Characterization of Carotid Smooth Muscle Cells during Phenotypic Transition

Goikuria, Haize; Freijo, María Del Mar; Manrique, Reyes Vega; Sastre, Marı́a Teresa Muñoz; Elizagaray, Elena; Lorenzo, Ana; Vandenbroeck, Koen; Alloza, Iraide

doi:10.3390/cells7030023

Cited by 25 publications

(31 citation statements)

References 44 publications

(59 reference statements)

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“…Furthermore, another study revealed that MKl2 functioned as a pro-migratory gene in VSMcs (34). in the present study, MKl2 was found to be underexpressed in the serum of patients with aS compared with that of healthy volunteers, which was consistent with the findings of a previous study (35). In addition, via gain-of-function and loss-of-function approaches, transfection with miR-142-5p inhibitor significantly increased the mRNA and protein expression level of MKL2 in HASMCs; however, transfection with MKl2-sirna resulted in a decreased MKL2 expression.…”

Section: Discussionsupporting

confidence: 93%

Downregulation of miR‑142‑5p inhibits human aortic smooth muscle cell proliferation and migration by targeting MKL2

Shang

Dai

et al. 2020

Mol Med Rep

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The increased proliferation and migration of vascular smooth muscle cells (VSMcs) are critical in the progression of atherosclerosis (aS). Platelet-derived growth factor type BB (PdGF-BB) may induce VSMc proliferation and migration. mir-142-5p plays a critical role in various biological processes, including tumorigenesis, angiogenesis and inflammation. However, whether miR-142-5p is involved in regulating the pathological process of arteriosclerosis remains to be elucidated. Therefore, in this study, the role of mir-142-5p in PdGF-BB-induced human aortic smooth muscle cell (HSAMC) proliferation and migration was investigated. The results revealed that the expression level of mir-142-5p was enhanced in the serum of patients with aS, while that of its target gene, myocardin-like protein 2 (MKl2) was decreased, compared with that in healthy volunteers. Moreover, there was a negative correlation between mir-142-5p and MKl2 expression in the serum of patients with aS. Furthermore, the downregulation of miR-142-5p inhibited PDGF-BB-induced HASMC proliferation and migration; however, the inhibition of HASMC proliferation and migration was reversed by co-transfection with small interfering rna (sirna) against MKl2 (sirna-MKl2). in addition, transfection with mir-142-5p inhibitor significantly increased the expression levels of MKl2, and decreased those of matrix metalloproteinase (MMP)2 and 9, and these effects were reversed by transfection with sirna-MKl2. Finally, MKl2 was proven to be a target of miR-142-5p. On the whole, the findings of the present study demonstrate that the downregulation of mir-142-5p inhibits human aortic smooth muscle cell (HSAMC) proliferation and migration possibly by targeting MKL2. Hence, miR-142-5p may prove to be a novel therapeutic target in the treatment of aS.

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Section: Discussionsupporting

confidence: 93%

Downregulation of miR‑142‑5p inhibits human aortic smooth muscle cell proliferation and migration by targeting MKL2

Shang

Dai

et al. 2020

Mol Med Rep

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“…Consistent with previous reports showing that DNA hypomethylating agents can remove the epigenetic “brake” and allow stem cells to undergo differentiation ( 17 ), we found that the DNA methylation inhibitor 5′-Aza not only upregulated expression of genes imperative for differentiation but also functionally depleted the LSC population and inhibited its colony formation ( 20 , 54 ). 5′-Aza-induced LSC differentiation was supported by the observation that 5′-Aza treatment significantly increased the expression of markers of fully differentiated smooth muscle cells, such as MYH11 ( 44 ). Notably, we found that RU486 pretreatment did not significantly affect the LM cells’ colony-forming activity and was less efficient in inhibiting LM regeneration compared with 5′-Aza treatment, suggesting that LSC deficient in steroid hormone receptors may remain quiescent, constituting a small population of cells resistant to RU486 treatment.…”

Section: Discussionmentioning

confidence: 88%

“…TIMP3, tissue inhibitor of metalloproteinase 3, regulates extracellular matrix at the tumor–stromal interface ( 39 ) and is critical in driving differentiation and decreasing tumorigenesis in the mammary gland and muscle tissues ( 40 , 41 ). The ROR2 pathway plays complex roles in stem cell function and carcinogenesis ( 42 , 43 ), and MYH11 is a marker of fully differentiated smooth muscle cells ( 44 ).…”

Section: Resultsmentioning

confidence: 99%

Targeting DNA Methylation Depletes Uterine Leiomyoma Stem Cell–enriched Population by Stimulating Their Differentiation

Liu

Yin

et al. 2020

Endocrinology

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Uterine leiomyoma is the most common tumor in women and can cause severe morbidity. Leiomyoma growth requires maintenance and proliferation of a stem cell population. Dysregulated DNA methylation has been reported in leiomyoma, but its role in leiomyoma stem cell regulation remains unclear. Here, we FACS sorted cells from human leiomyoma tissues into three populations: stem-cell like cells (LSC, 5%), intermediate cells (LIC, 7%), and differentiated cells (LDC, 88%) and analyzed the transcriptome and epigenetic landscape of leiomyoma cells at different differentiation stages. LSC harbored a unique methylome, with 8862 differentially methylated regions compared to LIC and 9444 compared to LDC, most of which were hypermethylated. Consistent with global hypermethylation, transcript levels of TET1 and TET3 methylcytosine dioxygenases were lower in LSC. Integrative analyses revealed an inverse relationship between methylation and gene expression changes during LSC differentiation. In LSC, hypermethylation suppressed genes important for myometrium- and leiomyoma-associated functions, including muscle contraction and hormone action, to maintain stemness. The hypomethylating drug, 5'-Aza stimulated LSC differentiation, depleting the stem cell population and inhibiting tumor initiation. Our data suggest that DNA methylation maintains the pool of LSC, which is critical for the regeneration of leiomyoma tumors.

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“…These analyses, however, confirmed that the two genes were heterogeneously expressed throughout the vessel and lesion, with the majority of Cnn1 expressed in the wall as expected, as it is a VSMC marker and this is where most VSMC are located. 16 Cnn1-expressing cells were also found in the cap of the plaque, showing the involvement of VSMC in cap formation. 17 Timp2 was dispersed throughout the whole artery and both present in the wall and the plaque with a tendency towards a higher expression within the plaque itself ( Figure 6C-E).…”

Section: Liraglutide Treatment Effects On Gene Expressionmentioning

confidence: 90%

Liraglutide treatment improves endothelial function in the Ldlr−/− mouse model of atherosclerosis and affects genes involved in vascular remodelling and inflammation

Bjørnholm

Skovsted

Mitgaard‐Thomsen

et al. 2020

Basic Clin Pharma Tox

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The cardiovascular outcome trials LEADER and SUSTAIN-6 for liraglutide and semaglutide, respectively, have shown a significant cardiovascular disease (CVD) risk reduction on top of standard of care in people with type 2 diabetes (T2D), at increased risk of CVD in addition to control of glycaemia. 1,2 The improved cardiovascular risk profile has been suggested to be attributed-at least partly-to the anti-inflammatory properties of these long-acting glucagon-like peptide-1 (GLP-1) receptor agonists (GLP-1RA) independently of weight loss. 3-5 However, the physiological and cellular mechanism behind the CVD benefit has not yet been fully uncovered. Using the ApoE−/− and the Ldlr−/− mouse models of atherosclerosis, liraglutide has been demonstrated to result

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Characterization of Carotid Smooth Muscle Cells during Phenotypic Transition

Cited by 25 publications

References 44 publications

Downregulation of miR‑142‑5p inhibits human aortic smooth muscle cell proliferation and migration by targeting MKL2

Downregulation of miR‑142‑5p inhibits human aortic smooth muscle cell proliferation and migration by targeting MKL2

Targeting DNA Methylation Depletes Uterine Leiomyoma Stem Cell–enriched Population by Stimulating Their Differentiation

Liraglutide treatment improves endothelial function in the Ldlr−/− mouse model of atherosclerosis and affects genes involved in vascular remodelling and inflammation

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