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人类起源识别复合物对于 HP1 与染色质的结合和异染色质的组织至关重要。

Human origin recognition complex is essential for HP1 binding to chromatin and heterochromatin organization.

机构信息

Cold Spring Harbor Laboratory, Cold Spring Harbor, NY 11724, USA.

出版信息

Proc Natl Acad Sci U S A. 2010 Aug 24;107(34):15093-8. doi: 10.1073/pnas.1009945107. Epub 2010 Aug 5.

Abstract

The origin recognition complex (ORC) is a DNA replication initiator protein also known to be involved in diverse cellular functions including gene silencing, sister chromatid cohesion, telomere biology, heterochromatin localization, centromere and centrosome activity, and cytokinesis. We show that, in human cells, multiple ORC subunits associate with hetereochromatin protein 1 (HP1) alpha- and HP1beta-containing heterochromatic foci. Fluorescent bleaching studies indicate that multiple subcomplexes of ORC exist at heterochromatin, with Orc1 stably associating with heterochromatin in G1 phase, whereas other ORC subunits have transient interactions throughout the cell-division cycle. Both Orc1 and Orc3 directly bind to HP1alpha, and two domains of Orc3, a coiled-coil domain and a mod-interacting region domain, can independently bind to HP1alpha; however, both are essential for in vivo localization of Orc3 to heterochromatic foci. Direct binding of both Orc1 and Orc3 to HP1 suggests that, after the degradation of Orc1 at the G1/S boundary, Orc3 facilitates assembly of ORC/HP1 proteins to chromatin. Although depletion of Orc2 and Orc3 subunits by siRNA caused loss of HP1alpha association to heterochromatin, loss of Orc1 and Orc5 caused aberrant HP1alpha distribution only to pericentric heterochromatin-surrounding nucleoli. Depletion of HP1alpha from human cells also shows loss of Orc2 binding to heterochromatin, suggesting that ORC and HP1 proteins are mutually required for each other to bind to heterochromatin. Similar to HP1alpha-depleted cells, Orc2 and Orc3 siRNA-treated cells also show loss of compaction at satellite repeats, suggesting that ORC together with HP1 proteins may be involved in organizing higher-order chromatin structure and centromere function.

摘要

原点识别复合物(ORC)是一种 DNA 复制起始蛋白,也被认为参与多种细胞功能,包括基因沉默、姐妹染色单体粘连、端粒生物学、异染色质定位、着丝粒和中心体活性以及胞质分裂。我们表明,在人类细胞中,多个 ORC 亚基与异染色质蛋白 1(HP1)alpha 和包含 HP1beta 的异染色质焦点结合。荧光漂白研究表明,ORC 的多个亚基存在于异染色质中,Orc1 在 G1 期稳定地与异染色质结合,而其他 ORC 亚基在整个细胞分裂周期中具有短暂的相互作用。Orc1 和 Orc3 都直接与 HP1alpha 结合,并且 Orc3 的两个结构域,一个卷曲螺旋结构域和一个与调节蛋白相互作用的结构域,可以独立地与 HP1alpha 结合;然而,两者对于 Orc3 在异染色质焦点中的体内定位都是必需的。Orc1 和 Orc3 与 HP1 的直接结合表明,在 G1/S 边界处 Orc1 降解后,Orc3 有助于 ORC/HP1 蛋白组装到染色质上。尽管 siRNA 耗尽 Orc2 和 Orc3 亚基会导致 HP1alpha 与异染色质的关联丧失,但 Orc1 和 Orc5 的缺失仅导致异常的 HP1alpha 分布在着丝粒周围异染色质-核仁周围。从人类细胞中耗尽 HP1alpha 也会导致 Orc2 与异染色质的结合丧失,这表明 ORC 和 HP1 蛋白相互需要才能与异染色质结合。与 HP1alpha 耗尽的细胞相似,Orc2 和 Orc3 siRNA 处理的细胞也显示卫星重复序列的压缩丧失,这表明 ORC 与 HP1 蛋白一起可能参与组织更高阶的染色质结构和着丝粒功能。

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