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首页> 外文期刊>PLoS Computational Biology >Dependencies among Editing Sites in Serotonin 2C Receptor mRNA
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Dependencies among Editing Sites in Serotonin 2C Receptor mRNA

机译:血清素2C受体mRNA编辑位点之间的依赖性。

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The serotonin 2C receptor (5-HT2CR)–a key regulator of diverse neurological processes–exhibits functional variability derived from editing of its pre-mRNA by site-specific adenosine deamination (A-to-I pre-mRNA editing) in five distinct sites. Here we describe a statistical technique that was developed for analysis of the dependencies among the editing states of the five sites. The statistical significance of the observed correlations was estimated by comparing editing patterns in multiple individuals. For both human and rat 5-HT2CR, the editing states of the physically proximal sites A and B were found to be strongly dependent. In contrast, the editing states of sites C and D, which are also physically close, seem not to be directly dependent but instead are linked through the dependencies on sites A and B, respectively. We observed pronounced differences between the editing patterns in humans and rats: in humans site A is the key determinant of the editing state of the other sites, whereas in rats this role belongs to site B. The structure of the dependencies among the editing sites is notably simpler in rats than it is in humans implying more complex regulation of 5-HT2CR editing and, by inference, function in the human brain. Thus, exhaustive statistical analysis of the 5-HT2CR editing patterns indicates that the editing state of sites A and B is the primary determinant of the editing states of the other three sites, and hence the overall editing pattern. Taken together, these findings allow us to propose a mechanistic model of concerted action of ADAR1 and ADAR2 in 5-HT2CR editing. Statistical approach developed here can be applied to other cases of interdependencies among modification sites in RNA and proteins.
机译:血清素2C受体(5-HT2CR)是多种神经系统过程的关键调节剂,在五个不同的位点上通过位点特异性腺苷脱氨(A到I的前mRNA编辑)表现出其前mRNA编辑所产生的功能变异性。 。在这里,我们描述了一种统计技术,该技术用于分析五个站点的编辑状态之间的依赖性。通过比较多个个体中的编辑模式来估计观察到的相关性的统计显着性。对于人类和大鼠5-HT2CR,发现物理上近端位点A和B的编辑状态强烈相关。相反,站点C和D的编辑状态在物理上也很接近,似乎并不直接相关,而是分别通过对站点A和B的相关性链接在一起。我们观察到人类和大鼠的编辑模式之间存在明显差异:在人类中,位点A是其他位点的编辑状态的关键决定因素,而在大鼠中,此角色属于位点B。编辑位点之间的依存关系结构是与人类相比,大鼠明显更简单,这意味着对5-HT2CR编辑的调控更为复杂,并据此推断其在人脑中的功能。因此,对5-HT2CR编辑模式的详尽统计分析表明,站点A和B的编辑状态是其他三个站点的编辑状态的主要决定因素,因此也是整个编辑模式的主要决定因素。综上所述,这些发现使我们能够提出5-HT2CR编辑中ADAR1和ADAR2协同作用的机理模型。本文开发的统计方法可以应用于RNA和蛋白质修饰位点之间相互依赖的其他情况。

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