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电离辐射处理细胞中微小RNA表达的实时聚合酶链反应分析

Real-time PCR analysis of micro-RNA expression in ionizing radiation-treated cells.

作者信息

Chaudhry M Ahmad

机构信息

Department of Medical Laboratory and Radiation Sciences, University of Vermont, Burlington, VT 05405, USA.

出版信息

Cancer Biother Radiopharm. 2009 Feb;24(1):49-56. doi: 10.1089/cbr.2008.0513.

Abstract

The cellular response to ionizing radiation exposure is very complex and involves many pathways. A wide variety of biologic effects are induced after exposure to ionizing radiation, ranging from DNA damage processing, signal transduction, mutations, altered gene expression, cell-cycle arrest, genomic instability, and induction of carcinogenesis to cell death. To gain insight into this complex response, global alterations in the expression of genes in irradiated cells have been examined. Recent studies have provided evidence to associate micro-RNA (miRNA) with many cellular processes, including carcinogenesis, timing of cell-fate decision, apoptosis, and metabolic pathways controlling a range of events. The small noncoding miRNA are emerging as critical components in controlling the gene expression. Because miRNA target so many genes, we hypothesized that alterations in their expression may be associated with the overall response of cells to radiation treatment. To explore the role of miRNA in cellular response to ionizing radiation, we monitored the expression levels of several miRNA by employing the stem-loop real-time polymerase chain reaction in Jurkat and TK6 cells treated with gamma-radiation. The expression levels of several members of the let-7 family miRNA that functionally inhibit the mRNAs of Ras oncogenes were upregulated after ionizing radiation treatment in Jurkat cells but were downregulated in TK6 cells. The expressions of miRNA associated with MYC translocation were upregulated in both cell types. The modulation of miRNA involved in various cancers was also examined. These results provide a first glimpse to indicate the involvement of miRNA in radiation-induced stress response and will lead to functional studies dissecting the molecular details of these processes.

摘要

细胞对电离辐射暴露的反应非常复杂,涉及许多途径。暴露于电离辐射后会诱导多种生物学效应,范围从DNA损伤处理、信号转导、突变、基因表达改变、细胞周期停滞、基因组不稳定、致癌作用的诱导到细胞死亡。为了深入了解这种复杂的反应,人们已经研究了受辐射细胞中基因表达的整体变化。最近的研究提供了证据,表明微小RNA(miRNA)与许多细胞过程相关,包括致癌作用、细胞命运决定的时机、细胞凋亡以及控制一系列事件的代谢途径。小的非编码miRNA正成为控制基因表达的关键成分。由于miRNA靶向如此多的基因,我们推测它们表达的改变可能与细胞对放射治疗的整体反应有关。为了探索miRNA在细胞对电离辐射反应中的作用,我们在经γ射线照射的Jurkat细胞和TK6细胞中采用茎环实时聚合酶链反应监测了几种miRNA的表达水平。在Jurkat细胞中,电离辐射处理后,功能性抑制Ras癌基因mRNA的let-7家族miRNA的几个成员的表达水平上调,但在TK6细胞中下调。与MYC易位相关的miRNA的表达在两种细胞类型中均上调。我们还研究了参与各种癌症的miRNA的调节。这些结果初步表明miRNA参与了辐射诱导的应激反应,并将导致对这些过程分子细节进行剖析的功能研究。

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