MicroRNA-140 plays dual roles in both cartilage development and homeostasis

Miyaki, Shigeru; Sato, Tempei; Inoue, Atsushi; Otsuki, Shuhei; Ito, Yoshiaki; Yokoyama, Shigetoshi; Kato, Yoshio; Takemoto, Fuko; Nakasa, Tomoyuki; Yamashita, Satoshi; Takada, Shuji; Lotz, Martin; Ueno-Kudo, Hiroe; Asahara, Hiroshi

doi:10.1101/gad.1915510

Cited by 531 publications

(566 citation statements)

References 41 publications

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“…The results of these studies indicate that miR-140 is one of the main regulators of chondroblast differentiation through its effects on the expression of not only Sox9 (Karlsen et al 2013), but also several other targets (Hdac4, Sp1, Smad3, and aggrecan) (Pais et al 2010, Nakamura et al 2011, Karlsen et al 2013. Moreover, independent groups have developed miR-140-null mice, which displayed a concordant phenotype with major growth defects of endochondral bones (Miyaki et al 2010, Nakamura et al 2011, Papaioannou et al 2013. Interestingly, Sox9, L-Sox5, and Sox6 have been proved to cooperatively activate the miR-140 promoter in vivo and in vitro (Miyaki et al 2010, Yamashita et al 2012, as well as other chondrogenic differentiation-related miRNAs (Guerit et al 2013, Martinez-Sanchez & Murphy 2013.…”

Section: Mirnas and Chondroblast Differentiationmentioning

confidence: 84%

“…Moreover, independent groups have developed miR-140-null mice, which displayed a concordant phenotype with major growth defects of endochondral bones (Miyaki et al 2010, Nakamura et al 2011, Papaioannou et al 2013. Interestingly, Sox9, L-Sox5, and Sox6 have been proved to cooperatively activate the miR-140 promoter in vivo and in vitro (Miyaki et al 2010, Yamashita et al 2012, as well as other chondrogenic differentiation-related miRNAs (Guerit et al 2013, Martinez-Sanchez & Murphy 2013. miR-181a is highly expressed in chondrocytes, and it has been suggested that it works as a negative feedback system to preserve the homeostasis of cartilage by targeting Ccn1 (Ccna2; which promotes chondrogenesis) and Acan (encoding the protein aggrecan, the major proteoglycan in the cartilage ECM) (Sumiyoshi et al 2013).…”

Section: Mirnas and Chondroblast Differentiationmentioning

confidence: 99%

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MicroRNAs and post-transcriptional regulation of skeletal development

Gámez¹,

Rodríguez-Carballo²,

Ventura³

2014

Journal of Molecular Endocrinology

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MicroRNAs (miRNAs) have become integral nodes of post-transcriptional control of genes that confer cellular identity and regulate differentiation. Cell-specific signaling and transcriptional regulation in skeletal biology are extremely dynamic processes that are highly reliant on dose-dependent responses. As such, skeletal cell-determining genes are ideal targets for quantitative regulation by miRNAs. So far, large amounts of evidence have revealed a characteristic temporal miRNA signature in skeletal cell differentiation and confirmed the essential roles that numerous miRNAs play in bone development and homeostasis. In addition, microarray expression data have provided evidence for their role in several skeletal pathologies. Mouse models in which their expression is altered have provided evidence of causal links between miRNAs and bone abnormalities. Thus, a detailed understanding of the function of miRNAs and their tight relationship with bone diseases would constitute a powerful tool for early diagnosis and future therapeutic approaches.

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Section: Mirnas and Chondroblast Differentiationmentioning

confidence: 84%

Section: Mirnas and Chondroblast Differentiationmentioning

confidence: 99%

MicroRNAs and post-transcriptional regulation of skeletal development

Gámez¹,

Rodríguez-Carballo²,

Ventura³

2014

Journal of Molecular Endocrinology

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“…2 Abnormalities in cartilage development have been observed in Dicer gene dysfunction models, and miRNA is known to play a key role in cartilage differentiation. 3 miRNA plays a key role in differentiation and growth in organs and tissues, 2 and miRNAs expressed specifically in cartilage [4][5][6][7][8] have been reported. Till date, miR21, 4 miR22, 9 miR27a, 6 miR140, 10 and miR146 8 have been reported as miRNAs that are associated with cartilage metabolism.…”

mentioning

confidence: 99%

MicroRNA‐199a‐3p, microRNA‐193b, and microRNA‐320c are correlated to aging and regulate human cartilage metabolism

Ukai

Sato

Akutsu

et al. 2012

Journal Orthopaedic Research

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MicroRNAs (miRNAs) are small RNAs of $22 base pairs that regulate gene expression. We harvested cartilage tissue from patients with polydactylism, anterior cruciate ligament injury, and osteoarthritis undergoing total knee arthroplasty and used microarrays to identify miRNAs whose expression is upregulated or downregulated with age. The results were assessed by real-time PCR and MTT assay in a mimic group, in which synthetic double-stranded RNA from the isolated miRNA was transfected to upregulate expression, and in an inhibitor group, in which the miRNA was bound specifically to downregulate expression. The expression of two miRNAs (miR-199a-3p and miR-193b) was upregulated with age and that of one miRNA (miR-320c) was downregulated with age. A real-time PCR assay showed that type 2 collagen, aggrecan, and SOX9 expression were downregulated in the miR-199a-3p mimic group but was upregulated in the inhibitor group. Similar results were observed for miR-193b. By contrast, ADAMTS5 expression was downregulated in the miR-320c mimic group and upregulated in the inhibitor group. Cell proliferative activity was upregulated significantly in the miR-193b inhibitor group compared with the control group. We believe that miR-199a-3p and miR-193b are involved in the senescence of chondrocytes, and miR-320c is involved in the juvenile properties of chondrocytes. ß

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“…miRs also serve crucial roles in cell proliferation, apoptosis and differentiation (15 is regulated by miRs in humans (16). Furthermore, a number of studies have demonstrated that miR is not only involved in the regulation of cartilage development, but also serves pivotal roles in the pathogenesis of the nucleus pulposus degeneration and arthritis (17,18). However, it remains unknown whether miR is associated with the molecular mechanism of CEP degeneration.…”

Section: Introductionmentioning

confidence: 99%

Expression of miR-625 and Fas in cervical vertebral cartilage endplate

Zhan

Wang

et al. 2017

Exp Ther Med

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Abstract. The aim of the present study was to assess miR-625 and Fas expression in normal and degenerative cervical cartilage endplate (CEP) tissues. Following biof-informatics analysis, the Fas gene was predicted to be one of the targets of miR-625. Quantitative PCR (qPCR) and western blotting were used to detect miR-625 and Fas expression in normal and degenerative CEP. A luciferase reporter assay was used to identify whether miR-625 could directly target the 3' untranslated region (3'-UTR) of Fas. Lentiviral overexpression and/or inhibition vectors of miR-625 (pre-miR-625)/antigomiR-625 were constructed to determine whether overexpression or inhibition of miR-625 could affect Fas and B-cell lymphoma 2 (Bcl-2) expression in cartilaginous endplate cells (CECs) and tissues. qPCR analysis demonstrated that miR-625 expression in degenerative CEP was significantly lower than in normal CEP tissue, while the production of Fas in degenerated CEP was significantly higher. Results from western blotting also showed a significant increase in Fas expression in degenerative CEP. miR-625 can bind directly to the 3'-UTR of the Fas gene. However, this inhibition was attenuated by a target mutation in the miR-625-binding site of the 3'-UTR of Fas mRNA. In addition, following transfection of CECs with pre-miR-625 and antigomiR-625, expression of Fas significantly decreased and increased, respectively, and Bcl-2 expression was upregulated and downregulated, respectively. Upregulation of miR-625 can inhibit Fas expression and further affect Bcl-2 expression in CEP degeneration, suggesting that miR-625-mediated inhibition of the Fas gene is important in cervical degeneration.

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MicroRNA-140 plays dual roles in both cartilage development and homeostasis

Cited by 531 publications

References 41 publications

MicroRNAs and post-transcriptional regulation of skeletal development

MicroRNAs and post-transcriptional regulation of skeletal development

MicroRNA‐199a‐3p, microRNA‐193b, and microRNA‐320c are correlated to aging and regulate human cartilage metabolism

Expression of miR-625 and Fas in cervical vertebral cartilage endplate

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