2018
Volume 63, Number 1
Monday–Friday, March 5–9, 2018; Los Angeles, California
Session E50: Morphogenesis I
8:00 AM–11:00 AM,
Tuesday, March 6, 2018
LACC
Room: 511B
Sponsoring
Units:
DBIO GSOFT GSNP
Chair: Andrej Kosmrlj, Princeton Univ
Abstract ID: BAPS.2018.MAR.E50.1
Abstract: E50.00001 : Ensembles, Dynamics and Cell Types
8:00 AM–8:36 AM
Presenter:
Stuart Kauffman
(Institute for Systems Biology)
Author:
Stuart Kauffman
(Institute for Systems Biology)
A system’s state follows a trajectory in state space that flows to one repetitive cycle of states, an attractor. A network may have many attractors.
Such networks can be “Ordered”, “Critical” or “Chaotic”. K <2.0 is ordered. K =2.0 is critical. K > 2.0 is chaotic. Biases in the Boolean functions yield another parameter, P. In the K P plane a line of criticality separates order from chaos.
Critical networks are of high interest. The length of state cycles scales as square root N, the number of attractors scales as square root N, intense localization.
The natural hypothesis is that a cell type corresponds to an attractor of the network. Good evidence supports this.
The theory that evolved genetic regulatory networks are generic members of the critical ensemble predicts that the number of cell types in an organism should scale as a power law with respect to DNA per cell. The data across 11 distinct phyla shows a power law scaling of 0.88.
Cells appear dynamically critical, with a power law distribution of alteration in gene expression upon single mutations, and parallel flow in state space on perturbations.
Selection on chaotic or ordered networks yields critical networks suggesting an evolutionary pathway to their emergence.
Ensemble Theories bear on biology beyond Natural Selection.
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To cite this abstract, use the following reference: http://meetings.aps.org/link/BAPS.2018.MAR.E50.1
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