干细胞标记物基因 Musashi1 rs2522137位点单核甘酸多态性与肺癌关系的研究

项目名称： 干细胞标记物基因 Musashi1 rs2522137位点单核甘酸多态性与肺癌关系的研究

项目编号： No.81501962

项目类型： 青年科学基金项目

立项/批准年度： 2016

项目学科： 医药、卫生

项目作者： 王旭

作者单位： 吉林大学

项目金额： 18万元

中文摘要： Musashi1 (Msi1)是最新研究报道的肿瘤干细胞标志物之一，在肺癌及多种肿瘤中高表达，与肿瘤的发生、预后治疗相关，但其高表达的具体机制尚不清。本课题组在国际上首次发现位于Msi1基因3’非翻译区的rs2522137 单核甘酸多态性（SNP）是肺癌发病的独立危险因素，且与晚期非小细胞肺癌的预后相关。进一步的功能分析提示rs2522137位于6个不同miRNA结合位点的重叠区。因此rs2522137 SNP可能通过表观遗传学机制（miRNA）调控Msi1在肿瘤中的差异性表达及Msi1 mRNA的稳定性,从而影响肺癌干细胞的干性，增加肺癌发病危险。本课题将分析Msi1基因rs2522137与肺癌易感及预后的关系，探索该位点不同基因型在不同肺癌细胞系及组织样本中的Msi1表达的差异，阐明rs2522137调控Msi1表达的表观遗传学机制，最终为肿瘤的临床靶向治疗提供依据。

中文关键词： 肺肿瘤；干细胞标记物基因；Musashi1；单核甘酸多态性；小RNA

英文摘要： Musashi RNA-binding protein 1 (Musashi-1，Msi1), an RNA-binding protein, is expressed in various epithelial stem cells and plays an important role in regulating the maintenance and differentiation of stem/precursor cells. Msi1 is over-expressed in several tumor tissues including lung cancer, suggesting a correlation with oncogenic development.Our pilot study provides the first evidence to correlate the Musashi-1 rs2522137 SNP variant with lung cancer. Currently, we know very little about the detailed molecular mechanisms by which Musashi-1 rs2522137 polymorphisms contribute to lung cancer development. The 3’-UTR of mature Musashi-1mRNA is potentially targeted by several tumor suppressor miRNAs andevolutionarily conserved RNA-binding protein. Using the SNPinfo website(http:// snpinfo. niehs. nih.gov/), we found that the Musashi-13’-UTR also buries potential target sites for miRNAs hsa-miR-1275, hsa-miR-1285, hsa-miR-483-5p.,hsa-miR-486-3p, hsa-miR-612, and hsa-miR-625. It is worthwhile noting that Musashi-1 rs2522137 is located within these miRNA binding sites. we thus propose to characterize the role of rs2522137genotype in determining the stability of Msi1 mRNA, thus the stemness and self-renewal of lung cancer stem cells. We will fucos on the epigeneticmechanisms by which Musashi-1 rs2522137 GG variant affects its own mRNA expression through the microRNA pathway. The data obtained from this study will shed light on the molecular mechanisms for the regulation of the Msi1 in lung cancer. In addition, this project will provide a mechanistic rationale for designing antitumor drugs that target the overexpressed Msi1 in lung stem cancer cells.

英文关键词： lung cancer;cancer stem cell marker gene;Musashi1;SNP;micro-RNA