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撤回文章:西妥昔单抗对子宫颈癌细胞中辐射诱导的pEGFR介导的DNA-PK激活的下调作用

Retracted Article: Down-regulation of the radiation-induced pEGFR mediated activation of DNA-PK by Cetuximab in cervical cancer cells.

作者信息

Qi Yunxiang, Lang Jinyi, Zhu Xiaodong, Huang Jianming, Li Lu, Yi Guangming

机构信息

Sichuan Cancer Hospital & Institute, Sichuan Cancer Center, School of Medicine, University of Electronic Science and Technology of China Chengdu 610041 China

出版信息

RSC Adv. 2020 Jan 6;10(2):1132-1141. doi: 10.1039/c9ra04962b. eCollection 2020 Jan 2.

Abstract

The phosphorylation of EGFR is required for nuclear EGFR importing, and our previous study has shown that pEGFR is an independent prognostic factor for the low survival rate of patients with cervical squamous carcinoma. Now, we aim to examine the role of pEGFR in the activation of DNA-PK and radio resistance. Either CaSki or HeLa cells were exposed to a dose of 4 Gy with a 6 MV X-ray in the presence or absence of Cetuximab or Gefitinib, then EGFR, pEGFR, DNA-PKcs and pDNA-PK levels were determined using a western blot. DNA damage was quantified with γH2AX foci analysis and the response of CaSki and HeLa cells to irradiation was determined using a colony formation assay. In CaSki and HeLa cells, irradiation induced nuclear EGFR accumulation, and pEGFR and pDNA-PK levels were both significantly increased. Cetuximab pre-treatment significantly reduced the expression of pEGFR and pDNA-PK and enhanced the γH2AX foci per cell and sensitivity enhancement ratio in CaSki cells. Gefitinib pre-treatment had a similar but weaker effect. In HeLa cells, similar effects of Cetuximab and Gefitinib on pEGFR and pDNA-PK were observed, and no significant difference was found. We found that Cetuximab had a better effect than Gefitinib on attenuating the radio resistance in cervical squamous carcinoma cells inhibiting pEGFR-mediated nuclear EGFR transport and related DNA-PK-mediated DNA repair. However, in adenocarcinoma cells, both EGFR-targeted drugs had no remarkable effects on the radio sensitivity. Taken together, radiotherapy combined with Cetuximab may be a promising strategy to improve the therapeutic gain for cervical squamous carcinoma patients.

摘要

表皮生长因子受体(EGFR)的磷酸化是其核内转运所必需的,我们之前的研究表明,磷酸化的EGFR(pEGFR)是宫颈鳞癌患者低生存率的独立预后因素。现在,我们旨在研究pEGFR在DNA依赖蛋白激酶(DNA-PK)激活及放射抗性中的作用。将CaSki或HeLa细胞在有或无西妥昔单抗或吉非替尼存在的情况下,用6兆伏X射线照射4戈瑞剂量,然后用蛋白质免疫印迹法测定EGFR、pEGFR、DNA-PK催化亚基(DNA-PKcs)和磷酸化DNA-PK(pDNA-PK)水平。通过γH2AX焦点分析对DNA损伤进行定量,并使用集落形成试验确定CaSki和HeLa细胞对辐射的反应。在CaSki和HeLa细胞中,辐射诱导核EGFR积累,pEGFR和pDNA-PK水平均显著升高。西妥昔单抗预处理显著降低了CaSki细胞中pEGFR和pDNA-PK的表达,并增加了每个细胞的γH2AX焦点数量和增敏比。吉非替尼预处理有类似但较弱的效果。在HeLa细胞中,观察到西妥昔单抗和吉非替尼对pEGFR和pDNA-PK有类似作用,且无显著差异。我们发现,在抑制pEGFR介导的核EGFR转运及相关DNA-PK介导的DNA修复方面,西妥昔单抗在减弱宫颈鳞癌细胞放射抗性方面比吉非替尼效果更好。然而,在腺癌细胞中,两种EGFR靶向药物对放射敏感性均无显著影响。综上所述,放疗联合西妥昔单抗可能是提高宫颈鳞癌患者治疗获益的一种有前景的策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4363/9047960/5e2cc73be7ac/c9ra04962b-f1.jpg

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