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Trehalose Activates Hepatic and Myocardial Autophagy and Has Anti-Inflammatory Effects in db/db Diabetic Mice

Db/db mice (carrying a mutation in the gene encoding leptin receptor) show autophagy suppression. Our aim was to evaluate the effect of autophagy inducer trehalose on liver and heart autophagy in db/db mice and to study inflammation dysregulation and the suitability of chitinases’ expression levels...

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Autores principales: Korolenko, Tatiana A., Ovsyukova, Marina V., Bgatova, Nataliya P., Ivanov, Igor D., Makarova, Svetlana I., Vavilin, Valentin A., Popov, Alexey V., Yuzhik, Ekaterina I., Koldysheva, Elena V., Korolenko, Erik C., Zavjalov, Evgeny L., Amstislavskaya, Tamara G.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8950581/
https://www.ncbi.nlm.nih.gov/pubmed/35330193
http://dx.doi.org/10.3390/life12030442
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author Korolenko, Tatiana A.
Ovsyukova, Marina V.
Bgatova, Nataliya P.
Ivanov, Igor D.
Makarova, Svetlana I.
Vavilin, Valentin A.
Popov, Alexey V.
Yuzhik, Ekaterina I.
Koldysheva, Elena V.
Korolenko, Erik C.
Zavjalov, Evgeny L.
Amstislavskaya, Tamara G.
author_facet Korolenko, Tatiana A.
Ovsyukova, Marina V.
Bgatova, Nataliya P.
Ivanov, Igor D.
Makarova, Svetlana I.
Vavilin, Valentin A.
Popov, Alexey V.
Yuzhik, Ekaterina I.
Koldysheva, Elena V.
Korolenko, Erik C.
Zavjalov, Evgeny L.
Amstislavskaya, Tamara G.
author_sort Korolenko, Tatiana A.
collection PubMed
description Db/db mice (carrying a mutation in the gene encoding leptin receptor) show autophagy suppression. Our aim was to evaluate the effect of autophagy inducer trehalose on liver and heart autophagy in db/db mice and to study inflammation dysregulation and the suitability of chitinases’ expression levels as diabetes markers. Thirty-eight male db/db mice and C57/BL mice (control) were used. The db/db model manifested inflammation symptoms: overexpression of TNF-α in the spleen and underexpression of IL-10 in the liver and spleen (cytokine imbalance). Simultaneously, we revealed decreased expression of chitotriosidase (CHIT1) and acid mammalian chitinase (CHIA) in the liver of db/db mice. CHIA expression in db/db mice is significantly lower only in the spleen. Trehalose treatment significantly reduced blood glucose concentration and glycated hemoglobin. Treatment of db/db mice by trehalose was followed by increased autophagy induction in the heart and liver (increased autolysosomes volume density studied by morphometric electron-microscopic method). Trehalose exerted beneficial cardiac effects possibly via increased lipophagy (uptake of lipid droplets). The autophagy activation by trehalose had several positive effects on the heart and liver of db/db mice; therefore, lipophagy activation seems to be a promising therapy for diabetes.
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spelling pubmed-89505812022-03-26 Trehalose Activates Hepatic and Myocardial Autophagy and Has Anti-Inflammatory Effects in db/db Diabetic Mice Korolenko, Tatiana A. Ovsyukova, Marina V. Bgatova, Nataliya P. Ivanov, Igor D. Makarova, Svetlana I. Vavilin, Valentin A. Popov, Alexey V. Yuzhik, Ekaterina I. Koldysheva, Elena V. Korolenko, Erik C. Zavjalov, Evgeny L. Amstislavskaya, Tamara G. Life (Basel) Article Db/db mice (carrying a mutation in the gene encoding leptin receptor) show autophagy suppression. Our aim was to evaluate the effect of autophagy inducer trehalose on liver and heart autophagy in db/db mice and to study inflammation dysregulation and the suitability of chitinases’ expression levels as diabetes markers. Thirty-eight male db/db mice and C57/BL mice (control) were used. The db/db model manifested inflammation symptoms: overexpression of TNF-α in the spleen and underexpression of IL-10 in the liver and spleen (cytokine imbalance). Simultaneously, we revealed decreased expression of chitotriosidase (CHIT1) and acid mammalian chitinase (CHIA) in the liver of db/db mice. CHIA expression in db/db mice is significantly lower only in the spleen. Trehalose treatment significantly reduced blood glucose concentration and glycated hemoglobin. Treatment of db/db mice by trehalose was followed by increased autophagy induction in the heart and liver (increased autolysosomes volume density studied by morphometric electron-microscopic method). Trehalose exerted beneficial cardiac effects possibly via increased lipophagy (uptake of lipid droplets). The autophagy activation by trehalose had several positive effects on the heart and liver of db/db mice; therefore, lipophagy activation seems to be a promising therapy for diabetes. MDPI 2022-03-17 /pmc/articles/PMC8950581/ /pubmed/35330193 http://dx.doi.org/10.3390/life12030442 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Korolenko, Tatiana A.
Ovsyukova, Marina V.
Bgatova, Nataliya P.
Ivanov, Igor D.
Makarova, Svetlana I.
Vavilin, Valentin A.
Popov, Alexey V.
Yuzhik, Ekaterina I.
Koldysheva, Elena V.
Korolenko, Erik C.
Zavjalov, Evgeny L.
Amstislavskaya, Tamara G.
Trehalose Activates Hepatic and Myocardial Autophagy and Has Anti-Inflammatory Effects in db/db Diabetic Mice
title Trehalose Activates Hepatic and Myocardial Autophagy and Has Anti-Inflammatory Effects in db/db Diabetic Mice
title_full Trehalose Activates Hepatic and Myocardial Autophagy and Has Anti-Inflammatory Effects in db/db Diabetic Mice
title_fullStr Trehalose Activates Hepatic and Myocardial Autophagy and Has Anti-Inflammatory Effects in db/db Diabetic Mice
title_full_unstemmed Trehalose Activates Hepatic and Myocardial Autophagy and Has Anti-Inflammatory Effects in db/db Diabetic Mice
title_short Trehalose Activates Hepatic and Myocardial Autophagy and Has Anti-Inflammatory Effects in db/db Diabetic Mice
title_sort trehalose activates hepatic and myocardial autophagy and has anti-inflammatory effects in db/db diabetic mice
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8950581/
https://www.ncbi.nlm.nih.gov/pubmed/35330193
http://dx.doi.org/10.3390/life12030442
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