SND1 通过靶向 DNA 损伤反应促进宫颈癌细胞的抗放射能力

IF 10.1 1区 生物学 Q1 BIOTECHNOLOGY & APPLIED MICROBIOLOGY Genome Biology Pub Date : 2024-08-01 Epub Date: 2022-03-10 DOI:10.1089/cbr.2021.0371
Xiao Fu, Zhongchao Duan, Xin Lu, Yingyu Zhu, Yuanyuan Ren, Wei Zhang, Xiaoming Sun, Lin Ge, Jie Yang
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引用次数: 0

摘要

背景:放疗是宫颈癌患者最有效的治疗策略之一,但放射抗性介导的残留和复发肿瘤是治疗失败的主要原因。然而,肿瘤放射抗性的机制仍然难以捉摸。DNA 损伤反应途径是决定放射耐药性的关键因素。本研究旨在探讨 SND1 在宫颈癌放射抗性中的作用和机制。研究方法通过改良的 CRISPR/Cas9 双连接基因编辑系统生成稳定的 SND1 基因敲除 HeLa 细胞系(HeLa-KO)。通过慢病毒转染 pSil-SND1-sh-1 和 pSil-SND1-sh-2 质粒,构建了稳定的 SND1 基因敲除的 CaSki 细胞系(CaSki-Ctrl、CaSki-SND1-sh-1、CaSki-SND1-sh-2)。结果结果发现,SND1 的缺失会显著增加宫颈癌细胞的放射敏感性。研究还发现,沉默 SND1 能促进辐射诱导的细胞凋亡。值得注意的是,SND1 功能缺失的细胞表现出低效的共济失调毛细血管扩张症突变通路激活,进而影响 DNA 修复和 G2/M 检查点阻滞。此外,苏氨酸 103 是 SND1 在 DNA 损伤应激下的一个重要磷酸化位点。结论总之,本研究结果揭示了沉默 SND1 或 T103 突变对宫颈癌细胞的强效放射增敏作用,为宫颈癌治疗的潜在治疗策略提供了新的见解。
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SND1 Promotes Radioresistance in Cervical Cancer Cells by Targeting the DNA Damage Response.

Background: Radiotherapy is one of the most effective therapeutic strategies for cervical cancer patients, although radioresistance-mediated residual and recurrent tumors are the main cause of treatment failure. However, the mechanism of tumor radioresistance is still elusive. DNA damage response pathways are key determinants of radioresistance. The purpose of this study was to investigate the role and mechanism of SND1 in radioresistance of cervical cancer. Methods: A stable HeLa cell line with SND1 knockout (HeLa-KO) was generated through a modified CRISPR/Cas9 double-nicking gene editing system. The stable CaSki cell lines with SND1 knockdown (CaSki-Ctrl, CaSki-SND1-sh-1, CaSki-SND1-sh-2) were constructed through lentivirus transfection with the pSil-SND1-sh-1 and pSil-SND1-sh-2 plasmids. Results: It was observed that SND1 deficiency significantly increased the radiosensitivity of cervical cancer cells. It was also found that silencing SND1 promotes radiation-induced apoptosis. Significantly, the cells with a loss of SND1 function exhibited inefficient ataxia telangiectasia mutated pathway activation, subsequently impairing DNA repair and G2/M checkpoint arrest. In addition, threonine 103 is an important phosphorylation site of SND1 under DNA damaging stress. Conclusion: Collectively, the results of this study reveal a potent radiosensitizing effect of silencing SND1 or T103 mutation on cervical cancer cells, providing novel insights into potential therapeutic strategies for cervical cancer treatment.

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来源期刊
Genome Biology
Genome Biology Biochemistry, Genetics and Molecular Biology-Genetics
CiteScore
21.00
自引率
3.30%
发文量
241
审稿时长
2 months
期刊介绍: Genome Biology stands as a premier platform for exceptional research across all domains of biology and biomedicine, explored through a genomic and post-genomic lens. With an impressive impact factor of 12.3 (2022),* the journal secures its position as the 3rd-ranked research journal in the Genetics and Heredity category and the 2nd-ranked research journal in the Biotechnology and Applied Microbiology category by Thomson Reuters. Notably, Genome Biology holds the distinction of being the highest-ranked open-access journal in this category. Our dedicated team of highly trained in-house Editors collaborates closely with our esteemed Editorial Board of international experts, ensuring the journal remains on the forefront of scientific advances and community standards. Regular engagement with researchers at conferences and institute visits underscores our commitment to staying abreast of the latest developments in the field.
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