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尘肺病中外泌体miR-125a的上调通过抑制EZH2和hnRNPK的表达来抑制肺癌发展。

Up-regulation of exosomal miR-125a in pneumoconiosis inhibits lung cancer development by suppressing expressions of EZH2 and hnRNPK.

作者信息

Zhang Lin, Li Jiangfeng, Hao Changfu, Guo Wei, Wang Di, Zhang Jianhui, Zhao Youliang, Duan Shuyin, Yao Wu

机构信息

Department of Reproductive Medical Center, Third Affiliated Hospital of Zhengzhou University 7 Kangfuqian Road Zhengzhou 450001 China.

Department of Occupational and Environmental Health, School of Public Health, Zhengzhou University 100 Science Avenue Zhengzhou 450001 China

出版信息

RSC Adv. 2018 Jul 25;8(47):26538-26548. doi: 10.1039/c8ra03081b. eCollection 2018 Jul 24.

Abstract

Exposure to nanoparticles may lead to pneumoconiosis and lung cancer; however, whether patients suffering from pneumoconiosis also face a high risk of lung cancer has been under debate for decades. Recently, exosomes have been found to play critical roles in many diseases intercellular cargo transportation, which has provided a new insight into the mechanistic investigation of nanoparticle-induced respiratory disorders. Herein, we isolated exosomes from the venous blood of patients with pneumoconiosis and healthy controls and then, we profiled the expression signatures of exosomal miRNAs using high-throughput sequencing technology. A total of 14 aberrantly expressed miRNAs were identified and used to process target gene prediction and functional annotation. Specially, miR-125a along with its target genes EZH2 and hnRNPK was found to play a significant role in the development of lung cancer. We then adopted a series of cellular experiments to validate the role of miR-125a in lung cancer. From the results obtained, we found that the suppression of EZH2 and hnRNPK by high levels of miR-125a inhibited the development of nanoparticle-induced lung adenocarcinoma, which contributed to the clarification of the relation between pneumoconiosis and lung cancer.

摘要

接触纳米颗粒可能导致尘肺病和肺癌;然而,尘肺病患者是否也面临肺癌的高风险这一问题已争论了数十年。最近,人们发现外泌体在许多疾病的细胞间货物运输中发挥着关键作用,这为纳米颗粒诱导的呼吸系统疾病的机制研究提供了新的见解。在此,我们从尘肺病患者和健康对照者的静脉血中分离出外泌体,然后使用高通量测序技术分析外泌体微小RNA(miRNA)的表达特征。共鉴定出14种异常表达的miRNA,并用于进行靶基因预测和功能注释。特别地,发现miR-125a与其靶基因EZH2和hnRNPK在肺癌发生发展中起重要作用。然后我们采用了一系列细胞实验来验证miR-125a在肺癌中的作用。从获得的结果来看,我们发现高水平的miR-125a对EZH2和hnRNPK的抑制作用抑制了纳米颗粒诱导的肺腺癌的发展,这有助于阐明尘肺病与肺癌之间的关系。

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