Rutin treats myocardial damage caused by pirarubicin via regulating miR‐22‐5p‐regulated RAP1/ERK signaling pathway

Our experiments have previously demonstrated that rutin (RUT) can improve myocardial damage caused by pirarubicin (THP). However, the underlying molecular mechanisms remain uncertain. In this study, we developed an microRNA (miRNA) chip by replicating the rat model of THP‐induced myocardial injury a...

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Bibliographic Details
Published inJournal of biochemical and molecular toxicology Vol. 35; no. 1; pp. e22615 - n/a
Main Authors Qin, Meng, Li, Qi, Wang, Yadi, Li, Tengteng, Gu, Zehui, Huang, Peng, Ren, Liqun
Format Journal Article
LanguageEnglish
Published United States Wiley Subscription Services, Inc 01.01.2021
Subjects
Apoptosis
Cardiomyocytes
Chromosome 5
Damage
EKG
Electrocardiography
Extracellular signal-regulated kinase
In vivo methods and tests
Kinases
Metabolic pathways
MicroRNAs
miRNA
miR‐22‐5p
Molecular modelling
myocardial damage
pirarubicin
Proteins
Rap1 protein
RAP1/ERK signaling pathway
Reactive oxygen species
Ribonucleic acid
RNA
Rutin
Signal transduction
Signaling
myocardial damage
pirarubicin
rutin
miR-22-5p
RAP1/ERK signaling pathway
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Summary:Our experiments have previously demonstrated that rutin (RUT) can improve myocardial damage caused by pirarubicin (THP). However, the underlying molecular mechanisms remain uncertain. In this study, we developed an microRNA (miRNA) chip by replicating the rat model of THP‐induced myocardial injury and identified miR‐22‐5p and the RAP1‐member of RAS oncogene family/extracellular regulated protein kinases (RAP1/ERK) signaling pathway as an object of study. Also, in vivo experiments demonstrated that THP caused abnormal changes in the electrocardiogram, cardiac function, and histomorphology in rats (P < .01). THP also reduces the expression of miR‐22‐5p (P < .01) and increases the levels of RAP1/ERK signaling pathway‐related proteins (P < .01, P < .05). RUT significantly improved THP‐induced myocardial damage (P < .01), increased the expression of miR‐22‐5p (P < .01), and decreased the levels of RAP1/ERK signaling pathway‐related proteins (P < .01, P < .05). In vitro studies confirmed that Rap1a is one of the target genes of miR‐22‐5p. miR‐22‐5p overexpression in cardiomyocytes can affect the RAP1/ERK pathway and reduce reactive oxygen species production and cardiomyocyte apoptosis caused by THP (P < .01), which is consistent with the effect of RUT. Our results indicate that RUT treats THP‐induced myocardial damage, which may be achieved by upregulating miR‐22‐5p, causing changes in its target gene Rap1a and the RAP1/ERK pathway.
Bibliography:Qi Li and Yadi Wang should be considered as joint second author.
ISSN:1095-6670
1099-0461
DOI:10.1002/jbt.22615