Department of Biology, McMaster University, 1280 Main St. West Hamilton, ON, Canada L8S4K1.
Nucleic Acids Res. 2012 Oct;40(19):9661-74. doi: 10.1093/nar/gks745. Epub 2012 Aug 16.
The majority of Cockayne syndrome (CS) patients carry a mutation in Cockayne Syndrome group B (CSB), a large nuclear protein implicated in DNA repair, transcription and chromatin remodeling. However, whether CSB may play a role in telomere metabolism has not yet been characterized. Here, we report that CSB physically interacts with TRF2, a duplex telomeric DNA binding protein essential for telomere protection. We find that CSB localizes at a small subset of human telomeres and that it is required for preventing the formation of telomere dysfunction-induced foci (TIF) in CS cells. We find that CS cells or CSB knockdown cells accumulate telomere doublets, the suppression of which requires CSB. We find that overexpression of CSB in CS cells promotes telomerase-dependent telomere lengthening, a phenotype that is associated with a decrease in the amount of telomere-bound TRF1, a negative mediator of telomere length maintenance. Furthermore, we show that CS cells or CSB knockdown cells exhibit misregulation of TERRA, a large non-coding telomere repeat-containing RNA important for telomere maintenance. Taken together, these results suggest that CSB is required for maintaining the homeostatic level of TERRA, telomere length and integrity. These results further imply that CS patients carrying CSB mutations may be defective in telomere maintenance.
大多数 Cockayne 综合征(CS)患者携带 Cockayne 综合征 B 组(CSB)的突变,CSB 是一种与 DNA 修复、转录和染色质重塑相关的大型核蛋白。然而,CSB 是否可能在端粒代谢中发挥作用尚未得到表征。在这里,我们报告 CSB 与 TRF2 物理相互作用,TRF2 是一种双链端粒 DNA 结合蛋白,对端粒保护至关重要。我们发现 CSB 定位于人类端粒的一小部分,并且它对于防止 CS 细胞中端粒功能障碍诱导焦点(TIF)的形成是必需的。我们发现 CS 细胞或 CSB 敲低细胞积累端粒双链体,抑制 CSB 需要端粒双链体。我们发现 CSB 在 CS 细胞中的过表达促进了端粒酶依赖性端粒延长,这种表型与端粒结合的 TRF1 减少有关,TRF1 是端粒长度维持的负调节剂。此外,我们表明 CS 细胞或 CSB 敲低细胞表现出 TERRA 的失调,TERRA 是一种对端粒维持很重要的大型非编码端粒重复 RNA。总之,这些结果表明 CSB 是维持 TERRA、端粒长度和完整性的稳态水平所必需的。这些结果进一步表明,携带 CSB 突变的 CS 患者可能在端粒维持方面存在缺陷。
