A Role for the β-Catenin/T-Cell Factor Signaling Cascade in Vascular Remodeling

Wang, Xiaohong; Yan, Xiao; Mou, Yongshan; Zhao, Ying; Blankesteijn, W. Matthijs; Hall, Jennifer L.

doi:10.1161/hh0302.104466

Cited by 182 publications

(198 citation statements)

References 40 publications

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“…Altogether, this data suggest Wnt3a alters the phenotype of vascular smooth muscle cells. As Wnt signaling is upregulated after vascular injury, 7,14 this data highlight a potential role for Wnt3a in controlling smooth muscle cell phenotype during vascular wound repair and remodeling processes.…”

Section: Discussionmentioning

confidence: 83%

“…These channels are comprised of subunit proteins encoded by the multigene connexin family, of which connexin 43 is the predominant connexin expressed by vascular smooth muscle cells. 28 It has previously been reported that connexin 43 expression is upregulated in smooth muscle cells in response to injury in rodent models and in early human atherosclerosis, situations in which elevated Wnt signaling has been reported 7,14 and in which increased extracellular matrix synthesis is well documented. 3,38 Reducing connexin 43 expression has been shown to inhibit lesion development in rodent models of atherosclerosis and acute vascular injury, [39][40][41] suggesting potential pro-atherogenic functions for gap junction communication.…”

Section: Discussionmentioning

confidence: 99%

“…5,6 Growing evidence suggest a role for the Wnt family of secreted glycoproteins and their associated signaling pathways in regulating many of the processes involved in vascular wound repair and remodeling events. [7][8][9][10][11][12][13][14] However, the precise mechanisms and outcomes of Wnt signaling in such settings remain unclear. Moreover, the effect of specific Wnt family members on vascular cell phenotype remain undefined.…”

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confidence: 99%

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WNT3A induces a contractile and secretory phenotype in cultured vascular smooth muscle cells that is associated with increased gap junction communication

Carthy

Luo

McManus

2012

Laboratory Investigation

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Evidence suggests a role for Wnt signaling in vascular wound repair and remodeling events. Despite this, very little is known about the effect of Wnt ligands on the structure and function of vascular cells. In this study, we treated vascular smooth muscle cells with 250 ng/ml of recombinant Wnt3a for 72 h and observed changes in the cell phenotype. Our data suggest Wnt3a completely alters the phenotype of vascular smooth muscle cells. The Wnt3a-treated cells appeared larger and had increased formation of stress fibers. These cells also had increased expression of the smooth muscle contractile proteins, calponin and smooth muscle a-actin, and contracted a collagen lattice faster than control cells. The Wnt3a-treated smooth muscle cells displayed increased extracellular matrix synthesis, as measured by collagen I and III mRNA expression, along with increased expression of MMP2 and MMP9, but decreased TIMP2 levels. The Wnt3a-induced change in cell phenotype was associated with increased expression of the gap junction protein connexin 43. Consistent with this, Wnt3a-treated smooth muscle cells displayed enhanced intercellular communication, as measured by the scrape-loading dye transfer technique. The canonical Wnt antagonist, dickkopf-related protein 1, completely reversed the contractile protein and connexin 43 expression seen in the Wnt3a-treated cells, suggesting these changes were dependent on canonical Wnt signaling. Collectively, this data suggest Wnt3a promotes a contractile and secretory phenotype in vascular smooth muscle cells that is associated with increased gap junction communication. Numerous studies have demonstrated that after arterial injury, vessel walls follow a response-to-injury pattern of wound healing leading to stenosis secondary to the neointimal accumulation of smooth muscle cells and extracellular matrix. 1-4 A number of soluble mediators released at the site of vascular injury act as molecular cues that guide smooth muscle cell responses during repair. 5,6 Growing evidence suggest a role for the Wnt family of secreted glycoproteins and their associated signaling pathways in regulating many of the processes involved in vascular wound repair and remodeling events. [7][8][9][10][11][12][13][14] However, the precise mechanisms and outcomes of Wnt signaling in such settings remain unclear. Moreover, the effect of specific Wnt family members on vascular cell phenotype remain undefined.The Wnt signaling pathway is best recognized for its role in the development of multi-cellular organisms, 15,16 and is critically involved in normal heart formation. 17 The Wnt family is comprised of 19 secreted glycoproteins that bind the Frizzled receptor and its co-receptor, lipoprotein receptorrelated proteins 5/6, to initiate an intracellular signaling cascade that controls the turnover of b-catenin. 18 In the absence of Wnt ligand, b-catenin is targeted for ubiquitinmediated degradation by the 26S proteasome. However, upon ligand stimulation, canonical Wnt signaling triggers a series of phosphorylation even...

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Section: Discussionmentioning

confidence: 83%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

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WNT3A induces a contractile and secretory phenotype in cultured vascular smooth muscle cells that is associated with increased gap junction communication

Carthy

Luo

McManus

2012

Laboratory Investigation

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“…Interestingly, Wnt signaling in ECs has been shown to activate proinflammatory gene expression via inhibition of canonical Wnt signaling and activation of the noncanonical Ca 2+ ‐dependent pathway via ligand Wnt5a 88, 89. Several studies have demonstrated a direct link between canonical Wnt signaling via ligands Wnt1, Wnt2, and Wnt3a and arterial smooth muscle cell proliferation, which underlies the intimal thickening stage of atherosclerosis 20, 21, 90, 91. Canonical Wnt signaling and LRP5 have also been directly implicated in the promotion of foam cell formation 6.…”

Section: Implication Of Wnt Signaling In Atherosclerosis Pathologicalmentioning

confidence: 99%

Atherosclerotic Calcification: Wnt Is the Hint

Albanese

Khan

Barratt

et al. 2018

JAHA

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“…Interestingly, a specific role for TCF-4 has been shown in the process of vascular remodelling. Moreover, transcriptional activation of TCF-4 turns on the nuclear factor-.B signalling pathway, which regulates inflammatory signalling pathways [5]. Data from the MONICA/KORA Surveys showed that the T allelemodel assessment of per cent beta cell function and fasting insulin, suggesting a role in pancreatic beta cell function [3].…”

Section: Introductionmentioning

confidence: 99%

TCF7L2 single nucleotide polymorphisms, cardiovascular disease and all-cause mortality: the Atherosclerosis Risk in Communities (ARIC) study

et al. 2008

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Aims/hypothesis We hypothesised that TCF7L2 single nucleotide polymorphisms (SNPs) are associated with cardiovascular disease (CVD) and that the associations differ in diabetic and non-diabetic persons. Methods Our analysis included black and white participants from the Atherosclerosis Risk in Communities study who were free of prevalent CVD at baseline and had been genotyped for rs7903146, rs12255372, rs7901695, rs11196205 and rs7895340 (n=13,369). Cox proportional hazard regression was used to estimate the associations between polymorphisms and incident events; logistic and linear regression were used for associations with baseline risk factor levels. Results TCF7L2 SNPs were not significantly associated with incident coronary heart disease, ischaemic stroke, CVD, prevalent peripheral artery disease (PAD) or all-cause mortality in the full cohort or when stratified by race. Conclusions/interpretation In the whole cohort, TCF7L2 SNPs were not associated with incident CVD, all-cause mortality or prevalent PAD. This result suggests that the increased health risk associated with rs7903146 genotype is specific to diabetes.

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A Role for the β-Catenin/T-Cell Factor Signaling Cascade in Vascular Remodeling

Cited by 182 publications

References 40 publications

WNT3A induces a contractile and secretory phenotype in cultured vascular smooth muscle cells that is associated with increased gap junction communication

WNT3A induces a contractile and secretory phenotype in cultured vascular smooth muscle cells that is associated with increased gap junction communication

Atherosclerotic Calcification: Wnt Is the Hint

TCF7L2 single nucleotide polymorphisms, cardiovascular disease and all-cause mortality: the Atherosclerosis Risk in Communities (ARIC) study

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