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DNA 四链体稳定性、位置和染色质可及性与 CpG 岛甲基化有关。

DNA G-quadruplex stability, position and chromatin accessibility are associated with CpG island methylation.

机构信息

Department of Morphology, Piracicaba Dental School, University of Campinas - UNICAMP, Piracicaba, Brazil.

出版信息

FEBS J. 2020 Feb;287(3):483-495. doi: 10.1111/febs.15065. Epub 2019 Sep 26.

Abstract

CpG islands (CGI) are genomic regions associated with gene promoters and involved in gene expression regulation. Despite their high CpG content and unlike bulk genomic DNA methylation pattern, these regions are usually hypomethylated. So far, the mechanisms controlling the CGI methylation patterning remain unclear. G-quadruplex (G4) structures can inhibit DNA methyltransferases 1 enzymatic activity, leading to CGI hypomethylation. Our aim was to analyse the association of G4 forming sequences (G4FS) and CGI methylation as well as to determine the intrinsic and extrinsic characteristics of G4FS that may modulate this phenomenon. Using methylation data from human embryonic stem cells (hESCs) and three hESC-derived populations, we showed that hypomethylated CpGs located inside CGI (CGI/CpG) tend to be associated with highly stable G4FS (Minimum free energy ≤ -30 kcal·mol ). The association of highly stable G4FS and hypomethylation tend to be stronger when these structures are located at shorter distances (~ < 150 bp) from GCI/CpGs, when G4FS and CpGs are located within open chromatin and G4FS are inside CGI. Moreover, this association is not strongly influenced by the CpG content of CGI. Conversely, highly methylated CGI/CpG tend to be associated with low stability G4FS. Although CpGs inside CGIs without a G4FS tend to be more methylated, high stability G4FS within CGI neighbourhood were associated with decreased methylation. In summary, our data indicate that G4FS may act as protective cis elements against CGI methylation, and this effect seems to be influenced by the G4FS folding potential, its presence within CGI, CpG distance from G4FS and chromatin accessibility.

摘要

CpG 岛(CGI)是与基因启动子相关的基因组区域,参与基因表达调控。尽管它们的 CpG 含量很高,但与基因组 DNA 整体甲基化模式不同,这些区域通常呈低甲基化状态。到目前为止,控制 CGI 甲基化模式的机制仍不清楚。四链体(G4)结构可以抑制 DNA 甲基转移酶 1 的酶活性,导致 CGI 低甲基化。我们的目的是分析 G4 形成序列(G4FS)与 CGI 甲基化的相关性,并确定可能调节这种现象的 G4FS 的内在和外在特征。我们使用人类胚胎干细胞(hESC)和三个 hESC 衍生群体的甲基化数据表明,位于 CGI 内的低甲基化 CpG(CGI/CpG)倾向于与高度稳定的 G4FS 相关(最小自由能≤-30 kcal·mol)。当这些结构距离 CGI/CpGs 较近(~<150 bp),G4FS 和 CpGs 位于开放染色质内,并且 G4FS 位于 CGI 内时,高度稳定的 G4FS 与低甲基化的相关性更强。此外,这种相关性不受 CGI 中 CpG 含量的强烈影响。相反,高度甲基化的 CGI/CpG 往往与低稳定性的 G4FS 相关。尽管 CGI 内没有 G4FS 的 CpGs 往往更容易甲基化,但 CGI 附近的高稳定性 G4FS 与降低的甲基化相关。总之,我们的数据表明,G4FS 可能作为 CGI 甲基化的保护性顺式元件,这种效应似乎受 G4FS 折叠潜力、其在 CGI 内的存在、与 G4FS 的 CpG 距离和染色质可及性的影响。

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