Literature DB >> 21622224

Structural evidence of anti-atherogenic microRNAs.

Anthony Virtue1, Jietang Mai, Ying Yin, Shu Meng, Tran Tran, Xiaohua Jiang, Hong Wang, Xiao-Feng Yang.   

Abstract

Our research attempted to address two important questions--how microRNAs modulate atherogenic inflammatory genes from a panoramic viewpoint and whether their augmented expression results from reduced microRNAs suppression. To resolve these knowledge gaps, we employed a novel database mining technique in conjunction with statistical analysis criteria established from experimentally verified microRNAs. We found that the expression of 33 inflammatory genes up-regulated in atherosclerotic lesions contain structural features in the 3'UTR of their mRNAs for potential microRNAs regulation. Additionally, the binding features governing the interactions between the microRNAs and the inflammatory gene mRNA were statistically identical to the features of experimentally verified microRNAs. Furthermore, 21 of the 33 inflammatory genes (64%) were targeted by highly expressed microRNAs and 10 of these (48%) were targeted by a single microRNA, suggesting microRNA regulation specificity. Supplementing our findings, 7 out of the 20 unique microRNAs (35%) were previously confirmed to be down-regulated when treated with pro-atherogenic factors. These results indicate a critical role of anti-inflammatory microRNAs in suppressing pro-atherogenic inflammatory gene expression.

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Year:  2011        PMID: 21622224      PMCID: PMC3105347          DOI: 10.2741/3901

Source DB:  PubMed          Journal:  Front Biosci (Landmark Ed)        ISSN: 2768-6698


  51 in total

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Journal:  Physiol Genomics       Date:  2005-06-07       Impact factor: 3.107

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  11 in total

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5.  Upregulation of miR-142-5p in atherosclerotic plaques and regulation of oxidized low-density lipoprotein-induced apoptosis in macrophages.

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Review 8.  Early diagnosis of atherosclerosis with panoramic radiographs: a review.

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9.  Increased Expression of Resistin in MicroRNA-155-Deficient White Adipose Tissues May Be a Possible Driver of Metabolically Healthy Obesity Transition to Classical Obesity.

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10.  Increasing Upstream Chromatin Long-Range Interactions May Favor Induction of Circular RNAs in LysoPC-Activated Human Aortic Endothelial Cells.

Authors:  Angus Li; Yu Sun; Charles Drummer; Yifan Lu; Daohai Yu; Yan Zhou; Xinyuan Li; Simone J Pearson; Candice Johnson; Catherine Yu; William Y Yang; Kevin Mastascusa; Xiaohua Jiang; Jianxin Sun; Thomas Rogers; Wenhui Hu; Hong Wang; Xiaofeng Yang
Journal:  Front Physiol       Date:  2019-04-18       Impact factor: 4.566

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