靶向运载siRNA调控肾癌VEGF Pre-mRNA选择性剪接的作用及机制研究

项目名称： 靶向运载siRNA调控肾癌VEGF Pre-mRNA选择性剪接的作用及机制研究

项目编号： No.81202018

项目类型： 青年科学基金项目

立项/批准年度： 2013

项目学科： 肿瘤学2

项目作者： 蒋国松

作者单位： 华中科技大学

项目金额： 23万元

中文摘要： 血管内皮生长因子(VEGF) mRNA前体第8外显子选择性剪接可产生促血管生成和抗血管生成两类功能相反的变构体，靶向干预VEGF异常剪接已成为肾癌治疗研究的新内容。新近研究表明，针对可变剪接位点的siRNA能够在未沉默基因表达前提下，有效干预mRNA前体选择性剪接，为靶向调控肿瘤细胞基因异常剪接提供了新方法。据此，本课题将系统解析肾癌细胞VEGF 异常剪接的分子基础并设计siRNA进行靶向干预；在前期研究发现siRNA能够在转录水平抑制RNA聚合酶II功能的基础上，探讨siRNA干预选择性剪接的作用机制；在前期研究证实穿膜肽能够安全高效地将融合蛋白导入肿瘤细胞的基础上，设计并合成具有肾癌组织靶向性的G250单链抗体-低分子量鱼精蛋白(LMWP)融合蛋白载体运载siRNA。本项目的成功实施，将为进一步利用siRNA调控基因选择性剪接奠定理论基础，并为肾癌的靶向治疗提供更具针对性的新策略。

中文关键词： 血管内皮生长因子；选择性剪接；小干扰RNA；SETD2；miR-106b-5p

英文摘要： Vascular endothelial growth factor (VEGF) is produced either as a pro-angiogenic or anti-angiogenic protein depending upon alternative splicing site choice in eighth exon. Since sustained angiogenesis is critical for renal cell carcinoma growth and metastasis, restoration of normal VEGF splicing presents a new approach. Recent studies have shown that aberrant splice site targeted siRNA efficiently restored splicing without reducing transcript levels, providing a novel strategy for the regulation of aberrant gene splicing in cancer cells. In this project, we will detect the molecular basis by which the pro-angiogenic splice site choice is mediated, and then specifically modulate VEGF splicing to promote anti-angiogenic isoforms in renal cell carcinoma by splice site-based siRNA. We have previously shown that siRNA could inhibit RNA polymerase II function at transcriptional level. As RNA polymerase II has been implicated in regulating alternative splicing, we hypothesized that siRNA may interfere splicing through indirect interaction with polymerase II. Our preliminary studies also confirmed that cell-penetrating peptide (CPP) could deliver fusion protein into tumor cells through an efficient and safe way. In the project, we will design and synthesize the renal cell carcinoma targeted fusion protein of single-chai

英文关键词： VEGF；alternative splicing；siRNA；SETD2；miR-106b-5p