Cancer Research Center of Toulouse, INSERM U1037, CNRS ERL5294, Université Paul Sabatier Toulouse III, Equipe labellisée Ligue Contre le Cancer, Laboratoire d'excellence Toulouse Cancer, Toulouse, France.
AP-HP, DRCI Hôpital Saint-Louis, Paris, France.
Mol Cell Biol. 2021 Oct 26;41(11):e0009021. doi: 10.1128/MCB.00090-21. Epub 2021 Aug 16.
DNA polymerase kappa (Pol κ) has been well documented thus far for its specialized DNA synthesis activity during translesion replication, progression of replication forks through regions difficult to replicate, restart of stalled forks, and replication checkpoint efficiency. Pol κ is also required for the stabilization of stalled forks, although the mechanisms are poorly understood. In this study, we unveiled an unexpected role for Pol κ in controlling the stability and abundance of checkpoint kinase 1 (Chk1), an important actor for the replication checkpoint and fork stabilization. We found that loss of Pol κ decreased the Chk1 protein level in the nuclei of four human cell lines. Pol κ and not the other Y family polymerase members is required to maintain the Chk1 protein pool all along the cell cycle. We showed that Pol κ depletion affected the protein stability of Chk1 and protected it from proteasome degradation. Importantly, we also observed that the fork restart defects observed in Pol κ-depleted cells could be overcome by the reexpression of Chk1. Strikingly, this new function of Pol κ does not require its catalytic activity. We propose that Pol κ could contribute to the protection of stalled forks through Chk1 stability.
DNA 聚合酶 κ(Pol κ)在跨损伤复制、复制叉通过难以复制的区域、复制叉的重新启动以及复制检查点效率等方面的特殊 DNA 合成活性方面得到了很好的研究。Pol κ 还需要稳定停滞的复制叉,尽管其机制尚不清楚。在这项研究中,我们揭示了 Pol κ 在控制检查点激酶 1(Chk1)的稳定性和丰度方面的一个意外作用,Chk1 是复制检查点和叉稳定的重要因子。我们发现,在四种人类细胞系中,Pol κ 的缺失会降低细胞核中的 Chk1 蛋白水平。Pol κ 而不是其他 Y 家族聚合酶成员,需要在整个细胞周期中维持 Chk1 蛋白库。我们表明,Pol κ 耗竭会影响 Chk1 的蛋白质稳定性,并保护其免受蛋白酶体降解。重要的是,我们还观察到在 Pol κ 耗尽的细胞中观察到的叉重新启动缺陷可以通过 Chk1 的重新表达来克服。引人注目的是,Pol κ 的这个新功能不要求其催化活性。我们提出,Pol κ 可以通过 Chk1 的稳定性来保护停滞的复制叉。
