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Modeling signaling‐dependent pluripotency with Boolean logic to predict cell fate transitions

机译:使用布尔逻辑对依赖信号的多能性进行建模以预测细胞命运的转变

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摘要

Pluripotent stem cells (PSCs) exist in multiple stable states, each with specific cellular properties and molecular signatures. The mechanisms that maintain pluripotency, or that cause its destabilization to initiate development, are complex and incompletely understood. We have developed a model to predict stabilized PSC gene regulatory network (GRN) states in response to input signals. Our strategy used random asynchronous Boolean simulations (R‐ABS) to simulate single‐cell fate transitions and strongly connected components (SCCs) strategy to represent population heterogeneity. This framework was applied to a reverse‐engineered and curated core GRN for mouse embryonic stem cells (mESCs) and used to simulate cellular responses to combinations of five signaling pathways. Our simulations predicted experimentally verified cell population compositions and input signal combinations controlling specific cell fate transitions. Extending the model to PSC differentiation, we predicted a combination of signaling activators and inhibitors that efficiently and robustly generated a Cdx2+Oct4 cells from naïve mESCs. Overall, this platform provides new strategies to simulate cell fate transitions and the heterogeneity that typically occurs during development and differentiation.
机译:多能干细胞(PSC)以多种稳定状态存在,每种状态都有特定的细胞特性和分子特征。维持多能性或导致其不稳定以启动发育的机制是复杂且不完整的。我们已经开发了一个模型来预测响应输入信号的稳定的PSC基因调控网络(GRN)状态。我们的策略使用随机异步布尔仿真(R-ABS)来模拟单细胞命运转变,并使用强连接组件(SCC)策略来表示种群异质性。该框架已应用于小鼠胚胎干细胞(mESC)的逆向工程和精选核心GRN,并用于模拟细胞对5种信号通路组合的反应。我们的模拟预测了经过实验验证的细胞群体组成和控制特定细胞命运转变的输入信号组合。将模型扩展到PSC分化,我们预测了信号激活剂和抑制剂的组合,它们可以有效地从原始mESCs产生Cdx2 + Oct4 -细胞。总体而言,该平台提供了新的策略来模拟细胞命运的转变以及发育和分化过程中通常发生的异质性。

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