Wu Lin, Pu Xingxiang, Wang Qianzhi, Cao Jun, Xu Fang, Xu L I, Li Kang
Department of Thoracic Medicine, The Affiliated Cancer Hospital of Xiangya School of Medicine, Central South University, Changsha, Hunan 410003, P.R. China.
Oncol Lett. 2016 Feb;11(2):945-952. doi: 10.3892/ol.2015.4000. Epub 2015 Dec 3.
Cisplatin is effective as a single agent or in combination with other drugs for the treatment of non-small cell lung cancer (NSCLC). A concerning clinical challenge with cisplatin-based NSCLC chemotherapy is the intrinsic and acquired chemoresistance to cisplatin. The sterile α motif domain-containing (SAMD9) gene has been reported as a potent tumor suppressor gene that inhibits tumorigenesis and progression of NSCLC. microRNAs (miRNA) have been revealed to play important roles in the regulation of cancer chemoresistance. To the best of our knowledge the present study explored the role of miRNA/SAMD9 signaling in regulating cisplatin chemoresistance in NSCLC for the first time. Out of the several candidate miRNAs predicted to bind the 3'-untranslated region (UTR) of the SAMD9 gene, miRNA-96 (miR-96) demonstrated significant target-sequence-specific inhibition of the SAMD9 3'-UTR luciferase reporter activity in NSCLC cells. In addition, while NSCLC tumor samples exhibited significantly higher expression levels of miR-96 compared with adjacent normal tissues, the expression levels of SAMD9 were significantly lower than those in adjacent normal tissues. miR-96 and SAMD9 were overexpressed and knocked down in the human NSCLC H358 and H23 cell lines and the half maximal inhibitory concentration (IC) of cisplatin and cell apoptosis rate under cisplatin treatment were used as measures of cisplatin chemoresistance. The present results identified that overexpression of miR-96 in NSCLC cells markedly decreased SAMD9 expression and cisplatin-induced apoptosis, and increased the cisplatin IC, which could be eliminated by overexpression of SAMD9. By contrast, knocking down miR-96 in NSCLC cells using antagomir-96 significantly increased SAMD9 expression and the cisplatin-induced apoptosis and decreased cisplatin IC, which could be completely reversed by a knockdown of SAMD9. In conclusion, the current study demonstrates that miR-96 targets and downregulates SAMD9 in NSCLC, which decreases cisplatin-induced apoptosis and induces cisplatin chemoresistance in NSCLC cells. The findings of the present study add novel insights into the function of miR-96 and SAMD9 in cancer, as well as into the molecular mechanisms underlying NSCLC chemoresistance.
顺铂作为单一药物或与其他药物联合使用对治疗非小细胞肺癌(NSCLC)有效。基于顺铂的NSCLC化疗面临的一个严峻临床挑战是对顺铂的内在和获得性化疗耐药性。含无菌α基序结构域(SAMD9)基因已被报道为一种有效的肿瘤抑制基因,可抑制NSCLC的肿瘤发生和进展。微小RNA(miRNA)已被揭示在癌症化疗耐药性的调节中发挥重要作用。据我们所知,本研究首次探讨了miRNA/SAMD9信号通路在调节NSCLC顺铂化疗耐药性中的作用。在预测与SAMD9基因3'-非翻译区(UTR)结合的几种候选miRNA中,miRNA-96(miR-96)在NSCLC细胞中对SAMD9 3'-UTR荧光素酶报告基因活性表现出显著的靶序列特异性抑制。此外,与相邻正常组织相比,NSCLC肿瘤样本中miR-96的表达水平显著更高,而SAMD9的表达水平显著低于相邻正常组织。在人NSCLC H358和H23细胞系中过表达和敲低miR-96和SAMD9,并将顺铂的半数最大抑制浓度(IC)和顺铂处理下的细胞凋亡率用作顺铂化疗耐药性的指标。目前的结果表明,NSCLC细胞中miR-96的过表达显著降低了SAMD9的表达和顺铂诱导的细胞凋亡,并提高了顺铂IC,而SAMD9的过表达可消除这种现象。相反,使用抗miR-96在NSCLC细胞中敲低miR-96可显著增加SAMD9的表达和顺铂诱导的细胞凋亡,并降低顺铂IC,而SAMD9的敲低可完全逆转这种现象。总之,当前研究表明,miR-96在NSCLC中靶向并下调SAMD9,这会降低顺铂诱导的细胞凋亡并诱导NSCLC细胞的顺铂化疗耐药性。本研究结果为miR-96和SAMD9在癌症中的功能以及NSCLC化疗耐药性的分子机制提供了新的见解。
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