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野生型和EC突变型多瘤病毒中起始近端DNA酶I超敏区域的精细结构

Fine structure of the origin-proximal DNAase I-hypersensitive region in wild-type and EC mutant polyoma.

作者信息

Herbomel P, Saragosti S, Blangy D, Yaniv M

出版信息

Cell. 1981 Sep;25(3):651-8. doi: 10.1016/0092-8674(81)90172-0.

Abstract

The chromatin of wild-type polyoma virus displays a unique DNAase I highly sensitive region in situ in the infected nuclei, extending for about 260 nucleotides from the origin of replication to the beginning of the late region. We show that this highly sensitive region is not homogeneous. It displays a well defined pattern of differential sensitivity along its 260 nucleotides, including one protected subregion and two hypersensitive sites, which concern a unique residue or very few nucleotides. All these features were mapped to a precision of +/- 5 bp relative to the DNA nucleotide sequence. In parallel, we studied a PyEC mutant, whose sequence is grossly rear-ranged in this very region. This allows the PyEC to overcome the block in the expression of the early genes in the mouse embryonal carcinoma PCC4 cell line. We show that this mutant, however, displays an identical highly sensitive region with the same fine structure. The mapping of this structure on the mutant nucleotides sequence coincides with that of the wild-type relative to any arbitrary point on the late side of the rearrangement; however, 60% of the mutant molecules display this unique local chromatin structure, instead of 20% for the wild-type ones. Finally, the sequence determinism of this singularity is discussed, as well as its possible role in the control of the early transcription and the establishment of the PyEC phenotype..

摘要

野生型多瘤病毒的染色质在受感染细胞核内原位显示出一个独特的对脱氧核糖核酸酶I高度敏感的区域,从复制起点延伸至晚期区域起始处约260个核苷酸。我们发现这个高度敏感区域并非均匀一致。它在其260个核苷酸上呈现出一种明确的差异敏感性模式,包括一个受保护的子区域和两个超敏位点,涉及一个独特的残基或极少的核苷酸。所有这些特征相对于DNA核苷酸序列的定位精度为±5个碱基对。同时,我们研究了一个PyEC突变体,其序列在这个特定区域有严重重排。这使得PyEC能够克服小鼠胚胎癌细胞系PCC4中早期基因表达的障碍。然而,我们发现这个突变体显示出与野生型相同的高度敏感区域以及相同的精细结构。相对于重排晚期的任意一个点,这种结构在突变体核苷酸序列上的定位与野生型的一致;然而,60%的突变体分子呈现出这种独特的局部染色质结构,而野生型只有20%。最后,讨论了这种独特性的序列决定性,以及它在早期转录调控和PyEC表型确立中可能发挥的作用。

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