Tamoxifen and bone morphogenic protein-7 modulate fibrosis and inflammation in the peritoneal fibrosis model developed in uremic rats

Tamoxifen and bone morphogenic protein-7 modulate fibrosis and inflammation in the peritoneal fibrosis model developed in uremic rats

Abstract Background Peritoneal fibrosis (PF) represents a long-term complication of peritoneal dialysis (PD), affecting peritoneal membrane (PM) integrity and function. Understanding the mechanisms underlying PF development in an uremic environment aiming alternative therapeutic strategies for treat...

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Main Authors: Filipe M. O. Silva, Elerson C. Costalonga, Cleonice Silva, Ana C. O. Carreira, Samirah A. Gomes, Mari C. Sogayar, Camilla Fanelli, Irene L. Noronha
Format: Article
Language:English
Published: BMC 2019-08-01
Series:Molecular Medicine
Subjects:
Peritoneal fibrosis
Peritoneal inflammation
Tamoxifen
BMP7
TGF-ß
Smads
Online Access:http://link.springer.com/article/10.1186/s10020-019-0110-5
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spelling doaj-1d71076c97ce453c8267a45c5b4fee0e2020-11-25T03:43:32ZengBMCMolecular Medicine1076-15511528-36582019-08-0125111810.1186/s10020-019-0110-5Tamoxifen and bone morphogenic protein-7 modulate fibrosis and inflammation in the peritoneal fibrosis model developed in uremic ratsFilipe M. O. Silva0Elerson C. Costalonga1Cleonice Silva2Ana C. O. Carreira3Samirah A. Gomes4Mari C. Sogayar5Camilla Fanelli6Irene L. Noronha7Laboratory of Cellular, Genetic, and Molecular Nephrology, Renal Division, University of São Paulo Medical SchoolLaboratory of Cellular, Genetic, and Molecular Nephrology, Renal Division, University of São Paulo Medical SchoolLaboratory of Cellular, Genetic, and Molecular Nephrology, Renal Division, University of São Paulo Medical SchoolCell and Molecular Therapy Center, University of São Paulo Medical SchoolLaboratory of Cellular, Genetic, and Molecular Nephrology, Renal Division, University of São Paulo Medical SchoolCell and Molecular Therapy Center, University of São Paulo Medical SchoolLaboratory of Cellular, Genetic, and Molecular Nephrology, Renal Division, University of São Paulo Medical SchoolLaboratory of Cellular, Genetic, and Molecular Nephrology, Renal Division, University of São Paulo Medical SchoolAbstract Background Peritoneal fibrosis (PF) represents a long-term complication of peritoneal dialysis (PD), affecting peritoneal membrane (PM) integrity and function. Understanding the mechanisms underlying PF development in an uremic environment aiming alternative therapeutic strategies for treating this process is of great interest. The aim of this study was to analyze the effects of tamoxifen (TAM) and recombinant BMP7 (rBMP7) in an experimental model of PF developed in uremic rats. Methods To mimic the clinical situation of patients on long-term PD, a combo model, characterized by the combination of PF and CKD with severe uremia, was developed in Wistar rats. PF was induced by intraperitoneal (IP) injections of chlorhexidine gluconate (CG), and CKD was induced by an adenine-rich diet. Uremia was confirmed by severe hypertension, increased blood urea nitrogen (BUN> 120 mg/dL) and serum creatinine levels (> 2 mg/dL). Uremic rats with PF were treated with TAM (10 mg/Kg by gavage) or BMP7 (30 μg/Kg, IP). Animals were followed up for 30 days. Results CG administration in uremic rats induced a striking increase in PM thickness, neoangiogenesis, demonstrated by increased capillary density, and failure of ultrafiltration capacity. These morphological and functional changes were blocked by TAM or rBMP7 treatment. In parallel, TAM and rBMP7 significantly ameliorated the PM fibrotic response by reducing α-SMA, extracellular matrix proteins and TGF-ß expression. TAM or rBMP7 administration significantly inhibited peritoneal Smad3 expression in uremic rats with PF, prevented Smad3 phosphorylation, and induced a remarkable up-regulation of Smad7, an intracellular inhibitor of TGFβ/Smad signaling, contributing to a negative modulation of profibrotic genes. Both treatments were also effective in reducing local inflammation, possibly by upregulating IκB-α expression in the PM of uremic rats with PF. In vitro experiments using primary peritoneal fibroblasts activated by TGF-ß confirmed the capacity of TAM or rBMP7 in blocking inflammatory mediators, such as IL-1ß expression. Conclusions In conclusion, these findings indicate important roles of TGF-ß/Smad signaling in PF aggravated by uremia, providing data regarding potential therapeutic approaches with TAM or rBMP7 to block this process.http://link.springer.com/article/10.1186/s10020-019-0110-5Peritoneal fibrosisPeritoneal inflammationTamoxifenBMP7TGF-ßSmads
collection DOAJ
language English
format Article
sources DOAJ
author Filipe M. O. Silva
Elerson C. Costalonga
Cleonice Silva
Ana C. O. Carreira
Samirah A. Gomes
Mari C. Sogayar
Camilla Fanelli
Irene L. Noronha
spellingShingle Filipe M. O. Silva
Elerson C. Costalonga
Cleonice Silva
Ana C. O. Carreira
Samirah A. Gomes
Mari C. Sogayar
Camilla Fanelli
Irene L. Noronha
Tamoxifen and bone morphogenic protein-7 modulate fibrosis and inflammation in the peritoneal fibrosis model developed in uremic rats
Molecular Medicine
Peritoneal fibrosis
Peritoneal inflammation
Tamoxifen
BMP7
TGF-ß
Smads
author_facet Filipe M. O. Silva
Elerson C. Costalonga
Cleonice Silva
Ana C. O. Carreira
Samirah A. Gomes
Mari C. Sogayar
Camilla Fanelli
Irene L. Noronha
author_sort Filipe M. O. Silva
title Tamoxifen and bone morphogenic protein-7 modulate fibrosis and inflammation in the peritoneal fibrosis model developed in uremic rats
title_short Tamoxifen and bone morphogenic protein-7 modulate fibrosis and inflammation in the peritoneal fibrosis model developed in uremic rats
title_full Tamoxifen and bone morphogenic protein-7 modulate fibrosis and inflammation in the peritoneal fibrosis model developed in uremic rats
title_fullStr Tamoxifen and bone morphogenic protein-7 modulate fibrosis and inflammation in the peritoneal fibrosis model developed in uremic rats
title_full_unstemmed Tamoxifen and bone morphogenic protein-7 modulate fibrosis and inflammation in the peritoneal fibrosis model developed in uremic rats
title_sort tamoxifen and bone morphogenic protein-7 modulate fibrosis and inflammation in the peritoneal fibrosis model developed in uremic rats
publisher BMC
series Molecular Medicine
issn 1076-1551
1528-3658
publishDate 2019-08-01
description Abstract Background Peritoneal fibrosis (PF) represents a long-term complication of peritoneal dialysis (PD), affecting peritoneal membrane (PM) integrity and function. Understanding the mechanisms underlying PF development in an uremic environment aiming alternative therapeutic strategies for treating this process is of great interest. The aim of this study was to analyze the effects of tamoxifen (TAM) and recombinant BMP7 (rBMP7) in an experimental model of PF developed in uremic rats. Methods To mimic the clinical situation of patients on long-term PD, a combo model, characterized by the combination of PF and CKD with severe uremia, was developed in Wistar rats. PF was induced by intraperitoneal (IP) injections of chlorhexidine gluconate (CG), and CKD was induced by an adenine-rich diet. Uremia was confirmed by severe hypertension, increased blood urea nitrogen (BUN> 120 mg/dL) and serum creatinine levels (> 2 mg/dL). Uremic rats with PF were treated with TAM (10 mg/Kg by gavage) or BMP7 (30 μg/Kg, IP). Animals were followed up for 30 days. Results CG administration in uremic rats induced a striking increase in PM thickness, neoangiogenesis, demonstrated by increased capillary density, and failure of ultrafiltration capacity. These morphological and functional changes were blocked by TAM or rBMP7 treatment. In parallel, TAM and rBMP7 significantly ameliorated the PM fibrotic response by reducing α-SMA, extracellular matrix proteins and TGF-ß expression. TAM or rBMP7 administration significantly inhibited peritoneal Smad3 expression in uremic rats with PF, prevented Smad3 phosphorylation, and induced a remarkable up-regulation of Smad7, an intracellular inhibitor of TGFβ/Smad signaling, contributing to a negative modulation of profibrotic genes. Both treatments were also effective in reducing local inflammation, possibly by upregulating IκB-α expression in the PM of uremic rats with PF. In vitro experiments using primary peritoneal fibroblasts activated by TGF-ß confirmed the capacity of TAM or rBMP7 in blocking inflammatory mediators, such as IL-1ß expression. Conclusions In conclusion, these findings indicate important roles of TGF-ß/Smad signaling in PF aggravated by uremia, providing data regarding potential therapeutic approaches with TAM or rBMP7 to block this process.
topic Peritoneal fibrosis
Peritoneal inflammation
Tamoxifen
BMP7
TGF-ß
Smads
url http://link.springer.com/article/10.1186/s10020-019-0110-5
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