Single-Cell Reprogramming in Mouse Embryo Development through a Critical Transition State

被引:3
作者
Tsuchiya, Masa [1 ,2 ]
Giuliani, Alessandro [3 ]
Yoshikawa, Kenichi [4 ]
机构
[1] SRI, SEIKO Life Sci Lab, Osaka 540659, Japan
[2] Keio Univ, Sch Media & Governance, Syst Biol Program, Fujisawa, Kanagawa 2520882, Japan
[3] Ist Super Sanita, Environm & Hlth Dept, I-00161 Rome, Italy
[4] Doshisha Univ, Fac Life & Med Sci, Kyotanabe 6100394, Japan
关键词
single-cell early embryo development; single-cell reprogramming; statistical thermodynamics; non-equilibrium dynamics; transition state; self-organized criticality; critical states; critical gene ensemble; REGULATORY NETWORK; GENE-EXPRESSION;
D O I
10.3390/e19110584
中图分类号
O4 [物理学];
学科分类号
0702 ;
摘要
Our previous work on the temporal development of the genome-expression profile in single-cell early mouse embryo indicated that reprogramming occurs via a critical transition state, where the critical-regulation pattern of the zygote state disappears. In this report, we unveil the detailed mechanism of how the dynamic interaction of thermodynamic states (critical states) enables the genome system to pass through the critical transition state to achieve genome reprogramming right after the late 2-cell state. Self-organized criticality (SOC) control of overall expression provides a snapshot of self-organization and explains the coexistence of critical states at a certain experimental time point. The time-development of self-organization is dynamically modulated by changes in expression flux between critical states through the cell nucleus milieu, where sequential global perturbations involving activation-inhibition of multiple critical states occur from the middle 2-cell to the 4-cell state. Two cyclic fluxes act as feedback flow and generate critical-state coherent oscillatory dynamics. Dynamic perturbation of these cyclic flows due to vivid activation of the ensemble of low-variance expression (sub-critical state) genes allows the genome system to overcome a transition state during reprogramming. Our findings imply that a universal mechanism of long-term global RNA oscillation underlies autonomous SOC control, and the critical gene ensemble at a critical point (CP) drives genome reprogramming. Identification of the corresponding molecular players will be essential for understanding single-cell reprogramming.
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页数:18
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