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Internal regulation of a modular system: the different faces of internal control

机译:模块化系统的内部调节:内部控制的不同方面

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The living cell houses a multitude of molecular processes that operate simultaneously in a mutually consistent fashion. A certain degree of organization stands out, e.g. in terms of the various metabolic pathways, transcription versus translation, signal transduction versus metabolism. This paper shows that by taking one of the aforementioned organizational principles into account, the complexity of understanding cell function quantitatively may be reduced significantly. To this aim the definition of the corresponding type of organization is refined and the conceptual tools used in the analysis of the control of cell function are adjusted. The approach is elaborated for a theoretical model of cell function, in which the latter depends on a constellation of interdependent but unconnected modules. The organization of a system is reduced to global control within a limited set of partaking modules and the links between them. Information about the systems total internal control and regulability is then drastically reduced to the information specifying global control and the regulability of the pathways that constitute the system. It is shown quantitatively how control at a lower level of organization bears on the control of the cell as a whole. The approach centers on writing the product of control (matrix) and elasticity (matrix) at a number of different levels of aggregation; these products equalling the identity (matrix) under different conditions. We demonstrate that there are at least three ways in which control and regulability of a system can be matched. In one, the true control within and between the modules of the systems is the inverse of the primary regulability (i.e. elasticity plus stoichiometry). In a second, the control internal to a module (but partly determined through the other modules) is matched by the inverse of newly defined 'global' regulabilities for each module separately, which comprise the regulatory impact of the remainder of the system. In the third, the regulabilities are the ones intrinsic to the module and the control is taken equal to the control that would reign in the absence of the regulatory interactions between the units. In making these distinctions, it becomes transparent how much control stems from control within the organizational modules, and how much derives from the regulatory interactions between them. Control through other modules turns out to be equivalent, al steady state, to control within a module. The implications of this type of cellular organization for the location of the steady-state operating point is discussed. (C) 1997 Elsevier Science Ireland Ltd.
机译:活细胞内有许多分子过程,它们以相互一致的方式同时运行。一定程度的组织脱颖而出,例如就各种代谢途径而言,转录与翻译,信号转导与代谢有关。本文表明,通过考虑上述组织原则之一,可以显着降低定量了解细胞功能的复杂性。为此,对相应组织类型的定义进行了完善,并调整了细胞功能控制分析中使用的概念工具。该方法针对细胞功能的理论模型进行了阐述,其中细胞功能取决于相互依存但未连接的模块的构象。系统的组织简化为有限的一组分配模块及其之间的链接的全局控制。然后,将有关系统总体内部控制和可调节性的信息急剧减少为指定全局控制和构成系统的路径的可调节性的信息。定量显示了较低级别组织的控制如何影响整个单元的控制。该方法的重点是在许多不同的聚合级别上写控制量(矩阵)和弹性(矩阵)的乘积。这些乘积在不同条件下等于身份(矩阵)。我们证明了至少有三种方法可以匹配系统的控制和可调节性。在一个方面,系统模块内部和模块之间的真正控制是主要可调节性(即弹性加化学计量)的倒数。在第二秒中,模块内部的控制(但部分通过其他模块确定)通过每个模块分别新定义的“全局”可调节性的倒数进行匹配,这包括系统其余部分的调节影响。在第三种中,可调节性是模块固有的,而控制则等同于在单元之间不存在调节相互作用的情况下将占据主导地位的控制。在做出这些区分时,透明的是多少控制来自组织模块内部的控制,多少来自它们之间的监管交互。事实证明,通过其他模块进行的控制在模块内部处于等效状态(稳态)。讨论了这种类型的细胞组织对稳态工作点位置的影响。 (C)1997爱思唯尔科学爱尔兰有限公司

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