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EMBO Journal

IF: 8.3
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FOXP1 phosphorylation antagonizes its O-GlcNAcylation in regulating ATR activation in response to replication stress

Published:1 January 2025 DOI: 10.1038/s44318-024-00323-x PMID: 39623140
Xuefei Zhu,?Congwen Gao,?Bin Peng,?Jingwei Xue,?Donghui Xia,?Liu Yang,?Jiexiang Zhang,?Xinrui Gao,?Yilin Hu,?Shixian Lin,?Peng Gong,?Xingzhi Xu

Abstract

ATR signaling is essential in sensing and responding to the replication stress; as such, any defects can impair cellular function and survival. ATR itself is activated via tightly regulated mechanisms. Here, we identify FOXP1, a forkhead-box-containing transcription factor, as a regulator coordinating ATR activation. We show that, unlike its role as a transcription factor, FOXP1 functions as a scaffold and directly binds to RPA-ssDNA and ATR-ATRIP complexes, facilitating the recruitment and activation of ATR. This process is regulated by FOXP1 O-GlcNAcylation, which represses its interaction with ATR, while CHK1-mediated phosphorylation of FOXP1 inhibits its O-GlcNAcylation upon replication stress. Supporting the physiological relevance of this loop, we find pathogenic FOXP1 mutants identified in various tumor tissues with compromised ATR activation and stalled replication fork stability. We thus conclude that FOXP1 may serve as a potential chemotherapeutic target in related tumors.

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Materials
Procduct Name CAS Molecular Formula Supplier Price
Broxuridine 59-14-3 C9H11BrN2O5 518 suppliers $7.00-$308338.00
Broxuridine 59-14-3 C9H11BrN2O5 518 suppliers $7.00-$308338.00
Broxuridine 59-14-3 C9H11BrN2O5 518 suppliers $7.00-$308338.00
Broxuridine 59-14-3 C9H11BrN2O5 518 suppliers $7.00-$308338.00

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