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The MRE11–RAD50–NBS1 Complex Conducts the Orchestration of Damage Signaling and Outcomes to Stress in DNA Replication and Repair
Annual Review of Biochemistry ( IF 12.1 ) Pub Date : 2018-06-20 00:00:00 , DOI: 10.1146/annurev-biochem-062917-012415
Aleem Syed 1 , John A Tainer 1, 2
Affiliation  

Genomic instability in disease and its fidelity in health depend on the DNA damage response (DDR), regulated in part from the complex of meiotic recombination 11 homolog 1 (MRE11), ATP-binding cassette–ATPase (RAD50), and phosphopeptide-binding Nijmegen breakage syndrome protein 1 (NBS1). The MRE11–RAD50–NBS1 (MRN) complex forms a multifunctional DDR machine. Within its network assemblies, MRN is the core conductor for the initial and sustained responses to DNA double-strand breaks, stalled replication forks, dysfunctional telomeres, and viral DNA infection. MRN can interfere with cancer therapy and is an attractive target for precision medicine. Its conformations change the paradigm whereby kinases initiate damage sensing. Delineated results reveal kinase activation, posttranslational targeting, functional scaffolding, conformations storing binding energy and enabling access, interactions with hub proteins such as replication protein A (RPA), and distinct networks at DNA breaks and forks. MRN biochemistry provides prototypic insights into how it initiates, implements, and regulates multifunctional responses to genomic stress.

中文翻译:



MRE11–RAD50–NBS1 复合物协调 DNA 复制和修复过程中的损伤信号传导和应激结果



疾病中的基因组不稳定性及其在健康中的保真度取决于 DNA 损伤反应 (DDR),部分由减数分裂重组 11 同源物 1 (MRE11)、ATP 结合盒 - ATP 酶 (RAD50) 和磷酸肽结合奈梅亨复合体调节断裂综合征蛋白 1 (NBS1)。 MRE11–RAD50–NBS1 (MRN) 复合体构成了多功能 DDR 机器。在其网络组件中,MRN 是对 DNA 双链断裂、复制叉停滞、端粒功能失调和病毒 DNA 感染进行初始和持续反应的核心导体。 MRN 会干扰癌症治疗,是精准医学的一个有吸引力的目标。它的构象改变了激酶启动损伤感知的范式。描绘的结果揭示了激酶激活、翻译后靶向、功能支架、存储结合能和实现访问的构象、与复制蛋白 A (RPA) 等中心蛋白的相互作用,以及 DNA 断裂和分叉处的独特网络。 MRN 生物化学提供了关于它如何启动、实施和调节对基因组应激的多功能反应的原型见解。

更新日期:2018-06-20
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