Sp1 and Sp3 Transcription Factors Mediate Malondialdehyde-induced Collagen α1(I) Gene Expression in Cultured Hepatic Stellate Cells

Garcia‐Ruiz, Itziar; Torre, Paz de la; Díaz, Teresa Cobo; Esteban, Elena; Fernández, Inmaculada; Muņoz‐Yagüe, Teresa; Solı́s-Herruzo, José A.

doi:10.1074/jbc.m203368200

Cited by 42 publications

(25 citation statements)

References 52 publications

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“…Among them, Sp1 levels were significantly increased when compared with controls in these cells. Findings from previous studies have also demonstrated the Sp1/Sp3 association with the collagen biosynthetic pathway (Chen et al, 1998;Ruiz et al, 2000;Czuwara-Ladykowska et al, 2001;Garcia-Ruiz et al, 2002). Our RT-PCR data also demonstrate ET-induced expression of Sp1, whereas rottlerin and PD98059 attenuated the Fig.…”

Section: Role Of Pkc␦ In Et-induced Collagen Expression 695supporting

confidence: 72%

“…One study on osteoblastic cells suggests the involvement of PKC and ERK pathways in TGF-␤ 1 -induced type I collagen expression (Palcy and Goltzman, 1999). Several previous reports have implicated the role of Sp1 and Sp3 in collagen transcription in various models (Li et al, 1995;Chen et al, 1998;Ihn and Tamaki, 2000;Ruiz et al, 2000;Czuwara-Ladykowska et al, 2001;Garcia-Ruiz et al, 2002). In the present study, we show a role for PKC, ERK1/2, and Sp1 in ET-induced type I collagen expression in cardiac myoFb.…”

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confidence: 64%

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Role of Protein Kinase Cδ in Endothelin-Induced Type I Collagen Expression in Cardiac Myofibroblasts Isolated from the Site of Myocardial Infarction

Chintalgattu

Katwa²

2004

J Pharmacol Exp Ther

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The role of endothelin-1 (ET) in tissue remodeling/fibrogenesis has been demonstrated in various in vitro and in vivo models. Our previous studies have revealed ET-induced expression of type I collagen in cardiac myofibroblasts (myoFb). Here we report that protein kinase C␦ (PKC␦) and mitogen-activated protein kinase/extracellular signal-regulated kinase-1/2 (MAPK/ERK1/2) play a role in ET-induced type I collagen expression using specific pharmacological inhibitors. The present study also reveals the expression of various isoforms of PKC including PKC␣, PKC␤I, PKC␤II, PKC␥, PKC␦, PKC⑀, PKC, and PKC in cardiac myoFb. Our results from mRNA and protein studies demonstrate that calphostin-C, a PKC inhibitor, decreased the ET-induced type I collagen expression suggesting a role for the PKC pathway. Further treatment with rottlerin, a PKC␦ isoform-specific inhibitor, demonstrated attenuation of 80 to 90% of type I collagen expression induced by ET. However, Go6976 [12-(2-cyanoethyl)-6,7,12,13-tetrahydro-13-methyl-5-oxo-5H-indolo[2,3-a]pyrrolo [3,4-c]carbazole]], an inhibitor of Ca 2ϩ -dependent PKC isoforms (PKC␣ and PKC␤I), showed little to no effect on ET-stimulated type I collagen expression. Furthermore, the MAPK inhibitor PD98059 (2Ј-amino-3Ј-methoxyflavone) attenuated ETdependent activation of p44/42 MAPK (pERK1/2) and also down-regulated type I collagen expression. Similarly, rottlerin inhibited the activation of p44/42 MAPK (pERK) implicating the involvement of PKC and MAPK/ERK1/2 in ET-induced type I collagen expression. Our protein/DNA array and reverse transcription-polymerase chain reaction results from ET-treated samples showed a significant increase in Sp1 expression. PD98059 and rottlerin decreased ET-induced Sp1 expression, suggesting a possible interaction of Sp1 with PKC␦ and MAPK in ET-induced type I collagen expression in cardiac myoFb.

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Section: Role Of Pkc␦ In Et-induced Collagen Expression 695supporting

confidence: 72%

supporting

confidence: 64%

Role of Protein Kinase Cδ in Endothelin-Induced Type I Collagen Expression in Cardiac Myofibroblasts Isolated from the Site of Myocardial Infarction

Chintalgattu

Katwa²

2004

J Pharmacol Exp Ther

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“…The best-studied component of hepatic scar is collagen type I, the expression of which is regulated both transcriptionally and posttranscriptionally in hepatic stellate cells by a growing number of stimuli and pathways. A detailed review of collagen gene regulation in stellate cells is beyond the focus of this review, but several recent references are recommended (7,188,257,258,260,354,528,(617)(618)(619)652).…”

Section: Perpetuationmentioning

confidence: 99%

Hepatic Stellate Cells: Protean, Multifunctional, and Enigmatic Cells of the Liver

Friedman

2008

Physiological Reviews

2,388

2,549

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The hepatic stellate cell has surprised and engaged physiologists, pathologists, and hepatologists for over 130 years, yet clear evidence of its role in hepatic injury and fibrosis only emerged following the refinement of methods for its isolation and characterization. The paradigm in liver injury of activation of quiescent vitamin A-rich stellate cells into proliferative, contractile, and fibrogenic myofibroblasts has launched an era of astonishing progress in understanding the mechanistic basis of hepatic fibrosis progression and regression. But this simple paradigm has now yielded to a remarkably broad appreciation of the cell's functions not only in liver injury, but also in hepatic development, regeneration, xenobiotic responses, intermediary metabolism, and immunoregulation. Among the most exciting prospects is that stellate cells are essential for hepatic progenitor cell amplification and differentiation. Equally intriguing is the remarkable plasticity of stellate cells, not only in their variable intermediate filament phenotype, but also in their functions. Stellate cells can be viewed as the nexus in a complex sinusoidal milieu that requires tightly regulated autocrine and paracrine cross-talk, rapid responses to evolving extracellular matrix content, and exquisite responsiveness to the metabolic needs imposed by liver growth and repair. Moreover, roles vital to systemic homeostasis include their storage and mobilization of retinoids, their emerging capacity for antigen presentation and induction of tolerance, as well as their emerging relationship to bone marrow-derived cells. As interest in this cell type intensifies, more surprises and mysteries are sure to unfold that will ultimately benefit our understanding of liver physiology and the diagnosis and treatment of liver disease.

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“…Similar to the aforementioned net activation of a signaling cascade following inhibition of a signaling protein, the inhibition and alkylation of the lipid and protein dual phosphatase PTEN (phosphatase and tensin homolog) was demonstrated to coincide with, and postulated to mediate, stimulation of PI3K/Akt signaling by exposure of cells to HNE [ 76 ]. Further examples of such alkylations by lipid peroxidation products inducing pathophysiologically relevant signaling processes include the stimulated expression of the proinfl ammatory protein cyclooxygenase-2 (COX-2) via stress-responsive kinase p38 MAPK upon exposure to HNE [ 77 ], or the stimulation of collagen expression (a crucial step in the pathogenesis of fi brosis) in fi broblasts [ 78 ] or hepatic stellate cells [ 79 ] following exposure to MDA.…”

Section: Lipid Peroxidation Productsmentioning

confidence: 99%

Reactive Oxygen Species as Initiators and Mediators of Cellular Signaling Processes

Klotz

2015

Oxidative Stress in Applied Basic Research and Clinical Practice

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Sp1 and Sp3 Transcription Factors Mediate Malondialdehyde-induced Collagen α1(I) Gene Expression in Cultured Hepatic Stellate Cells

Cited by 42 publications

References 52 publications

Role of Protein Kinase Cδ in Endothelin-Induced Type I Collagen Expression in Cardiac Myofibroblasts Isolated from the Site of Myocardial Infarction

Role of Protein Kinase Cδ in Endothelin-Induced Type I Collagen Expression in Cardiac Myofibroblasts Isolated from the Site of Myocardial Infarction

Hepatic Stellate Cells: Protean, Multifunctional, and Enigmatic Cells of the Liver

Reactive Oxygen Species as Initiators and Mediators of Cellular Signaling Processes

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