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曲古抑菌素A诱导的组蛋白乙酰化导致间期染色质解聚。

Trichostatin A-induced histone acetylation causes decondensation of interphase chromatin.

作者信息

Tóth Katalin Fejes, Knoch Tobias A, Wachsmuth Malte, Frank-Stöhr Monika, Stöhr Michael, Bacher Christian P, Müller Gabriele, Rippe Karsten

机构信息

Kirchhoff-Institut für Physik, AG Molekulare Biophysik, Ruprecht-Karls-Universität Heidelberg, Im Neuenheimer Feld 227, 69120 Heidelberg, Germany.

出版信息

J Cell Sci. 2004 Aug 15;117(Pt 18):4277-87. doi: 10.1242/jcs.01293. Epub 2004 Aug 3.

Abstract

The effect of trichostatin A (TSA)-induced histone acetylation on the interphase chromatin structure was visualized in vivo with a HeLa cell line stably expressing histone H2A, which was fused to enhanced yellow fluorescent protein. The globally increased histone acetylation caused a reversible decondensation of dense chromatin regions and led to a more homogeneous distribution. These structural changes were quantified by image correlation spectroscopy and by spatially resolved scaling analysis. The image analysis revealed that a chromatin reorganization on a length scale from 200 nm to >1 microm was induced consistent with the opening of condensed chromatin domains containing several Mb of DNA. The observed conformation changes could be assigned to the folding of chromatin during G1 phase by characterizing the effect of TSA on cell cycle progression and developing a protocol that allowed the identification of G1 phase cells on microscope coverslips. An analysis by flow cytometry showed that the addition of TSA led to a significant arrest of cells in S phase and induced apoptosis. The concentration dependence of both processes was studied.

摘要

利用稳定表达与增强型黄色荧光蛋白融合的组蛋白H2A的HeLa细胞系,在体内观察了曲古抑菌素A(TSA)诱导的组蛋白乙酰化对间期染色质结构的影响。整体组蛋白乙酰化增加导致致密染色质区域可逆性解聚,并导致分布更加均匀。通过图像相关光谱法和空间分辨标度分析对这些结构变化进行了量化。图像分析表明,诱导了从200纳米到大于1微米长度尺度的染色质重组,这与包含数兆碱基DNA的浓缩染色质结构域的开放一致。通过表征TSA对细胞周期进程的影响并开发一种能够在显微镜盖玻片上识别G1期细胞的方案,观察到的构象变化可归因于G1期染色质的折叠。流式细胞术分析表明,添加TSA导致细胞在S期显著停滞并诱导凋亡。研究了这两个过程的浓度依赖性。

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