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巴氏小体中较高浓度的组蛋白macroH2A与较高的核小体密度相关。

Higher concentrations of histone macroH2A in the Barr body are correlated with higher nucleosome density.

作者信息

Perche P Y, Vourc'h C, Konecny L, Souchier C, Robert-Nicoud M, Dimitrov S, Khochbin S

机构信息

Equipe, DyOGen, Institut Albert Bonniot, Faculté de Médecine, et Laboratoire de Biologie Moléculaire et Cellulaire de la Différenciation, INSERM U309, Domaine de la Merci, 38706,., La Tronche Cedex, France.

出版信息

Curr Biol. 2000 Nov 30;10(23):1531-4. doi: 10.1016/s0960-9822(00)00832-0.

Abstract

Histone macroH2A, which is a subtype of histone H2A, possesses a histone H2A-like portion fused to a relatively long non-histone portion. MacroH2A has been shown to associate preferentially with the inactive X chromosome [1]. To investigate the specificity of this association, the nuclear distribution of macroH2A was compared with that of regular core histones. In normal human female fibroblasts, all anti-histone antibodies that were tested (including anti-macroH2A antibody) preferentially labeled the inactive X chromosome. Moreover, when expressed as green fluorescent protein (GFP) fusions, both histone H2A and macroH2A were concentrated in the Barr body. These data clearly show the presence of a higher density of nucleosomes in the inactive X chromosome. Accordingly, the specificity of the macroH2A association with the inactive X chromosome should be reconsidered. While investigating the role of macroH2A, we found that the proximity of the non-histone region of macroH2A to a promoter could lead to a specific repression of transcription, suggesting that the incorporation of macroH2A into chromatin might help to establish the stable pattern of gene expression in differentiated cells.

摘要

组蛋白macroH2A是组蛋白H2A的一种亚型,它具有一个与相对较长的非组蛋白部分融合的类组蛋白H2A部分。MacroH2A已被证明优先与失活的X染色体相关联[1]。为了研究这种关联的特异性,将macroH2A的核分布与常规核心组蛋白的核分布进行了比较。在正常人类女性成纤维细胞中,所有测试的抗组蛋白抗体(包括抗macroH2A抗体)都优先标记失活的X染色体。此外,当作为绿色荧光蛋白(GFP)融合蛋白表达时,组蛋白H2A和macroH2A都集中在巴氏小体中。这些数据清楚地表明失活的X染色体中存在更高密度的核小体。因此,应重新考虑macroH2A与失活X染色体关联的特异性。在研究macroH2A的作用时,我们发现macroH2A的非组蛋白区域靠近启动子可能导致转录的特异性抑制,这表明将macroH2A整合到染色质中可能有助于在分化细胞中建立稳定的基因表达模式。

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