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首页> 外文期刊>Nucleic acids research >Targeted manipulation of heterochromatin rescues MeCP2 Rett mutants and re-establishes higher order chromatin organization
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Targeted manipulation of heterochromatin rescues MeCP2 Rett mutants and re-establishes higher order chromatin organization

机译:异染色质的靶向操作可拯救MeCP2 Rett突变体并重新建立更高阶的染色质组织

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Heterochromatic regions represent a significant portion of the mammalian genome and have been implied in several important cellular processes, including cell division and genomic stability. However, its composition and dynamics remain largely unknown. To better understand how heterochromatin functions and how it is organized within the context of the cell nucleus, we have developed molecular tools allowing the targeting of virtually any nuclear factor specifically to heterochromatic regions and, thereby, the manipulation, also in a temporally controlled manner, of its composition. To validate our approach, we have ectopically targeted MeCP2 chromatin binding deficient Rett mutants to constitutive heterochromatic regions and analyze its functional consequences. We could show that, once bound to their endogenous target regions, their ability to re-organize higher order chromatin structure is restored. Furthermore, a temporally controlled targeting strategy allowed us to monitor MeCP2-mediated chromatin rearrangements in vivo and to visualize large-scale chromatin movements over several micrometers, as well as heterochromatic foci fusion events. This novel strategy enables specific tethering of any protein to heterochromatin and lays the ground for controlled manipulation of its composition and organization.
机译:异色区域代表了哺乳动物基因组的重要部分,并且隐含在几个重要的细胞过程中,包括细胞分裂和基因组稳定性。但是,其组成和动力学仍然未知。为了更好地了解异染色质如何发挥功能以及如何在细胞核的背景下进行组织,我们开发了分子工具,可将几乎任何核因子专门靶向异色区,从而也可以以时间控制的方式进行操作,其组成。为了验证我们的方法,我们已经异位靶向MeCP2染色质结合缺陷的Rett突变体至组成型异色区域,并分析了其功能后果。我们可以证明,一旦绑定到它们的内源性目标区域,它们重组高阶染色质结构的能力就会恢复。此外,时间控制的靶向策略使我们能够在体内监测MeCP2介导的染色质重排,并可视化大规模染色质在数微米范围内的移动以及异色焦点融合事件。这种新颖的策略可以使任何蛋白质与异染色质特异性连接,并为对其组成和组织的受控操纵奠定了基础。

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