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张介平,郑莉,王娟,等.氧化应激诱导的大鼠Müller细胞微小RNA表达谱的初步研究[J].同济大学学报（医学版）,2015,36(6):1-7. [点击复制]
ZHANG Jie-ping,ZHENG Li,WANG Juan,et al.Expression profile of small RNA in rat Müller cells under oxidative stress[J].同济大学学报（医学版）,2015,36(6):1-7. [点击复制]

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氧化应激诱导的大鼠Müller细胞微小RNA表达谱的初步研究
张介平,郑莉,王娟,吕立夏,徐国彤
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(同济大学医学院眼科研究所,上海 200092;同济大学医学院再生医学系,上海 200092;同济大学医学院干细胞研究中心,上海 200092)

摘要:

目的研究在氧化应激条件下视网膜Müller细胞的miRNA表达谱,为寻找氧化应激条件下Müller细胞的靶向分子提供线索。方法用2mmol乙二醛处理大鼠Müller细胞48h,然后收集细胞,抽提总RNA,本研究采用小RNA两端加接头序列,反转录,克隆,随机测序的方法构建大鼠Müller细胞系的小RNA文库,序列经Genebank Blastn和miRBase比对分析,Mfold软件在线预测二级结构验证miRNA,经qRT-PCR鉴定miRNA,通过miRPath分析müller细胞表达的miRNA相关信号通路。结果本文库获得163个有效序列,31个克隆为已知miRNA序列,代表13种miRNA,它们与PI3K-AKT,MAPK,细胞外基质的合成及相互作用等多条信号通路密切相关。发现1个新miRNA序列。结论氧化应激条件下表达的miRNA为更好地了解在生理和疾病条件下的Müller细胞功能提供有益的线索。

关键词: 氧化应激微小RNA Müller细胞大鼠

DOI：10.16118/j.1008-0392.2015.06.001

投稿时间：2015-05-13

基金项目:国家重点基础研究发展计划(2013CB967501)

Expression profile of small RNA in rat Müller cells under oxidative stress

ZHANG Jie-ping,ZHENG Li,WANG Juan,LV Li-xia,XU Guo-tong

(Tongji Eye Institute, Medical College, Tongji University, Shanghai 200092, China;Dept.of Regenerative Medicine, Medical College, Tongji University, Shanghai 200092, China;Stem Cell Research Center, Medical College, Tongji University, Shanghai 200092, China)

Abstract:

Objective To investigate the miRNA expression profile of rat Müller cells under oxidative stress. Methods Rat Müller cells were treated with 2mM of glyoxal for 48 h and total RNA was extracted. The small RNA library was generated by adding linkers to both ends of small RNA, reverse transcription, cloning and random sequencing. The sequences were subjected to Genebank Blastn and miRBase for sequence alignment analysis and Mfold online software for secondary structure prediction in order to screen out potential miRNAs. The results were finally confirmed by qRT-PCR. The signaling pathways related to discovered miRNAs were evaluated by miRPath. ResultsFrom this library, 163 clones were sequenced. 31 clones of them were known miRNAs, representing 13 families of miRNAs. They were closely related to PI3K-AKT pathway, MAPK pathway, extracellular matrix synthesis and interaction related pathway. A new miRNA sequence was found. Conclusion Highly expressed miRNAs of Müller cell under oxidative stress provide useful clues for better understanding its function in physiological and pathological context.

Key words: oxidative stress microRNA Müller cell