Baicalin modulates microRNA expression in UVB irradiated mouse skin 被引量：3

Baicalin modulates microRNA expression in UVB irradiated mouse skin

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摘要 This study aimed to evaluate the effects of baicalin on ultraviolet radiation B （UVB）-mediated microRNA （miRNA） expression in mouse skin. We determined miRNA expression profiles in UVB irradiated mice, baicalin treated irradiated mice, and untreated mice, and conducted TargetScan and Gene Ontology analyses to predict miRNA targets. Three miRNAs （mmu-miR-125a-5p, mmu-miR-146a, and mmu-miR-141） were downregulated and another three （mmu-miR-188-5p, mmu-miR-223 and mmu-miR-22） were upregulated in UVB irradiated mice compared with untreated mice. Additionally, these miRNAs were predicted to be related to photocarcinogenesis, hypomethylation and apoptosis. Three miRNAs （mmu-miR-378, mmu-miR-199a-3p and mmu-miR-181b） were downregulated and one （mmu-miR-23a） was upregulated in baicalin treated mice compared with UVB irradiated mice, and they were predicted to be related to DNA repair signaling pathway. These deregulated miRNAs are potentially involved in the pathogenesis of photodamage, and may aid treatment and prevention of UVB-induced dermatoses. This study aimed to evaluate the effects of baicalin on ultraviolet radiation B （UVB）-mediated microRNA （miRNA） expression in mouse skin. We determined miRNA expression profiles in UVB irradiated mice, baicalin treated irradiated mice, and untreated mice, and conducted TargetScan and Gene Ontology analyses to predict miRNA targets. Three miRNAs （mmu-miR-125a-5p, mmu-miR-146a, and mmu-miR-141） were downregulated and another three （mmu-miR-188-5p, mmu-miR-223 and mmu-miR-22） were upregulated in UVB irradiated mice compared with untreated mice. Additionally, these miRNAs were predicted to be related to photocarcinogenesis, hypomethylation and apoptosis. Three miRNAs （mmu-miR-378, mmu-miR-199a-3p and mmu-miR-181b） were downregulated and one （mmu-miR-23a） was upregulated in baicalin treated mice compared with UVB irradiated mice, and they were predicted to be related to DNA repair signaling pathway. These deregulated miRNAs are potentially involved in the pathogenesis of photodamage, and may aid treatment and prevention of UVB-induced dermatoses.

作者 Yang Xu Bingrong Zhou Di Wu Zhiqiang Yin Dan Luo

机构地区 Department of Dermatology

出处《The Journal of Biomedical Research》 CAS 2012年第2期125-134,共10页 生物医学研究杂志（英文版）

基金 supported by the National Natural Science Foundation of China (No 30771946)

关键词 MICRORNA MICROARRAY ultraviolet radiation B PHOTODAMAGE BAICALIN microRNA, microarray, ultraviolet radiation B, photodamage, baicalin

分类号 Q522 [生物学—生物化学] TS103.823 [轻工技术与工程—纺织工程]

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The Journal of Biomedical Research

2012年第2期

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