首页> 外文期刊>Methods: A Companion to Methods in Enzymology >Using molecular tethering to analyze the role of nuclear compartmentalization in the regulation of mammalian gene activity.
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Using molecular tethering to analyze the role of nuclear compartmentalization in the regulation of mammalian gene activity.

机译:使用分子束缚分析核区室化在调节哺乳动物基因活性中的作用。

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摘要

The mammalian nucleus has a complex structural organization that dynamically interacts with the genome. Chromatin is organized into discrete domains by association with distinct nuclear compartments enriched in structural and regulatory proteins. Growing evidence suggests that gene activity is modulated by interactions with these sub-nuclear compartments. Therefore, analyzing how nuclear architecture controls genome activity will be necessary to fully understand complex biological processes such as development and disease. In this article we describe a molecular methodology involving inducible tethering that can be used to position genes at the inner nuclear membrane (INM)-lamina compartment. The consequences of such directed re-positioning on gene activity or other DNA transactions can then be analyzed. This approach can be generalized and extended to position genes or chromosomal domains within other nuclear compartments thereby greatly facilitating the analysis of nuclear structure and its impact ongenome activity.
机译:哺乳动物核具有复杂的结构组织,可与基因组动态相互作用。染色质通过与富含结构蛋白和调节蛋白的独特核区室结合而被组织成离散域。越来越多的证据表明,基因活性受与这些亚核区室的相互作用的调节。因此,有必要分析核结构如何控制基因组活性,以充分了解复杂的生物学过程,例如发育和疾病。在本文中,我们描述了一种涉及诱导性束缚的分子方法,该方法可用于将基因定位在内核膜(INM)层室中。然后可以分析这种定向重新定位对基因活性或其他DNA交易的影响。这种方法可以推广并扩展到在其他核区室中定位基因或染色体结构域,从而极大地促进了对核结构及其对基因组活性的影响的分析。

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