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首页> 外文期刊>Molecular biology reports >Nuclear matrix, dynamic histone acetylation and transcriptionally active chromatin.
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Nuclear matrix, dynamic histone acetylation and transcriptionally active chromatin.

机译:核基质,动态组蛋白乙酰化和转录活性染色质。

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摘要

The nuclear matrix, the RNA-protein skeleton of the nucleus, has a role in the organization and function of nuclear DNA. Nuclear processes associated with the nuclear matrix include transcription, replication and dynamic histone acetylation. Nuclear matrix proteins, which are tissue and cell type specific, are altered with transformation and state of differentiation. Transcription factors are associated with the nuclear matrix, with the spectra of nuclear matrix bound factors being cell type specific. There is compelling evidence that the transcription machinery is anchored to the nuclear matrix, and the chromatin fiber is spooled through this complex. Transcriptionally active chromatin domains are associated with dynamically acetylated histones. The energy exhaustive process of dynamic histone acetylation has several functions. Acetylation of the N-terminal tails of the core histones alters nucleosome and higher order chromatin structure, aiding transcriptional elongation and facilitating the binding of transcription factors to nucleosomes associated with regulatory DNA sequences. Histone acetylation can manipulate the interactions of regulatory proteins that bind to the N-terminal tails of the core histones. Lastly, dynamic acetylation may contribute to the transient attachment of transcriptionally active chromatin to the nuclear matrix. Reversible histone acetylation is catalyzed by histone acetyltransferase and deacetylase, enzymes associated with the nuclear matrix. The recent isolation and characterization of histone acetyltransferase and deacetylase reveals that these enzymes are related to transcriptional regulators, providing us with new insights about how these enzymes are targeted to nuclear matrix sites engaged in transcription.
机译:核基质,即核的RNA蛋白骨架,在核DNA的组织和功能中起作用。与核基质相关的核过程包括转录,复制和动态组蛋白乙酰化。具有组织和细胞类型特异性的核基质蛋白随转化和分化状态而改变。转录因子与核基质相关,核基质结合因子的光谱是细胞类型特异性的。有令人信服的证据表明,转录机制锚定在核基质上,染色质纤维绕线穿过该复合物。转录活性染色质域与动态乙酰化的组蛋白相关。动态组蛋白乙酰化的能量消耗过程具有多种功能。核心组蛋白的N末端尾部的乙酰化会改变核小体和更高阶的染色质结构,有助于转录伸长并促进转录因子与与调控DNA序列相关的核小体结合。组蛋白乙酰化可以操纵与核心组蛋白N末端尾部结合的调节蛋白的相互作用。最后,动态乙酰化可能有助于转录活性染色质与核基质的瞬时连接。组蛋白乙酰转移酶和脱乙酰酶(与核基质有关的酶)催化可逆的组蛋白乙酰化。最近对组蛋白乙酰转移酶和脱乙酰酶的分离和表征表明,这些酶与转录调节因子有关,这为我们提供了关于这些酶如何靶向参与转录的核基质位点的新见解。

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