Lithium ameliorates tubule-interstitial injury through activation of the mTORC2/protein kinase B pathway.

Lithium ameliorates tubule-interstitial injury through activation of the mTORC2/protein kinase B pathway.

Tubule-interstitial injury (TII) is a critical step in the progression of renal disease. It has been proposed that changes in proximal tubule (PT) albumin endocytosis plays an important role in the development of TII. Some reports have shown protective effects of lithium on kidney injury animal mode...

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Main Authors: Douglas E Teixeira, Diogo B Peruchetti, Leandro S Silva, Rodrigo P Silva-Aguiar, Morgana B Oquendo, João Luiz Silva-Filho, Christina M Takiya, José Henrique Leal-Cardoso, Ana Acacia S Pinheiro, Celso Caruso-Neves
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2019-01-01
Series:PLoS ONE
Online Access:https://doi.org/10.1371/journal.pone.0215871
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spelling doaj-8e0eea98ae974579919e21fa8ce844eb2021-03-03T20:43:41ZengPublic Library of Science (PLoS)PLoS ONE1932-62032019-01-01144e021587110.1371/journal.pone.0215871Lithium ameliorates tubule-interstitial injury through activation of the mTORC2/protein kinase B pathway.Douglas E TeixeiraDiogo B PeruchettiLeandro S SilvaRodrigo P Silva-AguiarMorgana B OquendoJoão Luiz Silva-FilhoChristina M TakiyaJosé Henrique Leal-CardosoAna Acacia S PinheiroCelso Caruso-NevesTubule-interstitial injury (TII) is a critical step in the progression of renal disease. It has been proposed that changes in proximal tubule (PT) albumin endocytosis plays an important role in the development of TII. Some reports have shown protective effects of lithium on kidney injury animal models that was correlated to proteinuria. We tested the hypothesis that lithium treatment ameliorates the development of TII due to changes in albumin endocytosis. Two experimental models were used: (1) TII induced by albumin overload in an animal model; (2) LLC-PK1 cells, a PT cell line. Lithium treatment ameliorates TII induced by albumin overload measured by (1) proteinuria; (2) collagen deposition; (3) area of tubule-interstitial space, and (4) macrophage infiltration. Lithium treatment increased mTORC2 activity leading to the phosphorylation of protein kinase B (PKB) at Ser473 and its activation. This mechanism enhanced albumin endocytosis in PT cells, which decreased the proteinuria observed in TII induced by albumin overload. This effect did not involve changes in the expression of megalin, a PT albumin receptor. In addition, activation of this pathway decreased apoptosis in LLC-PK1 cells, a PT cell line, induced by higher albumin concentration, similar to that found in pathophysiologic conditions. Our results indicate that the protective role of lithium treatment on TII induced by albumin overload involves an increase in PT albumin endocytosis due to activation of the mTORC2/PKB pathway. These results open new possibilities in understanding the effects of lithium on the progression of renal disease.https://doi.org/10.1371/journal.pone.0215871
collection DOAJ
language English
format Article
sources DOAJ
author Douglas E Teixeira
Diogo B Peruchetti
Leandro S Silva
Rodrigo P Silva-Aguiar
Morgana B Oquendo
João Luiz Silva-Filho
Christina M Takiya
José Henrique Leal-Cardoso
Ana Acacia S Pinheiro
Celso Caruso-Neves
spellingShingle Douglas E Teixeira
Diogo B Peruchetti
Leandro S Silva
Rodrigo P Silva-Aguiar
Morgana B Oquendo
João Luiz Silva-Filho
Christina M Takiya
José Henrique Leal-Cardoso
Ana Acacia S Pinheiro
Celso Caruso-Neves
Lithium ameliorates tubule-interstitial injury through activation of the mTORC2/protein kinase B pathway.
PLoS ONE
author_facet Douglas E Teixeira
Diogo B Peruchetti
Leandro S Silva
Rodrigo P Silva-Aguiar
Morgana B Oquendo
João Luiz Silva-Filho
Christina M Takiya
José Henrique Leal-Cardoso
Ana Acacia S Pinheiro
Celso Caruso-Neves
author_sort Douglas E Teixeira
title Lithium ameliorates tubule-interstitial injury through activation of the mTORC2/protein kinase B pathway.
title_short Lithium ameliorates tubule-interstitial injury through activation of the mTORC2/protein kinase B pathway.
title_full Lithium ameliorates tubule-interstitial injury through activation of the mTORC2/protein kinase B pathway.
title_fullStr Lithium ameliorates tubule-interstitial injury through activation of the mTORC2/protein kinase B pathway.
title_full_unstemmed Lithium ameliorates tubule-interstitial injury through activation of the mTORC2/protein kinase B pathway.
title_sort lithium ameliorates tubule-interstitial injury through activation of the mtorc2/protein kinase b pathway.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2019-01-01
description Tubule-interstitial injury (TII) is a critical step in the progression of renal disease. It has been proposed that changes in proximal tubule (PT) albumin endocytosis plays an important role in the development of TII. Some reports have shown protective effects of lithium on kidney injury animal models that was correlated to proteinuria. We tested the hypothesis that lithium treatment ameliorates the development of TII due to changes in albumin endocytosis. Two experimental models were used: (1) TII induced by albumin overload in an animal model; (2) LLC-PK1 cells, a PT cell line. Lithium treatment ameliorates TII induced by albumin overload measured by (1) proteinuria; (2) collagen deposition; (3) area of tubule-interstitial space, and (4) macrophage infiltration. Lithium treatment increased mTORC2 activity leading to the phosphorylation of protein kinase B (PKB) at Ser473 and its activation. This mechanism enhanced albumin endocytosis in PT cells, which decreased the proteinuria observed in TII induced by albumin overload. This effect did not involve changes in the expression of megalin, a PT albumin receptor. In addition, activation of this pathway decreased apoptosis in LLC-PK1 cells, a PT cell line, induced by higher albumin concentration, similar to that found in pathophysiologic conditions. Our results indicate that the protective role of lithium treatment on TII induced by albumin overload involves an increase in PT albumin endocytosis due to activation of the mTORC2/PKB pathway. These results open new possibilities in understanding the effects of lithium on the progression of renal disease.
url https://doi.org/10.1371/journal.pone.0215871
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