PTEN loss defines a TGF-β-induced tubule phenotype of failed differentiation and JNK signaling during renal fibrosis

Lan, Rongpei; Geng, Hui; Polichnowski, Aaron J.; Singha, Prajjal K.; Saikumar, Pothana; McEwen, Donald G.; Griffin, Karen A.; Koesters, Robert; Weinberg, Joel M.; Bidani, A.; Kriz, Wilhelm; Venkatachalam, Manjeri A.

doi:10.1152/ajprenal.00660.2011

Cited by 102 publications

(98 citation statements)

References 48 publications

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“…There is little knowledge with respect to how cellular stress controls the production of profibrotic paracrine molecules. One main factor is the production of TGF-␤ (11,20,21,23,25,26,44,45). The TGF-␤ signaling pathway plays a major role in all fibrotic diseases.…”

Section: Discussionmentioning

confidence: 99%

Increased expression of p21^WAF1/CIP1 in kidney proximal tubules mediates fibrosis

Megyesi

Tarcsafalvi

et al. 2015

American Journal of Physiology-Renal Physiology

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Tissue fibrosis is a major cause of death in developed countries. It commonly occurs after either acute or chronic injury and affects diverse organs, including the heart, liver, lung, and kidney. Using the renal ablation model of chronic kidney disease, we previously found that the development of progressive renal fibrosis was dependent on p21WAF1/Cip1 expression; the genetic knockout of the p21 gene greatly alleviated this disease. In the present study, we expanded on this observation and report that fibrosis induced by two different acute injuries to the kidney is also dependent on p21. In addition, when p21 expression was restricted only to the proximal tubule, fibrosis after injury was induced in the whole organ. One molecular fibrogenic switch we describe is transforming growth factor-β induction, which occurred in vivo and in cultured kidney cells exposed to adenovirus expressing p21. Our data suggests that fibrosis is p21 dependent and that preventing p21 induction after stress could be a novel therapeutic target.

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Section: Discussionmentioning

confidence: 99%

Increased expression of p21^WAF1/CIP1 in kidney proximal tubules mediates fibrosis

Megyesi

Tarcsafalvi

et al. 2015

American Journal of Physiology-Renal Physiology

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“…TGF-␤ is a pleiotropic cytokine that plays a major role in stimulating extracellular matrix production after UUO, and blocking TGF-␤ has been shown to reduce tubular apoptosis in several models of chronic kidney injury (25,30). It contributes to renal fibrosis by several mechanisms including induced loss of phosphatase tensin homolog that contributes to the failure of regenerating epithelial cells to redifferentiate, thereby causing the retention of proliferative signaling and giving rise to profibrotic peptides (19). TGF-␤ also increases renal fibrosis not only by a direct effect on myofibroblasts but by inducing the production of Notch (1), CTGF (34), and PDGF␤ (40).…”

Section: Discussionmentioning

confidence: 99%

Proximal tubule PPARα attenuates renal fibrosis and inflammation caused by unilateral ureteral obstruction

Mariappan

Megyesi

et al. 2013

American Journal of Physiology-Renal Physiology

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“…In addition, autophagy has been implicated in tubular atrophy, 69,70 a pathologic phenotype in post-AKI tubules that may contribute critically to renal fibrosis. 71 It is also important to elucidate whether and how autophagy contributes to kidney repair after AKI, including fibrosis.…”

Section: Receptorsmentioning

confidence: 99%

Cellular and Molecular Mechanisms of AKI

Agarwal

Dong

Harris

et al. 2016

JASN

166

151

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In this article, we review the current evidence for the cellular and molecular mechanisms of AKI, focusing on epithelial cell pathobiology and related cell-cell interactions, using ischemic AKI as a model. Highlighted are the clinical relevance of cellular and molecular targets that have been investigated in experimental models of ischemic AKI and how such models might be improved to optimize translation into successful clinical trials. In particular, development of more context-specific animal models with greater relevance to human AKI is urgently needed. Comorbidities that could alter patient susceptibility to AKI, such as underlying diabetes, aging, obesity, cancer, and CKD, should also be considered in developing these models. Finally, harmonization between academia and industry for more clinically relevant preclinical testing of potential therapeutic targets and better translational clinical trial design is also needed to achieve the goal of developing effective interventions for AKI. Cellular and molecular mechanisms of AKI have been extensively investigated in a variety of experimental models, through which a number of candidate therapies for AKI have been identified. This article reviews the current evidence by dissecting the cellular and molecular mechanisms of AKI, focusing on epithelial cell pathobiology and related cell-cell interactions, and using the example of ischemic AKI to describe our approach. Specifically, we reviewed the cellular and molecular epithelial cell targets that have been investigated in experimental models of ischemic AKI, and considered the clinical relevance of these models in human AKI and how such models might be improved to optimize translation into successful clinical trials. We have structured our review to answer two key questions:

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PTEN loss defines a TGF-β-induced tubule phenotype of failed differentiation and JNK signaling during renal fibrosis

Cited by 102 publications

References 48 publications

Increased expression of p21^WAF1/CIP1 in kidney proximal tubules mediates fibrosis

Increased expression of p21^WAF1/CIP1 in kidney proximal tubules mediates fibrosis

Proximal tubule PPARα attenuates renal fibrosis and inflammation caused by unilateral ureteral obstruction

Cellular and Molecular Mechanisms of AKI

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PTEN loss defines a TGF-β-induced tubule phenotype of failed differentiation and JNK signaling during renal fibrosis

Cited by 102 publications

References 48 publications

Increased expression of p21WAF1/CIP1 in kidney proximal tubules mediates fibrosis

Increased expression of p21WAF1/CIP1 in kidney proximal tubules mediates fibrosis

Proximal tubule PPARα attenuates renal fibrosis and inflammation caused by unilateral ureteral obstruction

Cellular and Molecular Mechanisms of AKI

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Product

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Increased expression of p21^WAF1/CIP1 in kidney proximal tubules mediates fibrosis

Increased expression of p21^WAF1/CIP1 in kidney proximal tubules mediates fibrosis