FGF2-induced Ras/Erk MAPK signalling maintains lymphatic endothelial cell identity by up-regulating endothelial cell-specific gene expression and suppressing TGFβ signalling via Smad2

Ichise, Taeko; Yoshida, Nobuaki; Ichise, Hirotake

doi:10.1242/jcs.137836

Cited by 51 publications

(58 citation statements)

References 57 publications

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“…Interestingly, the expression of another microRNA that inhibits ALK5 expression, let-7b, is also highly dependent on FGF2 signaling, as the loss of FGFR1 results in the ablation of let-7b levels and an increase TGFβ activity and EndMT (Chen et al, 2012). These data corroborate and extend earlier reports where FGF2 was reported to reduce endothelial sensitivity to TGFβ (Kawai-Kowase et al, 2004;Ichise et al, 2014).…”

Section: (B-e) Light Microscopy Images Of Endothelial Cells (B) Untrsupporting

confidence: 87%

“…Interestingly, although we and others describe a protective effect of FGF2 against EndMT induction in mature and progenitor endothelial cells (Moonen et al, 2010;Ichise et al, 2014), others have linked FGF2 signaling to EndMT induction (Ghosh et al, 2010;Lee et al, 2012). Indeed, FGF2 is known to inhibit EndMT in macrovascular endothelial cells, whereas it induces EndMT is some microvascular endothelial cell types (Lee et al, 2004;Lee and Kay, 2006).…”

Section: (B-e) Light Microscopy Images Of Endothelial Cells (B) Untrmentioning

confidence: 73%

“…Endothelial mitogens inhibit EndMT (Medici and Kalluri, 2012;Okayama et al, 2012;Ichise et al, 2014;Zhang et al, 2015). We questioned whether this inhibitory effect might be (in part) due to the induction of miR-20a.…”

Section: Fgf2 Induces Mir-20a and Inhibits Endmtmentioning

confidence: 99%

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FGF2 inhibits endothelial–mesenchymal transition through microRNA-20a-mediated repression of canonical TGF-β signaling

Correia

Moonen

Brinker

et al. 2016

Journal of Cell Science

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Endothelial-to-mesenchymal transition (EndMT) is characterized by the loss of endothelial cell markers and functions, and coincides with de novo expression of mesenchymal markers. EndMT is induced by TGFβ1 and changes endothelial microRNA expression. We found that miR-20a is decreased during EndMT, and that ectopic expression of miR-20a inhibits EndMT induction. TGFβ1 induces cellular hypertrophy in human umbilical vein endothelial cells and abrogates VE-cadherin expression, reduces endothelial sprouting capacity and induces the expression of the mesenchymal marker SM22α (also known as TAGLN). We identified ALK5 (also known as TGFBR1), TGFBR2 and SARA (also known as ZFYVE9) as direct miR-20a targets. Expression of miR-20a mimics abrogate the endothelial responsiveness to TGFβ1, by decreasing ALK5, TGFBR2 and SARA, and inhibit EndMT, as indicated by the maintenance of VE-cadherin expression, the ability of the cells to sprout and the absence of SM22α expression. FGF2 increases miR-20a expression and inhibits EndMT in TGFβ1-stimulated endothelial cells. In summary, FGF2 controls endothelial TGFβ1 signaling by regulating ALK5, TGFBR2 and SARA expression through miR-20a. Loss of FGF2 signaling combined with a TGFβ1 challenge reduces miR-20a levels and increases endothelial responsiveness to TGFβ1 through elevated receptor complex levels and activation of Smad2 and Smad3, which culminates in EndMT.

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Section: (B-e) Light Microscopy Images Of Endothelial Cells (B) Untrsupporting

confidence: 87%

Section: (B-e) Light Microscopy Images Of Endothelial Cells (B) Untrmentioning

confidence: 73%

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FGF2 inhibits endothelial–mesenchymal transition through microRNA-20a-mediated repression of canonical TGF-β signaling

Correia

Moonen

Brinker

et al. 2016

Journal of Cell Science

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“…Overexpression of H-Ras rescued the EndMT-suppressing effects of FGF2 depletion via inhibition of TGFβ-mediated SMAD2 activation, implicating FGF2/FGFR/Ras in TGFβ signaling and maintenance of endothelial cellular identity. Knockdown of endogenous Ras reduced endothelial markers, suggesting that baseline Ras activity maintains endothelial and suppresses mesenchymal phenotypes in endothelial cells [103]. Taken together, these data suggest that FGF2 is able to prevent or reverse transdifferentiation to myofibroblasts from precursors such as endothelial and epithelial cells.…”

Section: Fgf2 Antagonizes Contractile Phenotypes and Myofibroblast DImentioning

confidence: 99%

Fibroblast Growth Factor 2 as an Antifibrotic: Antagonism of Myofibroblast Differentiation and Suppression of Pro-Fibrotic Gene Expression

Dolivo

Larson

Dominko

2017

Cytokine & Growth Factor Reviews

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Fibrosis is a pathological condition that is characterized by the replacement of dead or damaged tissue with a nonfunctional, mechanically aberrant scar, and fibrotic pathologies account for nearly half of all deaths worldwide. The causes of fibrosis differ somewhat from tissue to tissue and pathology to pathology, but in general some of the cellular and molecular mechanisms remain constant regardless of the specific pathology in question. One of the common mechanisms underlying fibroses is the paradigm of the activated fibroblast, termed the “myofibroblast,” a differentiated mesenchymal cell with demonstrated contractile activity and a high rate of collagen deposition. Fibroblast growth factor 2 (FGF2), one of the members of the mammalian fibroblast growth factor family, is a cytokine with demonstrated antifibrotic activity in non-human animal, human, and in vitro models. FGF2 is highly pleiotropic and its receptors are present on many different cell types throughout the body, lending a great deal of variety to the potential mechanisms of FGF2 effects on fibrosis. However, recent reports demonstrate that a substantial contribution to the antifibrotic effects of FGF2 comes from the inhibitory effects of FGF2 on connective tissue fibroblasts, activated myofibroblasts, and myofibroblast progenitors. FGF2 demonstrates effects antagonistic towards fibroblast activation and towards mesenchymal transition of potential myofibroblast-forming cells, as well as promotes a gene expression paradigm more reminiscent of regenerative healing, such as that which occurs in the fetal wound healing response, than fibrotic resolution. With a better understanding of the mechanisms by which FGF2 alters the wound healing cascade and results in a shift away from scar formation and towards functional tissue regeneration, we may be able to further address the critical need of therapy for varied fibrotic pathologies across myriad tissue types.

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“…2D) 62 . FGF2 also induces ERK1/2 activation 63 . And FGF2-dependent ERK1/2 signaling plays a key role in the maintenance of VEGFR2 expression 1 .…”

Section: Biology Of Rtk Endocytosis In Endotheliummentioning

confidence: 99%

Receptor Tyrosine Kinases Endocytosis in Endothelium

Zhang

Simons

2014

ATVB

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Receptor tyrosine kinases (RTKs) are involved in regulation of key process in roles in endothelial biology including proliferation, migration and angiogenesis. It is now generally accepted that RTK signaling occurs intracellularly as well as on the plasma membrane although many important details remain to be worked out. Endocytosis and subsequent intracellular trafficking spatiotemporally regulate RTK signaling while “signaling endosomes” provide a platform for the compartmentalization of signaling events. This review summarizes recent advances in our understanding of endothelial RTK endocytosis and signaling using vascular endothelial growth factor receptor-2 as a paradigm.

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FGF2-induced Ras/Erk MAPK signalling maintains lymphatic endothelial cell identity by up-regulating endothelial cell-specific gene expression and suppressing TGFβ signalling via Smad2

Cited by 51 publications

References 57 publications

FGF2 inhibits endothelial–mesenchymal transition through microRNA-20a-mediated repression of canonical TGF-β signaling

FGF2 inhibits endothelial–mesenchymal transition through microRNA-20a-mediated repression of canonical TGF-β signaling

Fibroblast Growth Factor 2 as an Antifibrotic: Antagonism of Myofibroblast Differentiation and Suppression of Pro-Fibrotic Gene Expression

Receptor Tyrosine Kinases Endocytosis in Endothelium

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