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人类 CTC1 可促进 TopBP1 的稳定性和 CHK1 的磷酸化,以响应端粒功能障碍和整体复制应激。

Human CTC1 promotes TopBP1 stability and CHK1 phosphorylation in response to telomere dysfunction and global replication stress.

机构信息

Department of Biological Sciences, University of South Carolina , Columbia, SC, USA.

出版信息

Cell Cycle. 2020 Dec;19(24):3491-3507. doi: 10.1080/15384101.2020.1849979. Epub 2020 Dec 3.


DOI:10.1080/15384101.2020.1849979
PMID:33269665
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7781613/
Abstract

CST (CTC1-STN1-TEN1) is a heterotrimeric, RPA-like complex that binds to single-stranded DNA (ssDNA) and functions in the replication of telomeric and non-telomeric DNA. Previous studies demonstrated that deletion of CTC1 results in decreased cell proliferation and telomere DNA damage signaling. However, a detailed analysis of the consequences of conditional CTC1 knockout (KO) has not been fully elucidated. Here, we investigated the effects of CTC1 KO on cell cycle progression, genome-wide replication and activation of the DNA damage response. Consistent with previous findings, we demonstrate that CTC1 KO results in decreased cell proliferation, G2 arrest and RPA-bound telomeric ssDNA. However, despite the increased levels of telomeric RPA-ssDNA, global ATR-dependent CHK1 and p53 phosphorylation was not detected in CTC1 KO cells. Nevertheless, we show that RPA-ssDNA does activate ATR, leading to the phosphorylation of RPA and autophosphorylation of ATR. Further analysis determined that inactivation of ATR, but not CHK1 or ATM, suppressed the accumulation of G2 arrested cells and phosphorylated RPA following CTC1 removal. These results suggest that ATR is localized and active at telomeres but is unable to elicit a global checkpoint response through CHK1. Furthermore, CTC1 KO inhibited CHK1 phosphorylation following hydroxyurea-induced replication stress. Additional studies revealed that this suppression of CHK1 phosphorylation, following replication stress, is caused by decreased levels of the ATR activator TopBP1. Overall, our results identify CST as a novel regulator of the ATR-CHK1 pathway.

摘要

CST(CTC1-STN1-TEN1)是一种三聚体、RPA 样复合物,可与单链 DNA(ssDNA)结合,并在端粒和非端粒 DNA 的复制中发挥作用。先前的研究表明,CTC1 的缺失会导致细胞增殖减少和端粒 DNA 损伤信号。然而,对条件性 CTC1 敲除(KO)的后果的详细分析尚未完全阐明。在这里,我们研究了 CTC1 KO 对细胞周期进程、全基因组复制和 DNA 损伤反应激活的影响。与先前的发现一致,我们证明 CTC1 KO 导致细胞增殖减少、G2 期阻滞和 RPA 结合的端粒 ssDNA。然而,尽管端粒 RPA-ssDNA 水平增加,但在 CTC1 KO 细胞中未检测到全基因组 ATR 依赖性 CHK1 和 p53 磷酸化。尽管如此,我们表明 RPA-ssDNA 确实激活了 ATR,导致 RPA 的磷酸化和 ATR 的自磷酸化。进一步的分析确定,ATR 的失活,而不是 CHK1 或 ATM,抑制了 CTC1 去除后 G2 期阻滞细胞和磷酸化 RPA 的积累。这些结果表明,ATR 定位于端粒并具有活性,但无法通过 CHK1 引发全基因组检查点反应。此外,CST KO 抑制了羟基脲诱导的复制应激后 CHK1 的磷酸化。进一步的研究表明,这种复制应激后 CHK1 磷酸化的抑制是由于 ATR 激活剂 TopBP1 水平降低所致。总的来说,我们的结果确定 CST 是 ATR-CHK1 通路的新型调节剂。

相似文献

[1]
Human CTC1 promotes TopBP1 stability and CHK1 phosphorylation in response to telomere dysfunction and global replication stress.

Cell Cycle. 2020-12

[2]
Reconstitution of RPA-covered single-stranded DNA-activated ATR-Chk1 signaling.

Proc Natl Acad Sci U S A. 2010-6-28

[3]
CST in maintaining genome stability: Beyond telomeres.

DNA Repair (Amst). 2021-6

[4]
Protection of telomeres 1 proteins POT1a and POT1b can repress ATR signaling by RPA exclusion, but binding to CST limits ATR repression by POT1b.

J Biol Chem. 2018-8-6

[5]
Overexpression of TopBP1, a canonical ATR/Chk1 activator, paradoxically hinders ATR/Chk1 activation in cancer.

J Biol Chem. 2021

[6]
TERRA and hnRNPA1 orchestrate an RPA-to-POT1 switch on telomeric single-stranded DNA.

Nature. 2011-3-13

[7]
RPA-coated single-stranded DNA promotes the ETAA1-dependent activation of ATR.

Cell Cycle. 2019-4-12

[8]
RHINO forms a stoichiometric complex with the 9-1-1 checkpoint clamp and mediates ATR-Chk1 signaling.

Cell Cycle. 2015

[9]
Tethering DNA damage checkpoint mediator proteins topoisomerase IIbeta-binding protein 1 (TopBP1) and Claspin to DNA activates ataxia-telangiectasia mutated and RAD3-related (ATR) phosphorylation of checkpoint kinase 1 (Chk1).

J Biol Chem. 2011-4-18

[10]
ATRIP binding to replication protein A-single-stranded DNA promotes ATR-ATRIP localization but is dispensable for Chk1 phosphorylation.

Mol Biol Cell. 2005-5

引用本文的文献

[1]
CTC1-STN1-TEN1 controls DNA break repair pathway choice via DNA end resection blockade.

Science. 2025-5-22

[2]
Telomere maintenance and the DNA damage response: a paradoxical alliance.

Front Cell Dev Biol. 2024-10-17

[3]
Suppression of CTC1 inhibits hepatocellular carcinoma cell growth and enhances RHPS4 cytotoxicity.

Mol Biol Rep. 2024-7-13

[4]
Human CST Stimulates Base Excision Repair to Prevent the Accumulation of Oxidative DNA Damage.

J Mol Biol. 2024-8-15

[5]
Guardians of the Genome: How the Single-Stranded DNA-Binding Proteins RPA and CST Facilitate Telomere Replication.

Biomolecules. 2024-2-22

[6]
Human CST complex restricts excessive PrimPol repriming upon UV induced replication stress by suppressing p21.

Nucleic Acids Res. 2024-4-24

[7]
Poly(ADP-Ribose) Polymerase-1 Lacking Enzymatic Activity Is Not Compatible with Mouse Development.

Cells. 2023-8-16

[8]
Cooperative interaction of CST and RECQ4 resolves G-quadruplexes and maintains telomere stability.

EMBO Rep. 2023-9-6

[9]
Deficiency in mammalian STN1 promotes colon cancer development via inhibiting DNA repair.

Sci Adv. 2023-5-10

[10]
Cis- and trans-resveratrol have opposite effects on histone serine-ADP-ribosylation and tyrosine induced neurodegeneration.

Nat Commun. 2022-6-10

本文引用的文献

[1]
CK2 kinase-mediated PHF8 phosphorylation controls TopBP1 stability to regulate DNA replication.

Nucleic Acids Res. 2020-11-4

[2]
The structure of human CST reveals a decameric assembly bound to telomeric DNA.

Science. 2020-6-5

[3]
Targeting ATR as Cancer Therapy: A new era for synthetic lethality and synergistic combinations?

Pharmacol Ther. 2019-12-11

[4]
Direct Visualization of DNA Replication at Telomeres Using DNA Fiber Combing Combined with Telomere FISH.

Methods Mol Biol. 2019

[5]
Human CST suppresses origin licensing and promotes AND-1/Ctf4 chromatin association.

Life Sci Alliance. 2019-4-12

[6]
Mammalian CST averts replication failure by preventing G-quadruplex accumulation.

Nucleic Acids Res. 2019-6-4

[7]
RPA-coated single-stranded DNA promotes the ETAA1-dependent activation of ATR.

Cell Cycle. 2019-4-12

[8]
Common motifs in ETAA1 and TOPBP1 required for ATR kinase activation.

J Biol Chem. 2019-4-2

[9]
Quantitative phosphoproteomics reveals mitotic function of the ATR activator ETAA1.

J Cell Biol. 2019-2-12

[10]
An intrinsic S/G checkpoint enforced by ATR.

Science. 2018-8-24

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