4.7 Article

Shortcuts in Stochastic Systems and Control of Biophysical Processes

Journal

PHYSICAL REVIEW X
Volume 12, Issue 2, Pages -

Publisher

AMER PHYSICAL SOC
DOI: 10.1103/PhysRevX.12.021048

Keywords

Biological Physics; Complex Systems; Statistical Physics

Funding

  1. U.S. National Science Foundation (NSF) [MCB-1651650]
  2. LabEx Cell(n)Scale [ANR-11-LABX-0038, ANR-10-IDEX-0001-02]
  3. U.S. Department of Energy [DOE-SC0009946]
  4. National Science Foundation Graduate Research Fellowship Program [DGE 1840340]

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Biochemical reaction networks regulating living systems are stochastic, and the use of counterdiabatic driving can control biological processes, with the possibility of implementing local control to adapt to limited external control in biological systems.
The biochemical reaction networks that regulate living systems are all stochastic to varying degrees. The resulting randomness affects biological outcomes at multiple scales, from the functional states of single proteins in a cell to the evolutionary trajectory of whole populations. Controlling how the distribution of these outcomes changes over time-via external interventions like time-varying concentrations of chemical species-is a complex challenge. In this work, we show how counterdiabatic (CD) driving, first developed to control quantum systems, provides a versatile tool for steering biological processes. We develop a practical graph-theoretic framework for CD driving in discrete-state continuous-time Markov networks. Though CD driving is limited to target trajectories that are instantaneous stationary states, we show how to generalize the approach to allow for nonstationary targets and local control-where only a subset of system states is targeted. The latter is particularly useful for biological implementations where there may be only a small number of available external control knobs, insufficient for global control. We derive simple graphical criteria for when local versus global control is possible. Finally, we illustrate the formalism with global control of a genetic regulatory switch and local control in chaperone-assisted protein folding. The derived control protocols in the chaperone system closely resemble natural control strategies seen in experimental measurements of heat shock response in yeast and E. coli.

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