Functional and molecular insights into the role of Sae2 C-terminus in the activation of MRX endonuclease.

IF 16.6 2区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Chiara Vittoria Colombo, Erika Casari, Marco Gnugnoli, Flavio Corallo, Renata Tisi, Maria Pia Longhese
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引用次数: 0

Abstract

The yeast Sae2 protein, known as CtIP in mammals, once phosphorylated at Ser267, stimulates the endonuclease activity of the Mre11-Rad50-Xrs2 (MRX) complex to cleave DNA ends that possess hairpin structures or protein blocks, such as the Spo11 transesterase or trapped topoisomerases. Stimulation of the Mre11 endonuclease by Sae2 depends on a Rad50-Sae2 interaction, but the mechanism by which this is achieved remains to be elucidated. Through genetic studies, we show that the absence of the last 23 amino acids from the Sae2 C-terminus specifically impairs MRX-dependent DNA cleavage events, while preserving the other Sae2 functions. Employing AlphaFold3 protein structure predictions, we found that the Rad50-Sae2 interface involves not only phosphorylated Ser267 but also the phosphorylated Thr279 residue and the C-terminus of Sae2. This region engages in multiple interactions with residues that are mutated in rad50-s mutants, which are known to be specifically defective in the processing of Spo11-bound DNA ends. These interactions are critical for stabilizing the association between Sae2 and Rad50, thereby ensuring the correct positioning of Mre11 in its active endonucleolytic state.

对 Sae2 C 端在激活 MRX 内切酶中的作用的功能和分子见解。
酵母 Sae2 蛋白(在哺乳动物中称为 CtIP)一旦在 Ser267 处磷酸化,就会刺激 Mre11-Rad50-Xrs2 (MRX)复合物的内切酶活性,从而裂解具有发夹结构或蛋白块(如 Spo11 转酯酶或被困的拓扑异构酶)的 DNA 末端。Sae2对Mre11内切酶的刺激依赖于Rad50-Sae2的相互作用,但这种作用的机制仍有待阐明。通过基因研究,我们发现 Sae2 C 端最后 23 个氨基酸的缺失会特异性地损害 MRX 依赖性 DNA 裂解事件,同时保留 Sae2 的其他功能。利用 AlphaFold3 蛋白结构预测,我们发现 Rad50-Sae2 界面不仅涉及磷酸化的 Ser267,还涉及磷酸化的 Thr279 残基和 Sae2 的 C-端。该区域与在 rad50-s 突变体中发生突变的残基发生了多种相互作用,众所周知,这些突变体在处理 Spo11 结合的 DNA 末端时存在特异性缺陷。这些相互作用对于稳定 Sae2 和 Rad50 之间的结合至关重要,从而确保 Mre11 在其活性核酸内切状态下的正确定位。
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来源期刊
Nucleic Acids Research
Nucleic Acids Research 生物-生化与分子生物学
CiteScore
27.10
自引率
4.70%
发文量
1057
审稿时长
2 months
期刊介绍: Nucleic Acids Research (NAR) is a scientific journal that publishes research on various aspects of nucleic acids and proteins involved in nucleic acid metabolism and interactions. It covers areas such as chemistry and synthetic biology, computational biology, gene regulation, chromatin and epigenetics, genome integrity, repair and replication, genomics, molecular biology, nucleic acid enzymes, RNA, and structural biology. The journal also includes a Survey and Summary section for brief reviews. Additionally, each year, the first issue is dedicated to biological databases, and an issue in July focuses on web-based software resources for the biological community. Nucleic Acids Research is indexed by several services including Abstracts on Hygiene and Communicable Diseases, Animal Breeding Abstracts, Agricultural Engineering Abstracts, Agbiotech News and Information, BIOSIS Previews, CAB Abstracts, and EMBASE.
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