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DNA 修复蛋白 XRCC1 在微分离条件下刺激 DNA 聚合酶 λ 的活性。

DNA Repair Protein XRCC1 Stimulates Activity of DNA Polymerase λ under Conditions of Microphase Separation.

机构信息

Institute of Chemical Biology and Fundamental Medicine (ICBFM), Siberian Branch of the Russian Academy of Sciences (SB RAS), Novosibirsk 630090, Russia.

出版信息

Int J Mol Sci. 2024 Jun 25;25(13):6927. doi: 10.3390/ijms25136927.

Abstract

Non-membrane compartments or biomolecular condensates play an important role in the regulation of cellular processes including DNA repair. Here, an ability of XRCC1, a scaffold protein involved in DNA base excision repair (BER) and single-strand break repair, to form protein-rich microphases in the presence of DNA duplexes was discovered. We also showed that the gap-filling activity of BER-related DNA polymerase λ (Pol λ) is significantly increased by the presence of XRCC1. The stimulation of the Pol λ activity was observed only at micromolar XRCC1 concentrations, which were well above the nanomolar dissociation constant determined for the XRCC1-Pol λ complex and pointed to the presence of an auxiliary stimulatory factor in addition to protein-protein interactions. Indeed, according to dynamic light scattering measurements, the stimulation of the Pol λ activity by XRCC1 was coupled with microphase separation in a protein-DNA mixture. Fluorescence microscopy revealed colocalization of Pol λ, XRCC1, and gapped DNA within the microphases. Thus, stimulation of Pol λ activity is caused both by its interaction with XRCC1 and by specific conditions of microphase separation; this phenomenon is shown for the first time.

摘要

非膜隔间或生物分子凝聚物在调节细胞过程中起着重要作用,包括 DNA 修复。在这里,发现了参与 DNA 碱基切除修复 (BER) 和单链断裂修复的支架蛋白 XRCC1 在存在 DNA 双链体时形成富含蛋白质的微区的能力。我们还表明,BER 相关 DNA 聚合酶 λ (Pol λ) 的缺口填充活性通过 XRCC1 的存在而显著增加。仅在微摩尔 XRCC1 浓度下观察到 Pol λ 活性的刺激,这远高于确定的 XRCC1-Pol λ 复合物的纳摩尔解离常数,表明除了蛋白质-蛋白质相互作用之外,还存在辅助刺激因子。事实上,根据动态光散射测量,XRCC1 对 Pol λ 活性的刺激与蛋白质-DNA 混合物中的微相分离相关联。荧光显微镜显示 Pol λ、XRCC1 和缺口 DNA 在微区内共定位。因此,Pol λ 活性的刺激既是由其与 XRCC1 的相互作用引起的,也是由微相分离的特定条件引起的;这种现象是首次被展示。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/30f6/11241748/23dab9215133/ijms-25-06927-g001.jpg

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