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噬菌体λ的OR控制系统。基因调控的物理化学模型。

The OR control system of bacteriophage lambda. A physical-chemical model for gene regulation.

作者信息

Shea M A, Ackers G K

出版信息

J Mol Biol. 1985 Jan 20;181(2):211-30. doi: 10.1016/0022-2836(85)90086-5.

Abstract

A quantitative model has been developed for processes in the bacteriophage lambda that control the switchover from lysogenic to lytic modes of growth. These processes include the interactions of cI repressor and cro proteins at the three DNA sites of the right operator, OR, the binding of RNA polymerase at promoters PR and PRM, the synthesis of cI repressor and cro proteins, and the degradative action of recA during induction of lysis. The model is comprised of two major physical-chemical components: a statistical thermodynamic theory for relative probabilities of the various molecular configurations of the control system; and a kinetic model for the coupling of these probabilities to functional events, including synthesis of regulatory proteins cI and cro. Using independently evaluated interaction constants and rate parameters, the model was found capable of predicting essential physiological characteristics of the system over an extended time. Sufficiency of the model to predict known physiological properties lends credence to the physical-chemical assumptions used in its construction. Several major physiological characteristics were found to arise as "system properties" through the non-linear, time-dependent, feedback-modulated combinations of molecular interactions prescribed by the model. These include: maintenance of the lysogenic state in the absence of recA-mediated cI repressor degradation; induction of lysis and the phenomenon of subinduction; and autogenous negative control of cro. We have used the model to determine the roles, within the composite system, of several key molecular processes previously characterized by studies in vitro. These include: co-operativity in cI repressor binding to DNA; interactions between repressors and RNA polymerase (positive control); and the monomer-dimer association of cI repressor molecules. A major role of cI repressor co-operativity is found to be that of guaranteeing stability of the lysogenic state against minor changes in cI repressor levels within the cell. The role of positive control seems to be that of providing for a peaked, rather than monotonic, dependence of PRM activity on cI repressor level, while permitting PR activity to be a step function. The model correlates an immense body of studies in vivo and in vitro, and it makes testable predictions about molecular phenomena as well as physiological characteristics of bacteriophage lambda. The approach developed in this study can be extended to include more features of the lambda system and to treat other systems of gene regulation.

摘要

已开发出一种定量模型,用于描述噬菌体λ中控制从溶原生长模式向裂解生长模式转换的过程。这些过程包括cI阻遏蛋白和cro蛋白在右操纵子OR的三个DNA位点上的相互作用、RNA聚合酶在启动子PR和PRM上的结合、cI阻遏蛋白和cro蛋白的合成,以及recA在裂解诱导过程中的降解作用。该模型由两个主要的物理化学组件组成:一个关于控制系统各种分子构型相对概率的统计热力学理论;以及一个将这些概率与功能事件(包括调节蛋白cI和cro的合成)相耦合的动力学模型。使用独立评估的相互作用常数和速率参数,发现该模型能够在较长时间内预测系统的基本生理特征。该模型预测已知生理特性的充分性为其构建中使用的物理化学假设提供了可信度。通过该模型规定的分子相互作用的非线性、时间依赖性、反馈调节组合,发现几个主要的生理特征作为“系统特性”出现。这些特征包括:在没有recA介导的cI阻遏蛋白降解的情况下维持溶原状态;裂解诱导和亚诱导现象;以及cro的自体负调控。我们已使用该模型来确定先前在体外研究中表征的几个关键分子过程在复合系统中的作用。这些过程包括:cI阻遏蛋白与DNA结合的协同性;阻遏蛋白与RNA聚合酶之间的相互作用(正调控);以及cI阻遏蛋白分子的单体 - 二聚体缔合。发现cI阻遏蛋白协同性的一个主要作用是保证溶原状态对细胞内cI阻遏蛋白水平微小变化的稳定性。正调控的作用似乎是使PRM活性对cI阻遏蛋白水平的依赖性呈峰值而非单调变化,同时允许PR活性为阶跃函数。该模型关联了大量体内和体外的研究,并且它对噬菌体λ的分子现象以及生理特征做出了可检验的预测。本研究中开发的方法可以扩展到包括λ系统的更多特征,并用于处理其他基因调控系统。

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