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基于酶促有限竞争的动力学记忆。

Kinetic memory based on the enzyme-limited competition.

作者信息

Hatakeyama Tetsuhiro S, Kaneko Kunihiko

机构信息

Department of Basic Science, Graduate School of Arts and Sciences, The University of Tokyo, Komaba, Meguro-ku, Tokyo, Japan.

出版信息

PLoS Comput Biol. 2014 Aug 14;10(8):e1003784. doi: 10.1371/journal.pcbi.1003784. eCollection 2014 Aug.

Abstract

Cellular memory, which allows cells to retain information from their environment, is important for a variety of cellular functions, such as adaptation to external stimuli, cell differentiation, and synaptic plasticity. Although posttranslational modifications have received much attention as a source of cellular memory, the mechanisms directing such alterations have not been fully uncovered. It may be possible to embed memory in multiple stable states in dynamical systems governing modifications. However, several experiments on modifications of proteins suggest long-term relaxation depending on experienced external conditions, without explicit switches over multi-stable states. As an alternative to a multistability memory scheme, we propose "kinetic memory" for epigenetic cellular memory, in which memory is stored as a slow-relaxation process far from a stable fixed state. Information from previous environmental exposure is retained as the long-term maintenance of a cellular state, rather than switches over fixed states. To demonstrate this kinetic memory, we study several models in which multimeric proteins undergo catalytic modifications (e.g., phosphorylation and methylation), and find that a slow relaxation process of the modification state, logarithmic in time, appears when the concentration of a catalyst (enzyme) involved in the modification reactions is lower than that of the substrates. Sharp transitions from a normal fast-relaxation phase into this slow-relaxation phase are revealed, and explained by enzyme-limited competition among modification reactions. The slow-relaxation process is confirmed by simulations of several models of catalytic reactions of protein modifications, and it enables the memorization of external stimuli, as its time course depends crucially on the history of the stimuli. This kinetic memory provides novel insight into a broad class of cellular memory and functions. In particular, applications for long-term potentiation are discussed, including dynamic modifications of calcium-calmodulin kinase II and cAMP-response element-binding protein essential for synaptic plasticity.

摘要

细胞记忆使细胞能够保留来自其环境的信息,这对于多种细胞功能至关重要,例如适应外部刺激、细胞分化和突触可塑性。尽管翻译后修饰作为细胞记忆的一个来源已受到广泛关注,但其引导此类改变的机制尚未完全揭示。在控制修饰的动态系统中,有可能将记忆嵌入多种稳定状态。然而,一些关于蛋白质修饰的实验表明,长期弛豫取决于所经历的外部条件,而没有在多稳定状态之间进行明确切换。作为多稳定性记忆方案的替代方案,我们提出用于表观遗传细胞记忆的“动力学记忆”,其中记忆作为远离稳定固定状态缓慢弛豫过程存储。先前环境暴露的信息作为细胞状态的长期维持而保留,而不是在固定状态之间切换。为了证明这种动力学记忆,我们研究了几个模型,其中多聚体蛋白质经历催化修饰(例如磷酸化和甲基化),并且发现当参与修饰反应的催化剂(酶)浓度低于底物浓度时,修饰状态会出现对数时间的缓慢弛豫过程。揭示了从正常快速弛豫阶段到这种缓慢弛豫阶段的急剧转变,并通过修饰反应之间的酶限制竞争来解释。通过蛋白质修饰催化反应的几个模型的模拟证实了缓慢弛豫过程,并且它能够记住外部刺激,因为其时间进程关键取决于刺激的历史。这种动力学记忆为广泛的细胞记忆和功能提供了新的见解。特别是,讨论了长期增强的应用,包括对突触可塑性至关重要的钙调蛋白激酶II和cAMP反应元件结合蛋白的动态修饰。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f07c/4133053/d0056f6133dc/pcbi.1003784.g001.jpg

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