Transforming Growth Factor-β–Independent Role of Connective Tissue Growth Factor in the Development of Liver Fibrosis

Sakai, Keiko; Jawaid, Safdar; Sasaki, Takako; Bou‐Gharios, George; Sakai, Takao

doi:10.1016/j.ajpath.2014.06.009

Cited by 22 publications

(20 citation statements)

References 27 publications

(28 reference statements)

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“…Evidence has been introduced and suggested that overexpression of CTGF has been noted in numerous fibrotic disorders, including pulmonary,12 renal,13 hepatic,14 skin15 and cardiac fibrosis 11 16. In our previous study, we first demonstrated a significant upregulation of mRNA and protein expression levels of CTGF in the GO orbital fibroblasts as compared with those of normal controls 17.…”

mentioning

confidence: 75%

Expression and clinical significance of connective tissue growth factor (CTGF) in Graves' ophthalmopathy

Huang

Chang

et al. 2016

Br J Ophthalmol

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mentioning

confidence: 75%

Expression and clinical significance of connective tissue growth factor (CTGF) in Graves' ophthalmopathy

Huang

Chang

et al. 2016

Br J Ophthalmol

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“…TGF-b, for instance, is the dominant and prototypical profibrogenic factor in liver fibrosis. Mice with deficiencies in the TGF-b signaling pathway, including TGF-b receptor (9) and SMAD proteins (10,11), display resistance to liver fibrosis. On the other hand, transgenic mice with liver-specific ABBREVIATIONS: AcH3, acetylated H3; ALT, alanine aminotransferase; a-SMA, a smooth muscle actin; AST, aspartate aminotransferase; BDL, bile duct ligation; ChIP, chromatin immunoprecipitation; cKO, conditional knockout; DZNep, 3-deazaneplanocin A; ECM, extracellular matrix; EZH2, enhancer of zeste homolog 2; H3K27Me3, trimethylated histone 3 lysine 27; H3K4Me3, trimethylated histone 3 lysine 4; HSC, hepatic stellate cell; PPARg, peroxisome proliferator activated receptor g; qPCR, quantitative PCR; Rosi, rosiglitazone; siRNA, small interfering RNA; SIRT1, silent information regulator 1; WT, wild type overexpression of TGF-b are more prone to develop fibrosis when exposed to CCl 4 (12) or LPS (13).…”

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confidence: 99%

SIRT1 antagonizes liver fibrosis by blocking hepatic stellate cell activation in mice

Hong

Hao

et al. 2017

FASEB j.

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Hepatic stellate cells (HSCs) are a major source of fibrogenesis in the liver, contributing to cirrhosis. When activated, HSCs transdifferentiate into myofibroblasts and undergo profound functional alterations paralleling an overhaul of the transcriptome, the mechanism of which remains largely undefined. We investigated the involvement of the class III deacetylase sirtuin [silent information regulator 1 (SIRT1)] in HSC activation and liver fibrosis. SIRT1 levels were down-regulated in the livers in mouse models of liver fibrosis, in patients with cirrhosis, and in activated HSCs as opposed to quiescent HSCs. SIRT1 activation halted, whereas SIRT1 inhibition promoted, HSC transdifferentiation into myofibroblasts. Liver fibrosis was exacerbated in mice with HSC-specific deletion of SIRT1 [conditional knockout (cKO)], receiving CCl (1 mg/kg) injection or subjected to bile duct ligation, compared to wild-type littermates. SIRT1 regulated peroxisome proliferator activated receptor γ (PPARγ) transcription by deacetylating enhancer of zeste homolog 2 (EZH2) in quiescent HSCs. Finally, EZH2 inhibition or PPARγ activation ameliorated fibrogenesis in cKO mice. In summary, our data suggest that SIRT1 plays an essential role guiding the transition of HSC phenotypes.-Li, M., Hong, W., Hao, C., Li, L., Wu, D., Shen, A., Lu, J., Zheng, Y., Li, P., Xu, Y. SIRT1 antagonizes liver fibrosis by blocking hepatic stellate cell activation in mice.

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“…These findings indicate that TGF-β signaling is indeed a dominant pathway in the development of liver fibrosis [62]. However, elimination of TGF-β or TRII does not completely prevent the accumulation of Col I in chronic liver injury, and in particular, TRII knockout livers still remain ~46.4% fibrosis compared to wild type [61,62]. Therefore, these findings clearly indicate the TGF-β-independent mechanism(s) in the development of liver fibrosis (see Section 3).…”

Section: Transforming Growth Factor-β (Tgf-β)mentioning

confidence: 74%

“…We hypothesized that the removal of fibronectin or TGF-β signaling in vivo could prevent extensive ECM network formation following tissue damage. To define the functional identity of fibronectin and TGF-β signaling in adult tissue remodeling, we recently established two animal models lacking fibronectin (both isoforms) or TRII, respectively, in adult liver [14,62]. Our new findings suggest fibronectin-/TGF-β-independent mechanisms are involved in the development of liver fibrosis.…”

Section: Possible Mechanisms Of Collagen Network Formationmentioning

confidence: 87%

“…Knockout livers actually show significantly lower ECM deposition (~46% compared to controls) in carbon tetrachloride (CCl 4 )-induced chronic injury, which is accompanied by the decreased expression of myofibroblast marker alpha-smooth muscle actin (α-SMA). These findings indicate that TGF-β signaling is indeed a dominant pathway in the development of liver fibrosis [62]. However, elimination of TGF-β or TRII does not completely prevent the accumulation of Col I in chronic liver injury, and in particular, TRII knockout livers still remain ~46.4% fibrosis compared to wild type [61,62].…”

Section: Transforming Growth Factor-β (Tgf-β)mentioning

confidence: 99%

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Mechanisms of Collagen Network Organization in Response to Tissue/Organ Damage

Saneyasu¹,

Yoshioka²,

Sakai³

2016

Composition and Function of the Extracellular Matrix in the Human Body

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Fibrosis is a part of the wound-healing response to tissue damage and characterized by excessive accumulation of mainly type I collagen-containing extracellular matrices (ECMs). Transforming growth factor beta (TGF-β) is a profibrogenic master cytokine responsible for promoting differentiation of tissue-resident fibroblasts into myofibroblasts, upregulation of ECM production, and downregulation of ECM degradation. The formation of ECM is an essential response in wound healing. Fibronectin is an ECM glycoprotein substantially expressed during tissue repair. Based on in vitro findings, it has been widely accepted that collagen network organization was exclusively fibronectin matrix dependent. Unexpectedly, our fibronectin conditional knockout mouse models have demonstrated a fibronectin-independent mechanism of collagen fibril formation following injury and identified TGF-β signaling and type V collagen as essential elements for collagen fibrillogenesis. Interestingly, the targeting of the TGF-β signaling alone, as proposed in some recent antifibrotic therapies of chronic fibrotic diseases, is not sufficient to completely prevent liver fibrosis. In this chapter, we focus on the present knowledge of the mechanisms of the collagen network organization following tissue/organ damage and pathological processes of chronic fibrotic diseases.

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Transforming Growth Factor-β–Independent Role of Connective Tissue Growth Factor in the Development of Liver Fibrosis

Cited by 22 publications

References 27 publications

Expression and clinical significance of connective tissue growth factor (CTGF) in Graves' ophthalmopathy

Expression and clinical significance of connective tissue growth factor (CTGF) in Graves' ophthalmopathy

SIRT1 antagonizes liver fibrosis by blocking hepatic stellate cell activation in mice

Mechanisms of Collagen Network Organization in Response to Tissue/Organ Damage

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