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Clusterin (CLU) and Lung Cancer

机译:簇蛋白(CLU)与肺癌

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Lung cancer is the leading cause of cancer-related mortality. It is categorized into two histological groups that have distinct clinical behaviors, the nonsmall cell lung cancers (NSCLC) and the small cell lung cancer (SCLC). When identified at an early stage, NSCLC is treated by surgical resection. However, patients who undergo surgical resection still have a relative low survival rate, primarily for tumor recurrence. Unfortunately, advances in cytotoxic therapy have reached a plateau and new approaches to treatment are needed together with new and better parameters for more accurate prediction of the outcome and more precise indication of the efficacy of the treatment. Several in vitro studies have examined the role of Clusterin (CLU) in carcinogenesis, lung cancer progression, and response to chemo- and radiotherapy. Studies performed in lung cancer cell lines and animal models showed that CLU is upregulated after exposure to chemo- and radiotherapy. A potential role proposed for the protein is cytoprotective. In vitro, CLU silencing by antisense oligonucleotides (ASO) and small-interfering RNAs (siRNA) directed against CLU mRNA in CLU-rich lung cancer cell lines sensitized cells to chemotherapy and radiotherapy and decreased their metastatic potential. In vivo, a recent work analyzed the prognostic role of CLU in NSCLC, showing that CLU-positive patients with lung cancer had a better overall survival and disease-free survival than those with CLU-negative tumors. These data are contradictory to the promising in vitro results. From the results of these studies we may hypothesize that in early-stage lung cancers CLU represents a positive biomarker correlating with better overall survival. In advanced patients, already treated with chemo- and radiotherapy, the induction of CLU may confer resistance to the treatments. However, many studies are needed to better understand the role of CLU in early-stage and advanced lung cancers with the aim to discriminate patients...
机译:肺癌是癌症相关死亡率的主要原因。它分为具有不同临床行为的两个组织学类别,非小细胞肺癌(NSCLC)和小细胞肺癌(SCLC)。在早期发现NSCLC时,可通过手术切除进行治疗。但是,接受外科手术切除的患者存活率仍然较低,主要是因为肿瘤复发。不幸的是,细胞毒性治疗的进展已达到平稳阶段,需要新的治疗方法以及新的更好的参数,以更准确地预测结果并更准确地指示治疗效果。几项体外研究检查了Clusterin(CLU)在致癌,肺癌进展以及对化学和放射疗法的反应中的作用。在肺癌细胞系和动物模型中进行的研究表明,CLU在接受化学和放射治疗后会上调。建议对该蛋白质的潜在作用是具有细胞保护作用。在体外,富含CLU的肺癌细胞系中的针对CLU mRNA的反义寡核苷酸(ASO)和小干扰RNA(siRNA)使CLU沉默,使细胞对化学疗法和放射疗法敏感,并降低了其转移潜力。在体内,最近的一项工作分析了CLU在NSCLC中的预后作用,表明CLU阳性的肺癌患者比CLU阴性的肿瘤患者具有更好的总体生存率和无病生存期。这些数据与有希望的体外结果相矛盾。从这些研究的结果中,我们可以假设在早期肺癌中CLU代表着阳性的生物标志物,与更好的总体生存率相关。在已经接受化学疗法和放射疗法治疗的晚期患者中,CLU的诱导可能对治疗产生耐药性。但是,需要进行大量研究以更好地了解CLU在早期和晚期肺癌中的作用,以区分患者。

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