DBF4 而不是 DRF1 是复制叉上 CDC7 激酶的关键调节因子。

IF 7.4 1区 生物学 Q1 CELL BIOLOGY
Journal of Cell Biology Pub Date : 2024-08-05 Epub Date: 2024-06-12 DOI:10.1083/jcb.202402144
Anja Göder, Chrystelle Antoinat Maric, Michael D Rainey, Aisling O'Connor, Chiara Cazzaniga, Daniel Shamavu, Jean-Charles Cadoret, Corrado Santocanale
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引用次数: 0

摘要

CDC7 激酶对 DNA 复制的启动至关重要,并参与叉处理和复制应激反应。人类 CDC7 的活性需要与 DBF4 或 DRF1 结合。然而,目前还不清楚这两个调控亚基是将 CDC7 定位于一组特定的底物,从而具有不同的生物学功能,还是它们的作用是多余的。利用基因组编辑技术,我们生成了缺乏 DBF4 或 DRF1 的同源细胞系:这些细胞可以存活,但有基因组不稳定的迹象,表明它们都能独立支持 CDC7 进行大量 DNA 复制。然而,DBF4 缺陷细胞显示出复制效率的改变、MCM 螺旋酶磷酸化的部分缺陷以及离散基因组区域复制时间的改变。值得注意的是,我们发现 CDC7 在复制叉上的功能完全依赖于 DBF4 而不是 DRF1。因此,DBF4 是 CDC7 活性的主要调节因子,在未受干扰的 DNA 复制和复制干扰时介导 CDC7 的大部分功能。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
DBF4, not DRF1, is the crucial regulator of CDC7 kinase at replication forks.

CDC7 kinase is crucial for DNA replication initiation and is involved in fork processing and replication stress response. Human CDC7 requires the binding of either DBF4 or DRF1 for its activity. However, it is unclear whether the two regulatory subunits target CDC7 to a specific set of substrates, thus having different biological functions, or if they act redundantly. Using genome editing technology, we generated isogenic cell lines deficient in either DBF4 or DRF1: these cells are viable but present signs of genomic instability, indicating that both can independently support CDC7 for bulk DNA replication. Nonetheless, DBF4-deficient cells show altered replication efficiency, partial deficiency in MCM helicase phosphorylation, and alterations in the replication timing of discrete genomic regions. Notably, we find that CDC7 function at replication forks is entirely dependent on DBF4 and not on DRF1. Thus, DBF4 is the primary regulator of CDC7 activity, mediating most of its functions in unperturbed DNA replication and upon replication interference.

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来源期刊
Journal of Cell Biology
Journal of Cell Biology 生物-细胞生物学
CiteScore
12.60
自引率
2.60%
发文量
213
审稿时长
1 months
期刊介绍: The Journal of Cell Biology (JCB) is a comprehensive journal dedicated to publishing original discoveries across all realms of cell biology. We invite papers presenting novel cellular or molecular advancements in various domains of basic cell biology, along with applied cell biology research in diverse systems such as immunology, neurobiology, metabolism, virology, developmental biology, and plant biology. We enthusiastically welcome submissions showcasing significant findings of interest to cell biologists, irrespective of the experimental approach.
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