Lipoxins Attenuate Renal Fibrosis by Inducing let-7c and Suppressing TGFβR1

Brennan, Eoin; Nolan, Karen A.; Börgeson, Emma; Gough, Oisín S.; McEvoy, Caitríona M.; Docherty, Neil G.; Higgins, Debra F.; Murphy, Madeline; Sadlier, Denise; Ali-Shah, Syed Tasadaque; Guiry, Patrick J.; Savage, David A.; Maxwell, Alexander P.; Martin, Finian; Godson, Catherine

doi:10.1681/asn.2012060550

Cited by 140 publications

(133 citation statements)

References 46 publications

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“…Several molecules were proposed to be involved in the profibrotic switch of fibroblasts (or pericytes) during renal fibrosis, including the Wnt signaling pathway (e.g., Wnt4, LRP-6, and DKK-1) (183,184), oxidative stress and NADPH oxidase (39,88,185), integrins including aV integrin (186), Rheb/mTORC1 signaling (187) as well as lipid mediators, including prostaglandins and their receptors like EP4 (188,189), prostacyclins (190), or lipoxins (191,192).…”

Section: The Role Of Interstitial Mesenchymal Cellsmentioning

confidence: 99%

Renal Allograft Fibrosis: Biology and Therapeutic Targets

Floege

2015

American Journal of Transplantation

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Section: The Role Of Interstitial Mesenchymal Cellsmentioning

confidence: 99%

Renal Allograft Fibrosis: Biology and Therapeutic Targets

Floege

2015

American Journal of Transplantation

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“…Recently, it was found that under normal conditions, let-7 maintains low levels of TGF-␤R1 expression in human umbilical vein endothelial cells and in adult human liver cells (30,31). In addition, in tubular epithelial cells, lipoxins were shown to down-regulate TGF-␤R1-induced fibrosis by up-regulating let-7c (32). Another recent paper also showed that let-7b targets TGF-␤R1 related to kidney fibrosis (33).…”

Section: Micrornas (Mirnas)mentioning

confidence: 99%

“…1, A-C). Recent reports have identified TGF-␤R1 as a target of let-7c and let-7b in renal cells (30,32,33). Interestingly, computational analysis using Target Scan software identified TGF-␤R1 as a potential profibrotic target of not only let-7b but also the other two miRNAs, miR-130b and miR-30e*.…”

Section: Decreased Expression Of Mir-130b and Let-7b In Tgf-␤1-treatementioning

confidence: 99%

“…TGF-␤1 Induces TGF-␤R1 Expression via Down-regulation of miR-130b and let-7b-It was recently reported that let-7c and let-7b directly bind and target the TGF-␤R1 3Ј-UTR in renal epithelial cells, leading to an attenuation of downstream genes associated with renal fibrosis (32,33). let-7 was also shown to target TGF-␤R1 in adult human liver cells to regulate human liver development (30).…”

Section: Decreased Expression Of Mir-130b and Let-7b In Tgf-␤1-treatementioning

confidence: 99%

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Transforming Growth Factor β1 (TGF-β1) Enhances Expression of Profibrotic Genes through a Novel Signaling Cascade and MicroRNAs in Renal Mesangial Cells

Castro

Kato

Park

et al. 2014

Journal of Biological Chemistry

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Increased TGF‐β1 expression in glomerular mesangial cells (MC) augments extracellular matrix accumulation, hypertrophy and pro‐fibrotic genes during the progression of diabetic nephropathy (DN), a debilitating renal complication of diabetes. microRNAs (miRNAs) play key roles in the pathogenesis of DN by modulating the actions of TGF‐β1 to enhance the expression of pro‐fibrotic genes like collagen. In this study, we found a significant decrease in the expression of key members of the miR‐130 and miR‐30 families in mouse MC (MMC) treated with TGF‐β1. In parallel there was a decrease in host genes 2610318N02RIK (RIK, miR‐130b host gene) and NF‐YC (miR‐30e* host gene), suggesting host gene‐dependent expression of these miRNAs. TGF‐β receptor1 (TGF‐βR1), was identified as a target of miR‐130b. Interestingly, the RIK promoter contains three NF‐YC binding sites and was regulated by NF‐YC, a potential target of miR‐216a which was also up‐regulated by TGF‐β1. Therefore, a novel cascade, ↑TGF‐β1>↑miR‐216a>↓NF‐YC>↓RIK (↓miR‐130b) may up‐regulate TGF‐βR1 to augment expression of TGF‐β1 target fibrotic genes. miR‐130 and miR‐30e* were down‐regulated, whereas TGF‐βR1, as well as the pro‐fibrotic genes COLIVa1, COLXIIa1, CTGF and PAI‐1 were up‐regulated by TGF‐β1 in MMC and in the glomeruli of streptozotocin injected diabetic mice, supporting in vivo relevance. Together, these results demonstrate a novel miRNA‐ and their host gene‐mediated cascade initiated by TGF‐β1 which results in the up‐regulation of pro‐fibrotic factors such as TGF‐βR1 and collagens associated with the progression of DN. Grant Funding Source: Supported by NIH R01 DK081705 and ADA 7‐10‐MI‐07

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“…[33][34][35] More recently, LXA 4 exhibited antifibrotic properties by upregulation of let-7c expression in renal fibrosis. 36 However, whether LXA 4 augments AFC through a particular miRNA in LPS-induced ALI, and if so, what the underlying mechanisms are remain unclear.…”

mentioning

confidence: 99%

Lipoxin A4 activates alveolar epithelial sodium channel gamma via the microRNA-21/PTEN/AKT pathway in lipopolysaccharide-induced inflammatory lung injury

Cai

et al. 2015

Laboratory Investigation

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Lipoxin A 4 (LXA 4 ), as an endogenously produced lipid mediator, promotes the resolution of inflammation. Previously, we demonstrated that LXA 4 stimulated alveolar fluid clearance through alveolar epithelial sodium channel gamma (ENaC-γ). In this study, we sought to investigate the mechanisms of LXA 4 in modulation of ENaC-γ in lipopolysaccharide (LPS)-induced inflammatory lung injury. miR-21 was upregulated during an LPS challenge and downregulated by LXA 4 administration in vivo and in vitro. Serum miR-21 concentration was also elevated in acute respiratory distress syndrome patients as compared with healthy volunteers. LPS increased miR-21 expression by activation of activator protein 1 (AP-1). In A549 cells, miR-21 upregulated phosphorylation of AKT activation via inhibition of phosphatase and tensin homolog (PTEN), and therefore reduced the expression of ENaC-γ. In contrast, LXA 4 reversed LPS-inhibited ENaC-γ expression through inhibition of AP-1 and activation of PTEN. In addition, an miR-21 inhibitor mimicked the effects of LXA 4 ; overexpression of miR-21 abolished the protective effects of LXA 4 . Finally, both AKT and ERK inhibitors (LY294002 and UO126) blocked effects of LPS on the depression of ENaC-γ. However, LXA 4 only inhibited LPS-induced phosphorylation of AKT. In summary, LXA 4 activates ENaC-γ in part via the miR-21/PTEN/AKT signaling pathway.

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Lipoxins Attenuate Renal Fibrosis by Inducing let-7c and Suppressing TGFβR1

Cited by 140 publications

References 46 publications

Renal Allograft Fibrosis: Biology and Therapeutic Targets

Renal Allograft Fibrosis: Biology and Therapeutic Targets

Transforming Growth Factor β1 (TGF-β1) Enhances Expression of Profibrotic Genes through a Novel Signaling Cascade and MicroRNAs in Renal Mesangial Cells

Lipoxin A4 activates alveolar epithelial sodium channel gamma via the microRNA-21/PTEN/AKT pathway in lipopolysaccharide-induced inflammatory lung injury

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