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耦合三维与一维扩散的缔合动力学。特定DNA位点缔合速率的链长依赖性。

Association kinetics with coupled three- and one-dimensional diffusion. Chain-length dependence of the association rate of specific DNA sites.

作者信息

Berg O G, Ehrenberg M

出版信息

Biophys Chem. 1982 Apr;15(1):41-51. doi: 10.1016/0301-4622(82)87015-4.

Abstract

The effective target size of a specific binding site on a long polymeric chain can be considerably enhanced if the associating molecules slide along the chain in a one-dimensional diffusion. Such a mechanism has been proposed to explain the "faster than diffusion controlled" association of the lac repressor protein with the operator site on a long DNA chain. An important experimental tool for investigating the properties of rate-enhancing mechanisms of this type is now becoming available. In these experiments the DNA chain length is varied and the association rate of the investigated protein is measured. Previous attempts to describe theoretically how such one-dimensional sliding processes behave under those conditions were either oversimplified or connected with fundamental errors. We present here a theory for the association rate of proteins with a specific site on DNA molecules with variable lengths. We use a steady-state approach as do Schranner and Richter (Biophys. Chem. 8 (1978)47) but, in contrast, use boundary conditions which appear to be physically more reasonable.

摘要

如果缔合分子沿长聚合物链进行一维扩散滑动,那么长聚合物链上特定结合位点的有效目标大小会显著增加。有人提出这样一种机制来解释乳糖阻遏蛋白与长DNA链上操纵基因位点的“快于扩散控制”的缔合。现在,一种用于研究这类速率增强机制特性的重要实验工具即将问世。在这些实验中,DNA链长度会发生变化,并测量所研究蛋白质的缔合速率。此前试图从理论上描述这种一维滑动过程在这些条件下的行为,要么过于简化,要么存在根本性错误。我们在此提出一种关于蛋白质与不同长度DNA分子上特定位点缔合速率的理论。我们采用了与施兰纳和里希特(《生物物理化学》8 (1978) 47)相同的稳态方法,但不同的是,我们使用的边界条件在物理上似乎更合理。

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