Thioredoxin overexpression in mitochondria showed minimum effects on aging and age-related diseases in male C57BL/6 mice

OBJECTIVE: In this study, the effects of overexpression of thioredoxin 2 (Trx2) on aging and age-related diseases were examined using Trx2 transgenic mice [Tg(TXN2](+/0)]. Because our previous studies demonstrated that thioredoxin (Trx) overexpression in the cytosol (Trx1) did not extend maximum lif...

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Autores principales: Roman, Madeline G., Flores, Lisa C., Cunningham, Geneva M., Cheng, Christie, Dube, Sara, Allen, Colton, Van Remmen, Holly, Bai, Yidong, Hubbard, Gene B., Saunders, Thomas L., Ikeno, Yuji
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2020
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8963792/
https://www.ncbi.nlm.nih.gov/pubmed/35356005
http://dx.doi.org/10.31491/apt.2020.03.009
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author Roman, Madeline G.
Flores, Lisa C.
Cunningham, Geneva M.
Cheng, Christie
Dube, Sara
Allen, Colton
Van Remmen, Holly
Bai, Yidong
Hubbard, Gene B.
Saunders, Thomas L.
Ikeno, Yuji
author_facet Roman, Madeline G.
Flores, Lisa C.
Cunningham, Geneva M.
Cheng, Christie
Dube, Sara
Allen, Colton
Van Remmen, Holly
Bai, Yidong
Hubbard, Gene B.
Saunders, Thomas L.
Ikeno, Yuji
author_sort Roman, Madeline G.
collection PubMed
description OBJECTIVE: In this study, the effects of overexpression of thioredoxin 2 (Trx2) on aging and age-related diseases were examined using Trx2 transgenic mice [Tg(TXN2](+/0)]. Because our previous studies demonstrated that thioredoxin (Trx) overexpression in the cytosol (Trx1) did not extend maximum lifespan, this study was conducted to test if increased Trx2 expression in mitochondria shows beneficial effects on aging and age-related pathology. METHODS: Trx2 transgenic mice were generated using a fragment of the human genome containing the TXN2 gene. Effects of Trx2 overexpression on survival, age-related pathology, oxidative stress, and redox-sensitive signaling pathways were examined in male Tg(TXN2)(+/0) mice. RESULTS: Trx2 levels were significantly higher (approximately 1.6- to 5-fold) in all of the tissues we examined in Tg(TXN2)(+/0) mice compared to wild-type (WT) littermates, and the expression levels were maintained during aging (up to 22-24 months old). Trx2 overexpression did not alter the levels of Trx1, glutaredoxin, glutathione, or other major antioxidant enzymes. Overexpression of Trx2 was associated with reduced reactive oxygen species (ROS) production from mitochondria and lower isoprostane levels compared to WT mice. When we conducted the survival study, male Tg(TXN2)(+/0) mice showed a slight extension (approximately 8-9%] of mean, median, and 10th percentile lifespans; however, the survival curve was not significantly different from WT mice. Cross-sectional pathological analysis (22-24 months old) showed that Tg(TXN2)(+/0) mice had a slightly higher severity of lymphoma; however, tumor burden, disease burden, and severity of glomerulonephritis and inflammation were similar to WT mice. Trx2 overexpression was also associated with higher c-Jun and c-Fos levels; however, mTOR activity and levels of NFκB p65 and p50 were similar to WT littermates. CONCLUSIONS: Our findings suggest that the increased levels of Trx2 in mitochondria over the lifespan in Tg(TXN2)(+/0) mice showed a slight life-extending effect, reduced ROS production from mitochondria and oxidative damage to lipids, but showed no significant effects on aging and age-related diseases.
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spelling pubmed-89637922022-03-29 Thioredoxin overexpression in mitochondria showed minimum effects on aging and age-related diseases in male C57BL/6 mice Roman, Madeline G. Flores, Lisa C. Cunningham, Geneva M. Cheng, Christie Dube, Sara Allen, Colton Van Remmen, Holly Bai, Yidong Hubbard, Gene B. Saunders, Thomas L. Ikeno, Yuji Aging Pathobiol Ther Article OBJECTIVE: In this study, the effects of overexpression of thioredoxin 2 (Trx2) on aging and age-related diseases were examined using Trx2 transgenic mice [Tg(TXN2](+/0)]. Because our previous studies demonstrated that thioredoxin (Trx) overexpression in the cytosol (Trx1) did not extend maximum lifespan, this study was conducted to test if increased Trx2 expression in mitochondria shows beneficial effects on aging and age-related pathology. METHODS: Trx2 transgenic mice were generated using a fragment of the human genome containing the TXN2 gene. Effects of Trx2 overexpression on survival, age-related pathology, oxidative stress, and redox-sensitive signaling pathways were examined in male Tg(TXN2)(+/0) mice. RESULTS: Trx2 levels were significantly higher (approximately 1.6- to 5-fold) in all of the tissues we examined in Tg(TXN2)(+/0) mice compared to wild-type (WT) littermates, and the expression levels were maintained during aging (up to 22-24 months old). Trx2 overexpression did not alter the levels of Trx1, glutaredoxin, glutathione, or other major antioxidant enzymes. Overexpression of Trx2 was associated with reduced reactive oxygen species (ROS) production from mitochondria and lower isoprostane levels compared to WT mice. When we conducted the survival study, male Tg(TXN2)(+/0) mice showed a slight extension (approximately 8-9%] of mean, median, and 10th percentile lifespans; however, the survival curve was not significantly different from WT mice. Cross-sectional pathological analysis (22-24 months old) showed that Tg(TXN2)(+/0) mice had a slightly higher severity of lymphoma; however, tumor burden, disease burden, and severity of glomerulonephritis and inflammation were similar to WT mice. Trx2 overexpression was also associated with higher c-Jun and c-Fos levels; however, mTOR activity and levels of NFκB p65 and p50 were similar to WT littermates. CONCLUSIONS: Our findings suggest that the increased levels of Trx2 in mitochondria over the lifespan in Tg(TXN2)(+/0) mice showed a slight life-extending effect, reduced ROS production from mitochondria and oxidative damage to lipids, but showed no significant effects on aging and age-related diseases. 2020 2020-03-27 /pmc/articles/PMC8963792/ /pubmed/35356005 http://dx.doi.org/10.31491/apt.2020.03.009 Text en https://creativecommons.org/licenses/by-sa/4.0/ Creative Commons 4.0 (https://creativecommons.org/licenses/by-sa/4.0/)
spellingShingle Article
Roman, Madeline G.
Flores, Lisa C.
Cunningham, Geneva M.
Cheng, Christie
Dube, Sara
Allen, Colton
Van Remmen, Holly
Bai, Yidong
Hubbard, Gene B.
Saunders, Thomas L.
Ikeno, Yuji
Thioredoxin overexpression in mitochondria showed minimum effects on aging and age-related diseases in male C57BL/6 mice
title Thioredoxin overexpression in mitochondria showed minimum effects on aging and age-related diseases in male C57BL/6 mice
title_full Thioredoxin overexpression in mitochondria showed minimum effects on aging and age-related diseases in male C57BL/6 mice
title_fullStr Thioredoxin overexpression in mitochondria showed minimum effects on aging and age-related diseases in male C57BL/6 mice
title_full_unstemmed Thioredoxin overexpression in mitochondria showed minimum effects on aging and age-related diseases in male C57BL/6 mice
title_short Thioredoxin overexpression in mitochondria showed minimum effects on aging and age-related diseases in male C57BL/6 mice
title_sort thioredoxin overexpression in mitochondria showed minimum effects on aging and age-related diseases in male c57bl/6 mice
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8963792/
https://www.ncbi.nlm.nih.gov/pubmed/35356005
http://dx.doi.org/10.31491/apt.2020.03.009
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