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首页> 外文期刊>Journal of biological inorganic chemistry: JBIC: a publication of the Society of Biological Inorganic Chemistry >Platination of telomeric DNA by cisplatin disrupts recognition by TRF2 and TRF1
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Platination of telomeric DNA by cisplatin disrupts recognition by TRF2 and TRF1

机译:顺铂端粒DNA的插入会破坏TRF2和TRF1的识别

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摘要

Telomeres, the nucleoprotein complexes located at the ends of chromosomes, are involved in chromosome protection and genome stability. Telomeric repeat binding factor 1 (TRF1) and telomeric repeat binding factor 2 (TRF2) are the two telomeric proteins that bind to duplex telomeric DNA through interactions between their C-terminal domain and several guanines of the telomeric tract. Since the antitumour drug cisplatin binds preferentially to two adjacent guanines, we have investigated whether cisplatin adducts could affect the binding of TRF1 and TRF2 to telomeric DNA and the property of TRF2 to stimulate telomeric invasion, a process that is thought to participate in the formation of the t-loop. We show that the binding of TRF1 and TRF2 to telomeric sequences selectively modified by one GG chelate of cisplatin is markedly affected by cisplatin but that the effect is more drastic for TRF2 than for TRF1 (3-5-fold more sensitivity for TRF2 than for TRF1). We also report that platinum adducts cause a decrease in TRF2-dependent stimulation of telomeric invasion in vitro. Finally, in accordance with in vitro data, analysis of telomeric composition after cisplatin treatment reveals that 60% of TRF2 dissociate from telomeres.
机译:端粒是位于染色体末端的核蛋白复合物,参与染色体保护和基因组稳定性。端粒重复结合因子1(TRF1)和端粒重复结合因子2(TRF2)是通过其C末端结构域和端粒的几个鸟嘌呤之间的相互作用与双链体端粒DNA结合的两个端粒蛋白。由于抗肿瘤药顺铂优先结合两个相邻的鸟嘌呤,我们研究了顺铂加合物是否会影响TRF1和TRF2与端粒DNA的结合以及TRF2刺激端粒入侵的特性,该过程被认为参与了端粒的形成。 T环。我们显示TRF1和TRF2绑定到由一个GG螯合物选择性修饰的端粒序列受顺铂显着影响,但对于TRF2的影响比对TRF1的影响更大(对TRF2的敏感性是对TRF1的3-5倍) )。我们还报告了铂加合物导致TRF2依赖的体外端粒入侵的刺激减少。最后,根据体外数据,顺铂处理后端粒组成的分析显示60%的TRF2与端粒解离。

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