首页> 美国卫生研究院文献>Molecular and Cellular Biology >Surprising deficiency of CENP-B binding sites in African green monkey alpha-satellite DNA: implications for CENP-B function at centromeres.
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Surprising deficiency of CENP-B binding sites in African green monkey alpha-satellite DNA: implications for CENP-B function at centromeres.

机译:非洲绿猴α-卫星DNA中CENP-B结合位点的惊人不足:对着丝粒处CENP-B功能的影响。

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摘要

Centromeres of mammalian chromosomes are rich in repetitive DNAs that are packaged into specialized nucleoprotein structures called heterochromatin. In humans, the major centromeric repetitive DNA, alpha-satellite DNA, has been extensively sequenced and shown to contain binding sites for CENP-B, an 80-kDa centromeric autoantigen. The present report reveals that African green monkey (AGM) cells, which contain extensive alpha-satellite arrays at centromeres, appear to lack the well-characterized CENP-B binding site (the CENP-B box). We show that AGM cells express a functional CENP-B homolog that binds to the CENP-B box and is recognized by several independent anti-CENP-B antibodies. However, three independent assays fail to reveal CENP-B binding sites in AGM DNA. Methods used include a gel mobility shift competition assay using purified AGM alpha-satellite, a novel kinetic electrophoretic mobility shift assay competition protocol using bulk genomic DNA, and bulk sequencing of 76 AGM alpha-satellite monomers. Immunofluorescence studies reveal the presence of significant levels of CENP-B antigen dispersed diffusely throughout the nuclei of interphase cells. These experiments reveal a paradox. CENP-B is highly conserved among mammals, yet its DNA binding site is conserved in human and mouse genomes but not in the AGM genome. One interpretation of these findings is that the role of CENP-B may be in the maintenance and/or organization of centromeric satellite DNA arrays rather than a more direct involvement in centromere structure.
机译:哺乳动物染色体的着丝粒富含重复的DNA,这些DNA被包装成称为异染色质的特殊核蛋白结构。在人类中,主要的着丝粒重复DNA(α-卫星DNA)已被广泛测序,并显示含有CENP-B(一种80 kDa着丝粒自身抗原)的结合位点。本报告显示,非洲绿猴(AGM)细胞在着丝粒处含有大量的α卫星阵列,似乎缺乏特征明确的CENP-B结合位点(CENP-B框)。我们显示,AGM细胞表达与CENP-B盒结合并被几种独立的抗CENP-B抗体识别的功能性CENP-B同源物。但是,三个独立的测定未能揭示AGM DNA中的CENP-B结合位点。所使用的方法包括使用纯化的AGMα-卫星的凝胶迁移率竞争分析,使用整体基因组DNA的新型动力学电泳迁移率竞争分析方案以及76种AGMα-卫星单体的序列测序。免疫荧光研究表明,存在大量的CENP-B抗原弥散分布在整个相间细胞核中。这些实验揭示了一个悖论。 CENP-B在哺乳动物中是高度保守的,但其DNA结合位点在人和小鼠基因组中却是保守的,而在AGM基因组中却没有。这些发现的一种解释是,CENP-B的作用可能在于着丝粒卫星DNA阵列的维持和/或组织,而不是更直接地参与着丝粒结构。

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