Continuous overexpression of thioredoxin 1 enhances cancer development and does not extend maximum lifespan in male C57BL/6 mice

Flores, Lisa C.; Roman, Madeline G.; Cunningham, Geneva M.; Cheng, Christie; Dube, Sara; Allen, Colton; Remmen, Holly Van; Hubbard, Gene B.; Saunders, Thomas L.; Ikeno, Yuji

doi:10.1080/20010001.2018.1533754

Cited by 17 publications

(33 citation statements)

References 45 publications

(71 reference statements)

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“…The cross-sectional pathological analyses of 23 Tg(TXN) +/0 and 19 WT mice (22-24 months old) showed that the major disease in these mice was neoplastic disease. The tumors observed were lymphoma, hemangioma/ hemangiosarcoma in the liver and spleen, pulmonary ad-enocarcinoma, hepatocellular carcinoma, and adenoma in the thyroid gland, and the most prevalent tumor was lymphoma, which is consistent with the pathology data from C57BL/6 mice and mice overexpressing Trx1 [11,13]. First, we compared the number of different types of tumors (tumor burden) for each mouse in both Tg(TXN2) +/0 and WT groups because aging mice may have several different types of tumors.…”

Section: Cross-sectional Pathologysupporting

confidence: 87%

“…The severity of lymphoma was slightly higher in Tg(TXN2) +/0 mice compared to WT mice, although the difference was not statistically significant. These pathological observations indicate that overexpression of Trx2 in mitochondria may play a similar role in the development and growth of lymphoma as the overexpression of Trx1 [11,13], i.e., accelerate the growth and development of lymphoma as they age. Subsequently, we measured several signaling pathways (i.e., mTOR, NFκB, and c-Jun/Fos) because substantial evidence shows that these pathways play important roles in cancer development and lifespan and can also be attenuated by Trx.…”

Section: Discussionmentioning

confidence: 79%

“…In humans, Trx1 and Trx2 have been identified in different compartments of the cell, i.e., Trx1 in cytosol [8] and Trx2 in mitochondria [9]. To test the pathophysiological roles of Trx1 during aging, two transgenic mice overexpressing Trx1 were generated using: 1) a transgene containing the human thioredoxin cDNA fused to the β-actin promoter [Tg(act-TXN) +/0 mice] [10] and 2) clones of the human TXN gene containing endogenous promoters [Tg(TXN) +/0 ] [11]. The initial aging study demonstrated that Tg(act-TXN) +/0 mice had an increased lifespan compared to their WT littermates [10,12].…”

Section: Introductionmentioning

confidence: 99%

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

Roman

Flores

Cunningham

et al. 2020

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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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Section: Cross-sectional Pathologysupporting

confidence: 87%

Section: Discussionmentioning

confidence: 79%

Section: Introductionmentioning

confidence: 99%

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

Roman

Flores

Cunningham

et al. 2020

APT

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“…The study showed that the survival curve of Tg(TXN) +/0 mice was not significantly different from WT mice. Although the early part of lifespan (75% survival) showed a 6.3% extension compared to WT mice, no significant life-extending effect was observed over the lifespan [16]. Therefore, our survival data obtained from Tg(TXN) +/0 mice indicate that continuous Trx1 overexpression in mice had some benefits only in the early part of life.…”

Section: Transgenic Mice/rats Overexpressing Thioredoxin 1 (Cytosol)mentioning

confidence: 64%

“…Next, we generated a new line of Trx1 transgenic mice (Tg(TXN) +/0 ) in order to determine whether continuous overexpression of Trx1 throughout life could extend maximum lifespan. These mice were generated using a fragment of the human genome containing the TXN gene [16]. Tg(TXN) +/0 mice showed significantly higher (approximately 20% to 40%) levels of Trx1 in the tissues than WT mice.…”

Section: Transgenic Mice/rats Overexpressing Thioredoxin 1 (Cytosol)mentioning

confidence: 99%

Thioredoxin and aging: What have we learned from the survival studies?

Roman¹,

Flores²,

Cunningham³

et al. 2020

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Our laboratory has conducted the first systematic survival studies to examine the biological effects of the antioxidant protein thioredoxin (Trx) on aging and age-related pathology. Our studies with C57BL/6 mice overexpressing Trx1 [Tg(act-TRX1) +/0 and Tg(TXN) +/0 ] demonstrated a slight extension in early lifespan compared to wild-type (WT) mice; however, no significant effects were observed in the later part of life. Overexpression of Trx2 in male C57BL/6 mice [Tg(TXN2) +/0 ] demonstrated a slightly extended lifespan compared to WT mice. The pathology results from two lines of Trx1 transgenic mice showed a slightly higher incidence of age-related neoplastic diseases compared to WT mice, and a slight increase in the severity of lymphoma, a major neoplastic disease, was observed in Trx2 transgenic mice. Together these studies indicate that Trx overexpression in one compartment of the cell (cytosol or mitochondria alone) has marginal beneficial effects on lifespan. On the other hand, down-regulation of Trx in either the cytosol (Trx1KO) or mitochondria (Trx2KO) showed no significant changes in lifespan compared to WT mice, despite several changes in pathophysiology of these knockout mice. When we examined the synergetic effects of overexpressing Trx1 and Trx2, TXNTg x TXN2Tg mice showed a significantly shorter lifespan with accelerated cancer development compared to WT mice. These results suggest that synergetic effects of Trx overexpression in both the cytosol and mitochondria on aging are deleterious and the development of age-related cancer is accelerated. On the other hand, we have recently found that down-regulation of Trx in both the cytosol and mitochondria in Trx1KO x Trx2KO mice has beneficial effects on aging. The results generated from our lab along with our ongoing study using Trx1KO x Trx2KO mice could elucidate the key pathways (i.e., apoptosis and autophagy) that prevent accumulation of damaged cells and genomic instability leading to reduced cancer formation.

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Metabolic reprogramming: a bridge between aging and tumorigenesis

2022

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Aging is the most robust risk factor for cancer development, with more than 60% of cancers occurring in those aged 60 and above. However, how aging and tumorigenesis are intertwined is poorly understood and a matter of significant debate. Metabolic changes are hallmarks of both aging and tumorigenesis. The deleterious consequences of aging include dysfunctional cellular processes, the build-up of metabolic byproducts and waste molecules in circulation and within tissues, and stiffer connective tissues that impede blood flow and oxygenation. Collectively, these age-driven changes lead to metabolic reprogramming in different cell types of a given tissue that significantly affects their cellular functions. Here, we put forward the idea that metabolic changes that happen during aging help create a favorable environment for tumorigenesis. We review parallels in metabolic changes that happen during aging and how these changes function both as adaptive mechanisms that enable the development of malignant phenotypes in a cell-autonomous manner and as mechanisms that suppress immune surveillance, collectively creating the perfect environment for cancers to thrive. Hence, antiaging therapeutic strategies that target the metabolic reprogramming that occurs as we age might provide new opportunities to prevent cancer initiation and/or improve responses to standard-of-care anticancer therapies.

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Continuous overexpression of thioredoxin 1 enhances cancer development and does not extend maximum lifespan in male C57BL/6 mice

Cited by 17 publications

References 45 publications

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

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

Thioredoxin and aging: What have we learned from the survival studies?

Metabolic reprogramming: a bridge between aging and tumorigenesis

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