Silencing of miR-101 Prevents Cartilage Degradation by Regulating Extracellular Matrix–related Genes in a Rat Model of Osteoarthritis

Osteoarthritis (OA) is a common, degenerative joint disease characterized by articular cartilage degradation. Currently, clinical trials based on microRNA therapy have been performed to treat various diseases. However, no treatment has been found for arthritis. This study investigated the functions...

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Published inMolecular therapy Vol. 23; no. 8; pp. 1331 - 1340
Main Authors Dai, Linghui, Zhang, Xin, Hu, Xiaoqing, Liu, Qiang, Man, Zhentao, Huang, Hongjie, Meng, Qingyang, Zhou, Chunyan, Ao, Yingfang
Format Journal Article
LanguageEnglish
Published United States Elsevier Inc 01.08.2015
Elsevier Limited
Nature Publishing Group
Subjects
Animals
Arthritis
Arthritis, Experimental - pathology
Arthritis, Experimental - therapy
Cartilage
Cartilage, Articular - metabolism
Clinical trials
Cytokines - metabolism
Disease
Disease Models, Animal
Extracellular matrix
Extracellular Matrix - metabolism
Gene Silencing
Genes
Genetic Vectors
Iodoacetates - chemistry
MicroRNAs
MicroRNAs - genetics
Microscopy
Microscopy, Fluorescence
Oligonucleotide Array Sequence Analysis
Original
Osteoarthritis
Osteoarthritis - chemically induced
Osteoarthritis - pathology
Osteoarthritis - therapy
Proteins
Protons
Rats
Rats, Sprague-Dawley
SOX9 Transcription Factor - metabolism
Sports injuries
Sports medicine
Synovial Fluid - metabolism
Beijing China
China
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Summary:Osteoarthritis (OA) is a common, degenerative joint disease characterized by articular cartilage degradation. Currently, clinical trials based on microRNA therapy have been performed to treat various diseases. However, no treatment has been found for arthritis. This study investigated the functions of miR-101 in cartilage degradation in vivo and evaluated the feasibility of using miR-101 as a therapeutic agent for OA. Mono-iodoacetate-induced arthritis (MIA) rats were used as an animal model of OA. miR-101 mimic or miR-101 inhibitor was injected into the rats’ knees to evaluate its effects on cartilage degradation. Cartilage degradation aggravated at 14 days after the injection of miR-101 mimic. By contrast, miR-101 silencing reduced cartilage degradation. Moreover, the administration of miR-101 mimic is sufficient to cause cartilage degradation in the normal cartilage of rats. By contrast, miR-101 inhibitor could prevent this change. Microarray and qPCR were used to investigate the different expressed genes after injecting miR-101 mimic and miR-101 inhibitor in the rats’ articular cartilage. Several cartilage degradation-related genes were selected and validated to function in cartilage degradation with miR-101. Our results demonstrated the therapeutic effect of miR-101 inhibition on cartilage degradation in MIA rats by regulating several cartilage degradation–related genes.
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The first two authors contributed equally to this work.
ISSN:1525-0016
1525-0024
DOI:10.1038/mt.2015.61