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RBM5 reduces small cell lung cancer growth increases cisplatin sensitivity and regulates key transformation-associated pathways

机译:RBM5减少小细胞肺癌的生长增加顺铂敏感性并调节关键的转化相关途径

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摘要

Small cell lung cancer (SCLC) is the most aggressive type of lung cancer, with almost 95% of patients succumbing to the disease. Although RBM5, a tumor suppressor gene, is downregulated in the majority of lung cancers, its role in SCLC is unknown. Using the GLC20 SCLC cell line, which has a homozygous deletion encompassing the RBM5 gene locus, we established stable RBM5 expressing sublines and investigated the effects of RBM5 re-expression. Transcriptome and target identification studies determined that RBM5 directly regulates the cell cycle and apoptosis in SCLC cells, as well as significantly downregulates other important transformation-associated pathways such as angiogenesis and cell adhesion. RNA sequencing of paired non-tumor and tumor SCLC patient specimens showed decreased RBM5 expression in the tumors, and expression alterations in the majority of the same pathways that were altered in the GLC20 cells and sublines. Functional studies confirmed RBM5 expression slows SCLC cell line growth, and increases sensitivity to the chemotherapy drug cisplatin. Overall, our work demonstrates the importance of RBM5 expression to the non-transformed state of lung cells and the consequences of its deletion to SCLC development and progression.
机译:小细胞肺癌(SCLC)是最积极的肺癌类型,几乎95%的患者死于该疾病。尽管RBM5(一种抑癌基因)在大多数肺癌中被下调,但其在SCLC中的作用尚不清楚。使用GLC20 SCLC细胞系(具有包含RBM5基因位点的纯合缺失),我们建立了稳定的RBM5表达亚系,并研究了RBM5重新表达的作用。转录组和靶标鉴定研究确定,RBM5直接调节SCLC细胞的细胞周期和凋亡,并显着下调其他重要的转化相关途径,如血管生成和细胞粘附。配对的非肿瘤和肿瘤SCLC患者标本的RNA测序显示,肿瘤中RBM5的表达降低,并且在GLC20细胞和亚系中改变的大多数相同途径中,表达均发生改变。功能研究证实,RBM5表达减慢了SCLC细胞系的生长,并增加了对化疗药物顺铂的敏感性。总的来说,我们的工作证明了RBM5表达对肺细胞非转化状态的重要性以及其缺失对SCLC发育和进展的影响。

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