Activin receptor-like kinase 2 and Smad6 regulate epithelial–mesenchymal transformation during cardiac valve formation

Desgrosellier, Jay S.; Mundell, Nathan A.; McDonnell, Maureen A.; Moses, Harold L.; Barnett, Joey V.

doi:10.1016/j.ydbio.2004.12.037

Cited by 81 publications

(111 citation statements)

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“…ALK2 has the highest sequence homology with ALK1 (ten Dijke et al, 1993). Further, ALK1 and ALK2 bind common ligands, interact with common RII subtypes, and mediate TGFb-associated function (Attisano et al, 1993;Ebner et al, 1993a, b;Miettinen et al, 1994;Ward et al, 2002;Goumans et al, 2003;Lebrin et al, 2004;Blanco et al, 2005;Desgrosellier et al, 2005). Using qRT-PCR, we found that ALK2 was expressed at high levels in PCa cells, and was over fourfold higher than ALK5 in both PC3 and PC3-M cells (Figure 5a).…”

Section: Eng Promotes Smad1 Signalingmentioning

confidence: 74%

Endoglin inhibits prostate cancer motility via activation of the ALK2-Smad1 pathway

et al. 2007

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Endoglin is a transforming growth factor b (TGFb) superfamily auxiliary receptor. We had previously shown that it suppressed prostate cancer (PCa) cell motility, and that its expression was lost during PCa progression. The mechanism by which endoglin inhibits PCa cell motility is unknown. Here we demonstrate that endoglin abrogates TGFb-mediated cell motility, but does not alter cell surface binding of TGFb. By measuring Smad-specific phosphorylation and Smad-responsive promoter activity, endoglin was shown to constitutively activate Smad1, with little-to-no effect upon Smad3. Knockdown of Smad1 increased motility and abrogated endoglin's effects. As type I activin receptor-like kinases (ALKs) are necessary for Smad activation, we went on to show that knockdown of ALK2, but not TGFbRI (ALK5), abrogated endoglinmediated decreases in cell motility and constitutively active ALK2 was sufficient to restore a low-motility phenotype in endoglin deficient cells. These findings provide the first evidence that endoglin decreases PCa cell motility through activation of the ALK2-Smad1 pathway.

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Section: Eng Promotes Smad1 Signalingmentioning

confidence: 74%

Endoglin inhibits prostate cancer motility via activation of the ALK2-Smad1 pathway

et al. 2007

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“…In addition, BMPs have the ability to redirect the differentiation of connective tissue progenitor cells [33][34][35] to orchestrate an endothelial-to-mesenchymal transition in these cells, often through inflammatory cell intermediates [36][37][38][39][40] . Interestingly, misexpression of constitutively active ACVR1/ALK2, a BMP type-I receptor and the gene mutated in fibrodysplasia ossificans progressiva, is sufficient to stimulate an endothelialto-mesenchymal transformation in endothelial cells of the heart 41 . Notably, BMP4, as well as hypoxia and inflammatory cytokines-conditions and factors that are present in the earliest preosseous lesions of heterotopic ossification-upregulate Tie2 in endothelial cells, which contributes to the angiogenic response 39,42 .…”

Section: Discussionmentioning

confidence: 99%

Identification of Progenitor Cells That Contribute to Heterotopic Skeletogenesis

Lounev

Ramachandran

Wosczyna

et al. 2009

The Journal of Bone and Joint Surgery-American Volume

268

342

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“…TBRII can also interact with another type I receptor, ALK2 (Ebner et al, 1993). ALK2 has been implicated in mediating TGF␤-stimulated EMT in AV cushion endocardial cells (Lai et al, 2000;Desgrosellier et al, 2005) and cultured NMuMG breast cancer epithelial cells (Miettinen et al, 1994). These data suggest that TGF␤ may signal by the activation of ALK5 or ALK2.…”

Section: Introductionmentioning

confidence: 92%

“…Activity of Smad6 protein produced by viral infection was determined by its ability to decrease Smad1-dependent alkaline phosphatase activity in C3H10T1/2 cells (McDonnell et al, 2001). Data regarding activity of viral constructs have been reported (Desgrosellier et al, 2005).…”

Section: Pe Explants Infected With Adenovirusmentioning

confidence: 99%

Transforming growth factor‐β stimulates epithelial–mesenchymal transformation in the proepicardium

Olivey

Mundell

Austin

et al. 2005

Developmental Dynamics

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The proepicardium (PE) migrates over the heart and forms the epicardium. A subset of these PE-derived cells undergoes epithelial-mesenchymal transformation (EMT) and gives rise to cardiac fibroblasts and components of the coronary vasculature. We report that transforming growth factor-␤ (TGF␤) 1 and TGF␤2 increase EMT in PE explants as measured by invasion into a collagen gel, loss of cytokeratin expression, and redistribution of ZO1. The type I TGF␤ receptors ALK2 and ALK5 are both expressed in the PE. However, only constitutively active (ca) ALK2 stimulates PE-derived epithelial cell activation, the first step in transformation, whereas caALK5 stimulates neither activation nor transformation in PE explants. Overexpression of Smad6, an inhibitor of ALK2 signaling, inhibits epithelial cell activation, whereas BMP7, a known ligand for ALK2, has no effect. These data demonstrate that TGF␤ stimulates transformation in the PE and suggest that ALK2 partially mediates this effect. Developmental Dynamics 235:50 -59, 2006.

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Activin receptor-like kinase 2 and Smad6 regulate epithelial–mesenchymal transformation during cardiac valve formation

Cited by 81 publications

References 50 publications

Endoglin inhibits prostate cancer motility via activation of the ALK2-Smad1 pathway

Endoglin inhibits prostate cancer motility via activation of the ALK2-Smad1 pathway

Identification of Progenitor Cells That Contribute to Heterotopic Skeletogenesis

Transforming growth factor‐β stimulates epithelial–mesenchymal transformation in the proepicardium

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