Smad3 Null Mice Develop Airspace Enlargement and Are Resistant to TGF-β-Mediated Pulmonary Fibrosis

Bonniaud, Philippe; Kolb, Martin; Galt, Tom; Robertson, John C.; Robbins, Clinton S.; Stämpfli, Martin R.; Lavery, Carol; Margetts, Peter J.; Roberts, Anita B.; Gauldie, Jack

doi:10.4049/jimmunol.173.3.2099

Cited by 351 publications

(293 citation statements)

References 64 publications

Supporting

Mentioning

267

Contrasting

Unclassified

Order By: Relevance

“…At the level of gene expression, we noticed that the duration of TIMP-1 upregulation following AdTGF-β3 was transient and returned to baseline by day 14, while this gene was persistently induced in AdTGF-β1 treated rats. These findings strongly support previous reports showing that transient fibrosis in the lungs following CTGF overexpression or using bleomycin or AdTGF-β1 in fibrosis resistant mice were accompanied by low levels of TIMP-1 gene induction (Bonniaud et al, 2004;Kolb et al, 2002).…”

Section: Discussionsupporting

confidence: 92%

Progressive pulmonary fibrosis is mediated by TGF-β isoform 1 but not TGF-β3

Ask

Bonniaud

Maaß

et al. 2008

The International Journal of Biochemistry & Cell Biology

Self Cite

154

114

View full text Add to dashboard Cite

Tissue repair is a well orchestrated biological process involving numerous soluble mediators, and an imbalance between these factors may result in impaired repair and fibrosis. Transforming growth factor (TGF) β is a key profibrotic element in this process and it is thought that its three isoforms act in a similar way. Here, we report that TGF-β3 administered to rat lungs using transient overexpression initiates profibrotic effects similar to those elicited by TGF-β1, but causes less severe and progressive changes. The data suggest that TGF-β3 does not lead to inhibition of matrix degradation in the same way as TGF-β1, resulting in non-fibrotic tissue repair. Further, TGF-β3 is able to downregulate TGF-β1 induced gene expression, suggesting a regulatory role of TGF-β3. TGF-β3 overexpression results in an upregulation of Smad proteins similar to TGF-β1, but is less efficient in inducing the ALK 5 and TGF-β type II receptor (TβRII). We provide evidence that this difference may contribute to the progressive nature of TGF-β1 induced fibrotic response, in contrast to the limited fibrosis observed following TGF-β3 overexpression. TGF-β3 is important in "normal wound healing", but is outbalanced by TGF-β1 in "fibrotic wound healing" in the lung.

show abstract

Section: Discussionsupporting

confidence: 92%

Progressive pulmonary fibrosis is mediated by TGF-β isoform 1 but not TGF-β3

Ask

Bonniaud

Maaß

et al. 2008

The International Journal of Biochemistry & Cell Biology

Self Cite

154

114

View full text Add to dashboard Cite

show abstract

“…Although studies by our group [12] and others [36] have shown the capacity of TGF-β1 to activate FAK in certain cell types, a role for SMAD3 in mediating this effect has not been previously demonstrated. The requirement for SMAD3 in FAK activation is consistent with a role for SMAD3 in myofibroblast differentiation both in-vitro [37,38] and in-vivo [39][40][41].…”

Section: Discussionsupporting

confidence: 73%

Combinatorial activation of FAK and AKT by transforming growth factor-β1 confers an anoikis-resistant phenotype to myofibroblasts

Horowitz

Rogers

Sharma

et al. 2007

Cellular Signalling

222

177

View full text Add to dashboard Cite

Transforming growth factor-β (TGF-β) is a prototypical tumour-suppressor cytokine with cytostatic and pro-apoptotic effects on most target cells; however, mechanisms of its pro-survival/antiapoptotic signalling in certain cell types and contexts remain unclear. In human lung fibroblasts, TGF-β1 is known to induce myofibroblast differentiation in association with the delayed activation of focal adhesion kinase (FAK) and protein kinase B (PKB/AKT). Here, we demonstrate that FAK and AKT are independently regulated by early activation of SMAD3 and p38 MAPK, respectively. Pharmacologic or genetic approaches that disrupt SMAD3 signalling block TGF-β1-induced activation of FAK, but not AKT; in contrast, disruption of early p38 MAPK signalling abrogates AKT activation, but does not alter FAK activation. TGF-β1 is able to activate AKT in cells expressing mutant FAK or in cells treated with an RGD-containing peptide that interferes with integrin signalling, inhibits FAK activation and induces anoikis (apoptosis induced by loss of adhesion signalling). TGF-β1 protects myofibroblasts from anoikis, in part, by activation of the PI3K-AKT pathway. Thus, TGF-β1 co-ordinately and independently activates the FAK and AKT protein kinase pathways to confer an anoikis-resistant phenotype to myofibroblasts. Activation of these prosurvival/anti-anoikis pathways in myofibroblasts likely contributes to essential roles of TGF-β1 in tissue fibrosis and tumour-promotion.

show abstract

“…Data TGF-b signaling in prostate cancer reactive stroma F Yang et al presented here are consistent with the implication of Smad3 in mediating wound healing and fibrosis. As might be predicted, Smad3 null mice were refractory to TGF-b1-induced pulmonary fibrosis (Bonniaud et al, 2004). However, the function of Smad3 in mediating TGF-b-induced responses in cancer-associated reactive stroma biology is poorly understood.…”

Section: Discussionmentioning

confidence: 95%

Fibroblast growth factor-2 mediates transforming growth factor-β action in prostate cancer reactive stroma

2007

View full text Add to dashboard Cite

Transforming growth factor-b (TGF-b) is overexpressed at sites of wound repair and in most adenocarcinomas including prostate cancer. In stromal tissues, TGF-b regulates cell proliferation, phenotype and matrix synthesis. To address mechanisms of TGF-b action in cancerassociated reactive stroma, we developed prostate stromal cells null for TGF-b receptor II (TbRII) or engineered to express a dominant-negative Smad3 to attenuate TGF-b signaling. The differential reactive stroma (DRS) xenograft model was used to evaluate altered stromal TGF-b signaling on LNCaP tumor progression. LNCaP xenograft tumors constructed with TbRII null or dominantnegative Smad3 stromal cells exhibited a significant reduction in mass and microvessel density relative to controls. Additionally, decreased cellular fibroblast growth factor-2 (FGF-2) immunostaining was associated with attenuated TGF-b signaling in stroma. In vitro, TGF-b stimulated stromal FGF-2 expression and release. However, stromal cells with attenuated TGF-b signaling were refractory to TGF-b-stimulated FGF-2 expression and release. Re-expression of FGF-2 in these stromal cells in DRS xenografts resulted in restored tumor mass and microvessel density. In summary, these data show that TGF-b signaling in reactive stroma is angiogenic and tumor promoting and that this effect is mediated in part through a TbRII/Smad3-dependent upregulation of FGF-2 expression and release.

show abstract

Smad3 Null Mice Develop Airspace Enlargement and Are Resistant to TGF-β-Mediated Pulmonary Fibrosis

Cited by 351 publications

References 64 publications

Progressive pulmonary fibrosis is mediated by TGF-β isoform 1 but not TGF-β3

Progressive pulmonary fibrosis is mediated by TGF-β isoform 1 but not TGF-β3

Combinatorial activation of FAK and AKT by transforming growth factor-β1 confers an anoikis-resistant phenotype to myofibroblasts

Fibroblast growth factor-2 mediates transforming growth factor-β action in prostate cancer reactive stroma

Contact Info

Product

Resources

About