Department of Oncology, University of Alberta, Edmonton, T6G 1Z2 Alberta, Canada.
J Cell Biol. 2010 Oct 4;191(1):45-60. doi: 10.1083/jcb.201003034.
Polycomb group (PcG) proteins are major determinants of cell identity, stem cell pluripotency, and epigenetic gene silencing during development. The polycomb repressive complex 1, which contains BMI1, RING1, and RING2, functions as an E3-ubuiquitin ligase. We found that BMI1 and RING2 are recruited to sites of DNA double-strand breaks (DSBs) where they contribute to the ubiquitylation of γ-H2AX. In the absence of BMI1, several proteins dependent on ubiquitin signaling, including 53BP1, BRCA1, and RAP80, are impaired in recruitment to DSBs. Loss of BMI1 sensitizes cells to ionizing radiation to the same extent as loss of RNF8. The simultaneous depletion of both proteins revealed an additive increase in radiation sensitivity. These data uncover an unexpected link between the polycomb and the DNA damage response pathways, and suggest a novel function for BMI1 in maintaining genomic stability.
多梳抑制复合物(PcG)蛋白是细胞特性、干细胞多能性和发育过程中表观遗传基因沉默的主要决定因素。包含 BMI1、RING1 和 RING2 的多梳抑制复合物 1 作为 E3-泛素连接酶发挥作用。我们发现 BMI1 和 RING2 被招募到 DNA 双链断裂 (DSB) 部位,在那里它们有助于 γ-H2AX 的泛素化。在没有 BMI1 的情况下,几种依赖于泛素信号的蛋白质,包括 53BP1、BRCA1 和 RAP80,在招募到 DSB 方面受到损害。BMI1 的缺失使细胞对电离辐射的敏感性与 RNF8 的缺失相同。两种蛋白的同时耗尽显示出辐射敏感性的累加增加。这些数据揭示了多梳和 DNA 损伤反应途径之间的意外联系,并表明 BMI1 在维持基因组稳定性方面具有新的功能。
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