Activation of Fibroblast Procollagen α1(I) Transcription by Mechanical Strain Is Transforming Growth Factor-β-dependent and Involves Increased Binding of CCAAT-binding Factor (CBF/NF-Y) at the Proximal Promoter

Lindahl, Gisela; Chambers, Rachel C.; Papakrivopoulou, Jenny; Dawson, Sally J.; Jacobsen, Marianne C.; Bishop, June E.; Laurent, Geoffrey J.

doi:10.1074/jbc.m108966200

Cited by 133 publications

(100 citation statements)

References 59 publications

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“…Both epicardium and epicardial populated structures (i.e., sulcus region between atria and ventricles, AV cushions) are positive for Tgf␤3 and as such might relate to the production of procollagen-1 formation of the fibrous heart skeleton. This assumption is supported by a positive effect of Tgf␤ on the expression of procollagen-1 (Lindahl et al, 2002). In conclusion, the three Tgf␤ isoforms exhibit characteristic spatiotemporal expression patterns in the developing heart, which partly overlap, implying both specific and complementary functions during cardiovascular morphogenesis.…”

Section: Epicardiummentioning

confidence: 65%

Expression patterns of Tgfβ1–3 associate with myocardialisation of the outflow tract and the development of the epicardium and the fibrous heart skeleton

Molin

Bartram

Heiden

et al. 2003

Developmental Dynamics

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Transforming growth factor-beta (Tgf␤) is essential for normal embryogenesis. The cardiac phenotypes obtained after knockout of each of the three mammalian isoforms suggest different roles during morphogenesis. We studied cardiovascular expression of Tgf␤1-3 in parallel tissue sections of normal mouse embryos from 9.5 to 15.5 days post coitum (dpc) by using radioactive in situ hybridisation. The Tgf␤ isoforms are differentially expressed in unique and in overlapping patterns during cardiovascular development. In the vessels, Tgf␤1 is found in the intima, whereas Tgf␤2 and -␤3 are mainly present in the media and adventitia of the great arteries. Tgf␤1 is present in the endocardium at all stages examined. The Tgf␤2 signal in the endocardium of the atrioventricular canal and outflow tract (9.5 dpc) shifts during epithelial-mesenchymal transformation toward the mesenchymal cushions (10.5-11.5 dpc) after which it exhibits a marked spatiotemporal expression pattern as the cushion differentiation progresses (11.5-15.5 dpc). The myocardium underlying the endocardial cushions and the atrial muscular septum are intensely positive for Tgf␤2 at early stages (9.5-11.5 dpc) and expression decreases at 12.5 days. In contrast to earlier reports, we find marked overlap of Tgf␤2 and -␤3 expression. Tgf␤3 expression shows a characteristic distribution in the mesenchymal cushions, suggesting a role in cushion differentiation, possibly additional to Tgf␤2. From 14.5 dpc onward, a strong Tgf␤3 signal is found in the fibrous septum primum of the atrium and in the fibrous skeleton of the heart. Special attention was paid to the proepicardial organ and its derivatives. The proepicardial organ strongly expresses Tgf␤2 as early as 9.5 days, and all isoforms are present in the epicardium from 12.5 dpc onward. The spatiotemporal cardiovascular expression of Tgf␤1-3 supports both specific and complementary functions during cardiovascular development that might explain functional redundancy between the Tgf␤-isoforms. The information provided favors novel roles of Tgf␤1-3 in epicardial development, of Tgf␤2 in myocardialisation, and of Tgf␤3 in differentiation of the fibrous structures of the heart. Developmental Dynamics 227: 431-444, 2003.

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Section: Epicardiummentioning

confidence: 65%

Expression patterns of Tgfβ1–3 associate with myocardialisation of the outflow tract and the development of the epicardium and the fibrous heart skeleton

Molin

Bartram

Heiden

et al. 2003

Developmental Dynamics

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“…In DNA binding assays, the formation of a CBF/NF-Y complex was unchanged upon CTGF overexpression in isolation. CBF binding activity has been reported to be enhanced by TGF␤ in rat fibroblasts (29) and in explanted fibroblasts from the skin (39) and lungs (Lindahl GE: unpublished observations) of patients with SSc. It is therefore possible either that CTGF is not involved in CBF activation or, perhaps more likely, that other factors in combination with CTGF are needed for induced CBF binding activity in fibrosis.…”

Section: Discussionmentioning

confidence: 95%

“…Nuclear extracts from cells transfected with either the pCMV-CTGF expression vector or the pCMV-EV empty control vector were prepared as described previously (29). Binding reactions were prepared in EMSA binding buffer (Promega) using 2.5 g nuclear extract and a 5Ј-end 32 P-␥ATP-labeled doublestranded oligonucleotide probe, used on its own or together with either a cold competitor consensus oligonucleotide (Promega or Santa Cruz Biotechnology) or a specific supershift/ blocking antibody (Santa Cruz Biotechnology).…”

Section: Methodsmentioning

confidence: 99%

Pivotal role of connective tissue growth factor in lung fibrosis: MAPK‐dependent transcriptional activation of type I collagen

Ponticos

Holmes

et al. 2009

Arthritis & Rheumatism

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213

151

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Objective. Connective tissue growth factor (CTGF; CCN2) is overexpressed in systemic sclerosis (SSc) and has been hypothesized to be a key mediator of the pulmonary fibrosis frequently observed in this disease. CTGF is induced by transforming growth factor ␤ (TGF␤) and is a mediator of some profibrotic effects of TGF␤ in vitro. This study was undertaken to investigate the role of CTGF in enhanced expression of type I collagen in bleomycin-induced lung fibrosis, and to delineate the mechanisms of action underlying the effects of CTGF on Col1a2 (collagen gene type I ␣2) in this mouse model and in human pulmonary fibroblasts.Methods. Transgenic mice that were carrying luciferase and ␤-galactosidase reporter genes driven by the Col1a2 enhancer/promoter and the CTGF promoter, respectively, were injected with bleomycin to induce lung fibrosis (or saline as control), and the extracted pulmonary fibroblasts were incubated with CTGF blocking agents. In vitro, transient transfection, promoter/ reporter constructs, and electrophoretic mobility shift assays were used to determine the mechanisms of action of CTGF in pulmonary fibroblasts.Results. In the mouse lung tissue, CTGF expression and promoter activity peaked 1 week after bleomycin challenge, whereas type I collagen expression and Col1a2 promoter activity peaked 2 weeks postchallenge. Fibroblasts isolated from the mouse lungs 14 days after bleomycin treatment retained a profibrotic expression pattern, characterized by greatly elevated levels of type I collagen and CTGF protein and increased promoter activity. In vitro, inhibition of CTGF by specific small interfering RNA and neutralizing antibodies reduced the collagen protein expression and Col1a2 promoter activity. Moreover, in vivo, anti-CTGF antibodies applied after bleomycin challenge significantly reduced the Col1a2 promoter activity by ϳ25%. The enhanced Col1a2 promoter activity in fibroblasts from bleomycintreated lungs was partly dependent on Smad signaling, whereas CTGF acted on the Col1a2 promoter by a mechanism that was independent of the Smad binding site, but was, instead, dependent on the ERK-1/2 and JNK MAPK pathways. The CTGF effect was mapped to the proximal promoter region surrounding the inverted CCAAT box, possibly involving CREB and c-Jun. In human lung fibroblasts, the human COL1A2 promoter responded in a similar manner, and the mechanisms of action also involved ERK-1/2 and JNK signaling.Conclusion. Our results clearly define a direct profibrotic effect of CTGF and demonstrate its contribution to lung fibrosis through transcriptional activation

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“…These include the consensus TATA and CCAAT motifs, which are the potential targets for the action of promoter-specific transcription factors (Chu et al, 1985;De Wet et al, 1987). Transcriptional activation of rat COL1A1 gene in cardiac fibroblasts subjected to mechanical stretching with a 10% strain at 1 Hz, similar to the physiological tension experienced by the cells in the heart, has been reported to be mediated by autocrine stimulation by TGF-β (Lindahl et al, 2002). This activation involves TGF-β response elements in the promoter region of the collagen gene and increased binding of CCAAT-binding factor (CBF/NF-Y) at the proximal promoter.…”

Section: Regulation Of Gene Expression In Fibroblasts By Mechanical Lmentioning

confidence: 96%

“…Finally, mechanisms that include triggering autocrine or paracrine release of growth factors such as TGF-β by mechanical loads to regulate the transcription of "mechanoresponsive genes" are also presented (Davies et al, 1997;Sadoshima and Izumo, 1997). Mechanical stress stimulates the release of TGF-β (Lindahl et al, 2002;Nakatani et al, 2002;Yang et al, 2004) as described in the previous section, as well as enhances its gene transcription through activation of EGR-1 . These indirect mechanotransduction mechanisms have been explained in detail previously (Chiquet, 1999;Sarasa-Renedo and Chiquet, 2005).…”

Section: Cellular Mechanotransductionmentioning

confidence: 99%

Mechanoregulation of gene expression in fibroblasts

Wang

Thampatty

Lin

et al. 2007

Gene

224

187

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Mechanical loads placed on connective tissues alter gene expression in fibroblasts through mechanotransduction mechanisms by which cells convert mechanical signals into cellular biological events, such as gene expression of extracellular matrix components (e.g., collagen). This mechanical regulation of ECM gene expression affords maintenance of connective tissue homeostasis. However, mechanical loads can also interfere with homeostatic cellular gene expression and consequently cause the pathogenesis of connective tissue diseases such as tendinopathy and osteoarthritis. Therefore, the regulation of gene expression by mechanical loads is closely related to connective tissue physiology and pathology. This article reviews the effects of various mechanical loading conditions on gene regulation in fibroblasts and discusses several mechanotransduction mechanisms. Future research directions in mechanoregulation of gene expression are also suggested.

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Activation of Fibroblast Procollagen α1(I) Transcription by Mechanical Strain Is Transforming Growth Factor-β-dependent and Involves Increased Binding of CCAAT-binding Factor (CBF/NF-Y) at the Proximal Promoter

Cited by 133 publications

References 59 publications

Expression patterns of Tgfβ1–3 associate with myocardialisation of the outflow tract and the development of the epicardium and the fibrous heart skeleton

Expression patterns of Tgfβ1–3 associate with myocardialisation of the outflow tract and the development of the epicardium and the fibrous heart skeleton

Pivotal role of connective tissue growth factor in lung fibrosis: MAPK‐dependent transcriptional activation of type I collagen

Mechanoregulation of gene expression in fibroblasts

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