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Ultrasensitivity in independent multisite systems

机译:独立多站点系统中的超敏性

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摘要

Multisite modifications are widely recognized as an essential feature of many switch-like responses in signal transduction. It is usually assumed that the modification of one site directly or indirectly increases the rate of modification of neighboring sites. In this paper we provide a new set of assumptions for a multisite system to become highly ultrasensitive even in the absence of cooperativity or allostery. We assume that the individual sites are modified independently of each other, and that protein activity is an ultrasensitive function of the fraction of modified sites. These assumptions are particularly useful in the context of multisite systems with a large (8+) number of sites. We estimate the apparent Hill coefficient of the dose responses in the sequential and nonsequential cases, highlight their different qualitative properties, and discuss a formula to approximate dose responses in the nonsequential case. As an example we describe a model of bacterial chemotaxis that features robust ultrasensitivity and perfect adaptation over a wide range of ligand concentrations, based on non-allosteric multisite behavior at the level of receptors and flagella. We also include a model of the inactivation of the yeast pheromone protein Ste5 by cell cycle proteins.
机译:在信号转导中,多位点修饰被认为是许多类似开关的响应的基本特征。通常假定一个位点的修饰直接或间接地增加了相邻位点的修饰速率。在本文中,我们提供了一套新的假设,使多站点系统即使在没有协作性或别构性的情况下也变得高度超灵敏。我们假设各个位点彼此独立修饰,并且蛋白质活性是修饰位点部分的超灵敏功能。这些假设在具有大量(8+)个站点的多站点系统的情况下特别有用。我们估计了顺序和非顺序情况下剂量反应的表观希尔系数,突出了它们的不同定性性质,并讨论了近似公式来近似非顺序情况下的剂量反应。作为一个例子,我们描述了一种细菌趋化性模型,该模型具有基于受体和鞭毛水平的非变构多位点行为,在广泛的配体浓度范围内具有强大的超敏性和完美的适应性。我们还包括通过细胞周期蛋白灭活酵母信息素Ste5的模型。

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