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乳腺癌中p53相关mirna的研究生物化学与分子生物学专业论文
ABSTRACTAs
ABSTRACT
As axl important tumor suppressor,p53 plays a pivotal role in the DNA damage and oncogene signaling pathway,mainly functioning as a transcription factor.When suffering fTom DNA damage,stimuli of oncogenic and hypoxia,the activated p53 protein can transcriptionally regulate a series of genes,resulting in arrest of cell cycle,apoptosis,DNA repair or senescence.miRNAs are a class of endogenous non—coding RNA,which call bind the target mRNA through complementary base
pairing,form RNA induced silencing complex tmsc),and lead to degradation or仃anslation inhibition of their target mKNAs.Numerous miRNAs have been found to be involved in the regulation of the p53 signaling pathway.Conversely,p53 regulates the transcription or processing of miRNAs.Given that complexities in the association between p53 and miRNAs exist,and due to the rapidly increasing amount
of literature regarding the interactions between p53 and miRNAs,the
present study systematically analyzed the associations between miRNAs
and p53 in breast cancer using a literature—based discovery approach and
next generation sequencing.
Using a literature—based discovery approach,natural language processing,we found that a total of 22 miRNAs were associated with p53 in the breast cancer.Next,three popular online tools(PicTar,miRanda
m
万方数据
and
and TargetScan)were used to predict the targets of each miRNA,and certain targets were validated by experiments.Gene Ontology annotation and network analysis demonstrated that the majority of the targets of the p53-related miRNAs were enriched in the cell cycle process and axonal
guidance signaling.
In addition,the breast cancer cell 1ine MCF.7 was infected with lentiviral p53 shRNA and empty vector lentivirus.At 72 hours after infection,puromycin were used to screen for stable cell lines.Then,we analyzed the small RNA expression profiles by the second—generation sequencing,and found that p53 interference significantly decreased
expression of 1 2 miRNAs.Realti
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