Parameter asymmetry and time-scale separation in core genetic commitment circuits

Theory allows studying why Evolution might select core genetic commitment circuit topologies over alternatives. The nonlinear dynamics of the underlying gene regulation together with the unescapable subtle interplay of intrinsic biochemical noise impact the range of possible evolutionary choices. The question of why certain genetic regulation circuits might present robustness to phenotype-delivery breaking over others, is therefore of high interest. Here, the behavior of systematically more complex commitment circuits is studied, in the presence of intrinsic noise, with a focus on two aspects relevant to biology： parameter asymmetry and time-scale separation. We show that phenotype delivery is broken in simple two- and three-gene circuits. In the two-gene circuit, we show how stochastic potential wells of different depths break commitment. In the three-gene circuit, we show that the onset of oscillations breaks the commitment phenotype in a systematic way. Finally, we also show that higher dimensional circuits （four-gene and five-gene circuits） may be intrinsically more robust.

Time-scale separation and stochasticity conspire to impact phenotypic dynamics in the canonical and inverted Bacillus subtilis core genetic regulation circuits

Backgrounds In this work, we study two seemingly unrelated aspects of core genetic nonlinear dynamical control of the competence phenotype in Bacillus subtilis, a common Gram-positive bacterium living in the soil. Methods: We focus on hitherto unchartered aspects of the dynamics by exploring the effect of time-scale separation between transcription and translation and, as well, the effect of intrinsic molecular stochasticity. We consider these aspects of regulatory control as two possible evolutionary handles. Results: Hence, using theory and computations, we study how the onset of oscillations breaks the excitability-based competence phenotype in two topologically close evolutionary-competing circuits: the canonical "wild-type" regulation circuit selected by Evolution and the corresponding indirect-feedback inverted circuit that failed to be selected by Evolution, as was shown elsewhere, due to dynamical reasons. Conclusions^ Relying on in-silico perturbation of the living state, we show that the canonical core genetic regulation of excitability-based competence is more robust against switching to phenotype-breaking oscillations than the inverted feedback organism. We show how this is due to time-scale separation and stochasticity.

Delineating the respective impacts of stochastic curl- and grad-forces in a family of idealized core genetic commitment circuits

Stochastic dynamics pervades gene regulation. Despite being random, the dynamics displays a kind of innate structure. In fact, two stochastic forces combine driving efforts： one force originates from the gradient of the underlying stochastic potential, and the other originates from the mathematical curl of the probability flux. The curl force gives rise to rotation. The gradient force gives rise to drift. Together they give rise to helical behavior. Here, it is shown that around and about the vicinity of attractive fixed points, the gradient force naturally wanes but the curl force is found to remain high. This leads to a locally noticeably different type of stochastic track near and about attractive fixed points, compared to tracks in regions where drift dominates. The consistency of this observation with the experimental fact that, in biology, fate commitment appears to not be a-priory locked-in, but rather necessitating active maintenance, is discussed. Hence attractive fixed-points are not only fuzzy, but may effectively be, locally, ＂more free＂.