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来自脆性X综合征患者的扩展CCG三联体重复DNA的甲基化增强了核小体排斥。

Methylation of expanded CCG triplet repeat DNA from fragile X syndrome patients enhances nucleosome exclusion.

作者信息

Wang Y H, Griffith J

机构信息

Lineberger Comprehensive Cancer Center, University of North Carolina, Chapel Hill, North Carolina 27599-7295, USA.

出版信息

J Biol Chem. 1996 Sep 20;271(38):22937-40.

PMID:8798475
Abstract

Long tracts of CCG trinucleotide or CCGNN pentanucleotide repeats in DNA have previously been shown to resist assembly into nucleosomes. This may provide a molecular explanation for the nature of certain rare, folate-sensitive fragile sites in human chromosomes that contain expanded CCG triplet tracts. Further, it is known that methylation of CpG dinucleotides at or near these fragile sites enhances the fragile phenotype. Here DNAs containing 76 tandem CCG triplets or 48 CCGNN pentanucleotide repeats were methylated with SssI methylase at three different levels of methylation. Using competitive nucleosome reconstitution/gel shift assays, the ability of these DNAs and a mixed sequence DNA from the pUC19 plasmid were compared in their ability to assemble into nucleosomes. DNA methylation had no significant effect on nucleosome formation over the pUC 19 fragment. However, the highly methylated DNAs containing 76 CCG triplets or 48 CCGNN pentanucleotide repeats were 2.0 +/- 0. 2-fold and 2.1 +/- 0.3-fold less efficient in nucleosome assembly than the respective unmethylated forms, and 4.4 +/- 0.4-fold and 12. 6 +/- 1.6-fold less efficient than a pUC19 fragment of similar length.

摘要

DNA中长片段的CCG三核苷酸或CCGNN五核苷酸重复序列先前已被证明难以组装成核小体。这可能为人类染色体中某些罕见的、对叶酸敏感的脆性位点的性质提供分子解释,这些位点包含扩展的CCG三联体序列。此外,已知这些脆性位点或其附近的CpG二核苷酸甲基化会增强脆性表型。在此,含有76个串联CCG三联体或48个CCGNN五核苷酸重复序列的DNA用SssI甲基转移酶进行了三种不同甲基化水平的甲基化。使用竞争性核小体重组/凝胶迁移试验,比较了这些DNA与来自pUC19质粒的混合序列DNA组装成核小体的能力。DNA甲基化对pUC19片段上的核小体形成没有显著影响。然而,含有76个CCG三联体或48个CCGNN五核苷酸重复序列的高度甲基化DNA在核小体组装中的效率分别比各自的未甲基化形式低2.0±0.2倍和2.1±0.3倍,比类似长度的pUC19片段低4.4±0.4倍和12.6±1.6倍。

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