MiRNA-203 Reduces Nasopharyngeal Carcinoma Radioresistance by Targeting IL8/AKT Signaling

Qu Jia-Quan; Yi Hong-Mei; Ye Xu; Zhu Jin-Feng; Yi Hong; Li Li-Na; Xiao Ta; Yuan Li; Li Jiao-Yang; Wang Yuan-Yuan; Feng Juan; He Qiu-Yan; Lu Shan-Shan; Xiao Zhi-Qiang

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MiRNA-203 Reduces Nasopharyngeal Carcinoma Radioresistance by Targeting IL8/AKT Signaling

机译：MiRNA-203通过靶向IL8 / AKT信号传导来减少鼻咽癌辐射敏感度

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Radioresistance poses a major challenge in nasopharyngeal carcinoma (NPC) treatment, but little is known about how miRNA (miR) regulates this phenomenon. In this study, we investigated the function and mechanism of miR-203 in NPC radioresistance, one of downregulated miRs in the radioresistant NPC cells identified by our previous microarray analysis. We observed that miR-203 was frequently downregulated in the radioresistant NPC tissues compared with radiosensitive NPC tissues, and its decrement significantly correlated with NPC radioresistance and poor patient survival, and was an independent predictor for reduced patient survival. In vitro radioresponse assays showed that miR-203 mimic markedly decreased NPC cell radioresistance. In a mouse model, therapeutic administration of miR-203 agomir dramatically sensitized NPC xenografts to irradiation. Mechanistically, we confirmed that IL8 was a direct target of miR-203, and found that reduced miR-203 promoted NPC cell radioresistance by activating IL8/AKT signaling. Moreover, the levels of IL8 and phospho-AKT were significantly increased in the radioresistant NPC tissues compared with radiosensitive NPC tissues, and negatively associated with miR-203 level. Our data demonstrate that miR-203 is a critical determinant of NPC radioresponse, and its decrement enhances NPC radioresistance through targeting IL8/AKT signaling, highlighting the therapeutic potential of the miR-203/IL8/AKT signaling axis in NPC radiosensitization. (C) 2015 AACR.

机译：放射线患者在鼻咽癌（NPC）治疗中提出了一项重大挑战，但对于MiRNA（MIR）如何调节这种现象而言，众所周知。在本研究中，我们研究了通过我们之前的微阵列分析所识别的放射性剂NPC细胞中的下调的MIR中MiR-203中miR-203的功能和机制。我们观察到，与放射性NPC组织相比，MiR-203经常在放射性NPC组织中下调，其递减与NPC辐射血频和患者存活率显着相关，并且是减少患者存活的独立预测因子。体外辐射测定结果显示MIR-203模拟显着降低的NPC细胞辐射敏感度。在小鼠模型中，MiR-203 Agomir的治疗施用显着敏感NPC异种移植物以照射。机械地，我们证实IL8是miR-203的直接靶标，发现通过激活IL8 / AKT信号传导，降低miR-203促进了NPC细胞辐射敏感度。此外，与放射性NPC组织相比，在放射体NPC组织中，IL8和磷酸磷-AKT的水平显着增加，与MIR-203水平负相关。我们的数据表明MIR-203是NPC辐射的关键决定因素，其递减通过靶向IL8 / AKT信号传导而增强NPC辐射抗体，突出显示MIR-203 / IL8 / AKT信号轴的治疗电位在NPC放射敏化中的治疗势。（c）2015年AACR。

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《Molecular cancer therapeutics》 |2015年第11期|共12页
作者
Qu Jia-Quan; Yi Hong-Mei; Ye Xu; Zhu Jin-Feng; Yi Hong; Li Li-Na; Xiao Ta; Yuan Li; Li Jiao-Yang; Wang Yuan-Yuan; Feng Juan; He Qiu-Yan; Lu Shan-Shan; Xiao Zhi-Qiang;
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Cent S Univ Xiangya Hosp Res Ctr Carcinogenesis &

Targeted Therapy Changsha 410008 Hunan;

Cent S Univ Xiangya Hosp Res Ctr Carcinogenesis &

Targeted Therapy Changsha 410008 Hunan;

Cent S Univ Xiangya Hosp Res Ctr Carcinogenesis &

Targeted Therapy Changsha 410008 Hunan;

Cent S Univ Xiangya Hosp Res Ctr Carcinogenesis &

Targeted Therapy Changsha 410008 Hunan;

Cent S Univ Xiangya Hosp Res Ctr Carcinogenesis &

Targeted Therapy Changsha 410008 Hunan;

Cent S Univ Xiangya Hosp Res Ctr Carcinogenesis &

Targeted Therapy Changsha 410008 Hunan;

Cent S Univ Xiangya Hosp Res Ctr Carcinogenesis &

Targeted Therapy Changsha 410008 Hunan;

Cent S Univ Xiangya Hosp Res Ctr Carcinogenesis &

Targeted Therapy Changsha 410008 Hunan;

Cent S Univ Xiangya Hosp Res Ctr Carcinogenesis &

Targeted Therapy Changsha 410008 Hunan;

Cent S Univ Xiangya Hosp Res Ctr Carcinogenesis &

Targeted Therapy Changsha 410008 Hunan;

Cent S Univ Xiangya Hosp Res Ctr Carcinogenesis &

Targeted Therapy Changsha 410008 Hunan;

Cent S Univ Xiangya Hosp Res Ctr Carcinogenesis &

Targeted Therapy Changsha 410008 Hunan;

Cent S Univ Xiangya Hosp Res Ctr Carcinogenesis &

Targeted Therapy Changsha 410008 Hunan;

Cent S Univ Xiangya Hosp Res Ctr Carcinogenesis &

Targeted Therapy Changsha 410008 Hunan;

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正文语种 eng
中图分类肿瘤学;
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1. MiRNA-203 Reduces Nasopharyngeal Carcinoma Radioresistance by Targeting IL8/AKT Signaling [J] . Qu Jia-Quan, Yi Hong-Mei, Ye Xu, Molecular cancer therapeutics . 2015,第11期

机译：MiRNA-203通过靶向IL8 / AKT信号传导来减少鼻咽癌辐射敏感度
2. ANXA6 Contributes to Radioresistance by Promoting Autophagy via Inhibiting the PI3K/AKT/mTOR Signaling Pathway in Nasopharyngeal Carcinoma [J] . Chen Qianping, Zheng Wang, Zhu Lin, Frontiers in Cell and Developmental Biology . 2020,第1期

机译：ANXA6通过抑制鼻咽癌中的PI3K / AKT / MTOR信号传导途径来促进自噬有助于胃肠饲料
3. 2-Methoxyestradiol inhibits the proliferation and migration and reduces the radioresistance of nasopharyngeal carcinoma CNE-2 stem cells via NF-kappa B/HIF-1 signaling pathway inactivation and EMT reversal [J] . Wu Shun-Long, Li Ya-Jun, Liao Kui, Oncology reports . 2017,第2期

机译：2-甲氧基雌二醇抑制增殖和迁移，并通过NF-Kappa B / HIF-1信号传导途径灭活和EMT逆转减少鼻咽癌CNE-2干细胞的辐射敏感度
4. ELF-1 Expression in Nasopharyngeal Carcinoma Facilitates Proliferation and Metastasis of Cancer Cells via Modulating CCL2/CCR2 Signaling [C] . Chang-Han Chen International Molecular Medicine Tri-Conference. . 2019

机译：鼻咽癌中的ELF-1表达促进通过调节CCL2 / CCR2信号传导的癌细胞增殖和转移
5. Identification of Novel Candidate Tumor Suppressor Genes at 11q and 15q for Esophageal Squamous Cell Carcinoma and Nasopharyngeal Carcinoma via Integrative Cancer Epigenetics and Genomics. [D] . Li, Jisheng. 2010

机译：通过综合癌症表观遗传学和基因组学鉴定食管鳞状细胞癌和鼻咽癌的11q和15q新型候选肿瘤抑制基因。
6. RNA binding motif protein 3 (RBM3) drives radioresistance in nasopharyngeal carcinoma by reducing apoptosis via the PI3K/AKT/Bcl-2 signaling pathway [O] . Rui Ma, Li-Na Zhao, Hua Yang, 2018

机译：RNA结合基序蛋白3（RBM3）通过减少PI3K / AKT / Bcl-2信号通路的凋亡来驱动鼻咽癌的放射抵抗
7. MiRNA-203 Reduces Nasopharyngeal Carcinoma Radioresistance by Targeting IL8/AKT Signaling [O] . Jia-Quan Qu, Hong-Mei Yi, Xu Ye, 2015

机译：MiRNA-203通过靶向IL8 / AKT信号传导来减少鼻咽癌辐射敏感度

MiRNA-203 Reduces Nasopharyngeal Carcinoma Radioresistance by Targeting IL8/AKT Signaling

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