Fn14, a Downstream Target of the TGF-[beta] Signaling Pathway, Regulates Fibroblast Activation

Fibrosis, the hallmark of human injuries and diseases such as serious burns, is characterized by excessive collagen synthesis and myofibroblast accumulation. Transforming growth factor-[beta] (TGF-[beta]), a potent inducer of collagen synthesis, has been implicated in fibrosis in animals. In additio...

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Published in:PloS one 2015-12, Vol.10 (12)
Main Authors: Chen, Shaoxian, Liu, Juli, Yang, Min, Lai, Wen, Ye, Litong, Chen, Jing, Hou, Xinghua, Ding, Hong, Zhang, Wenwei, Wu, Yueheng, Liu, Xiaoying, Huang, Shufang, Yu, Xiyong, Xiao, Dingzhang
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Language:English
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Cellular signal transduction
Fibroblasts
Genetic aspects
Physiological aspects
Transforming growth factors
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creator Chen, Shaoxian
Liu, Juli
Yang, Min
Lai, Wen
Ye, Litong
Chen, Jing
Hou, Xinghua
Ding, Hong
Zhang, Wenwei
Wu, Yueheng
Liu, Xiaoying
Huang, Shufang
Yu, Xiyong
Xiao, Dingzhang
description Fibrosis, the hallmark of human injuries and diseases such as serious burns, is characterized by excessive collagen synthesis and myofibroblast accumulation. Transforming growth factor-[beta] (TGF-[beta]), a potent inducer of collagen synthesis, has been implicated in fibrosis in animals. In addition to TGF-[beta], fibroblast growth factor-inducible molecule 14 (Fn14) has been reported to play an important role in fibrotic diseases, such as cardiac fibrosis. However, the function and detailed regulatory mechanism of Fn14 in fibrosis are unclear. Here, we investigated the effect of Fn14 on the activation of human dermal fibroblasts. In normal dermal fibroblasts, TGF-[beta] signaling increased collagen production and Fn14 expression. Furthermore, Fn14 siRNA blocked extracellular matrix gene expression; even when TGF-[beta] signaling was activated by TGF-[beta]1, fibroblast activation remained blocked in the presence of Fn14 siRNA. Overexpressing Fn14 increased extracellular matrix gene expression. In determining the molecular regulatory mechanism, we discovered that SMAD4, an important TGF-[beta] signaling co-mediator, bound to the Fn14 promoter and activated Fn14 transcription. Taken together, these results indicate that the TGF-[beta] signaling pathway activates Fn14 expression through the transcription factor SMAD4 and that activated Fn14 expression increases extracellular matrix synthesis and fibroblast activation. Therefore, Fn14 may represent a promising approach to preventing the excessive accumulation of collagen or ECM in skin fibrosis.
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subjects Cellular signal transduction
Fibroblasts
Genetic aspects
Physiological aspects
Transforming growth factors
title Fn14, a Downstream Target of the TGF-[beta] Signaling Pathway, Regulates Fibroblast Activation
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