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与组蛋白甲基化模式相关的序列偏倚的证据。

Evidence for sequence biases associated with patterns of histone methylation.

机构信息

Genome Biology Group, Duke Institute for Genome Sciences & Policy, Duke University, Durham, NC 27708, USA.

出版信息

BMC Genomics. 2012 Aug 2;13:367. doi: 10.1186/1471-2164-13-367.

Abstract

BACKGROUND

Combinations of histone variants and modifications, conceptually representing a histone code, have been proposed to play a significant role in gene regulation and developmental processes in complex organisms. While various mechanisms have been implicated in establishing and maintaining epigenetic patterns at specific locations in the genome, they are generally believed to be independent of primary DNA sequence on a more global scale.

RESULTS

To address this systematically in the case of the human genome, we have analyzed primary DNA sequences underlying patterns of 19 different methylated histones in human primary T-cells and patterns of three methylated histones across additional human cell lines. We report strong sequence biases associated with most of these histone marks genome-wide in each cell type. Furthermore, the sequence characteristics for such association are distinct for different groups of histone marks.

CONCLUSIONS

These findings provide evidence of an influence of genomic sequence on patterns of histone modification associated with gene expression and chromatin programming, and they suggest that the mechanisms responsible for global histone modifications may interpret genomic sequence in various ways.

摘要

背景

组蛋白变体和修饰的组合,概念上代表了一个组蛋白密码,被认为在复杂生物的基因调控和发育过程中发挥着重要作用。虽然各种机制都被认为与在基因组的特定位置建立和维持表观遗传模式有关,但在更广泛的范围内,它们通常被认为是独立于原始 DNA 序列的。

结果

为了在人类基因组的情况下系统地解决这个问题,我们分析了人类原代 T 细胞中 19 种不同甲基化组蛋白模式和其他人类细胞系中 3 种甲基化组蛋白模式下的原始 DNA 序列。我们报告了在每种细胞类型中,这些组蛋白标记的全基因组范围内都存在强烈的序列偏倚。此外,不同组蛋白标记的这种关联的序列特征也不同。

结论

这些发现为基因组序列对与基因表达和染色质编程相关的组蛋白修饰模式的影响提供了证据,并表明负责全局组蛋白修饰的机制可能以各种方式解释基因组序列。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7729/3532361/9bdf56ec30bf/1471-2164-13-367-1.jpg

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