Thyroid hormone preconditioning: Protection against ischemia-reperfusion liver injury in the rat

Fernández, Virgínia; Castillo, Iván; Tapia, Gladys; Romanque, Pamela; Uribe-Echevarría, Sebastián; Uribe, Mario; Cartier-Ugarte, Denise; Santander, Gonzalo; Vial, M; Videla, Luis A.

doi:10.1002/hep.21476

Cited by 74 publications

(96 citation statements)

References 40 publications

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“…The hormetic responses involved in thyroid hormone-induced liver preconditioning against IR injury (78) are also observed in the heart (88,89), with a pattern of protection closely resembling that of ischemic preconditioning (90), and constitute a preconditioning strategy that have clinical potential. This is an important issue considering that pharmacological and other liver preconditioning maneuvers have not been transferred to clinical application, with the exception of ischemic preconditioning (91).…”

Section: Discussionmentioning

confidence: 99%

Hormetic responses of thyroid hormone calorigenesis in the liver: Association with oxidative stress

Videla

2010

IUBMB Life

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SummaryThyroid hormone (L-3,3 0 ,5-triiodothyronine, T 3 ) exerts calorigenic effects by accelerating mitochondrial O 2 consumption through transcriptional activation of respiratory genes, with consequent increased reactive oxygen species (ROS) production. In the liver, ROS generation occurs at different sites of hepatocytes and in the respiratory burst of Kupffer cells, triggering the activation of the transcription factors nuclear factor-jB, signal transducer and activator of transcription 3, and activating protein 1. Under these conditions, the redox upregulation of Kupffer cell-dependent expression of cytokines [tumor necrosis factor-a, interleukin (IL)-1, and IL-6] is achieved, which upon interaction with specific receptors in hepatocytes trigger the expression of antioxidant enzymes (manganese superoxide dismutase, inducible nitric oxide synthase), antiapoptotic proteins (Bcl-2), and acute-phase proteins (haptoglobin, b-fibrinogen). These responses and the promotion of hepatocyte and Kupffer cell proliferation observed represent hormetic effects re-establishing redox homeostasis, promoting cell survival, and protecting the liver against ischemia-reperfusion (IR) injury. It is proposed that hormesis underlying T 3 action may constitute a novel preconditioning strategy for IR injury during liver surgery in man or in liver transplantation using reduced-size grafts from living donors, considering that (i) with the exception of the controversial ischemic preconditioning, all other studied strategies have failed to reach the clinical setting and (ii) T 3 is a well-tolerated therapeutic agent that either lacks major adverse effects or has minimal and controlled side effects. IUBMBIUBMB Life, 62(6): [460][461][462][463][464][465][466] 2010

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Section: Discussionmentioning

confidence: 99%

Hormetic responses of thyroid hormone calorigenesis in the liver: Association with oxidative stress

Videla

2010

IUBMB Life

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“…This ultimately increases liver iNOS expression and activity 232:2 together with other markers of oxidative stress including decreased liver glutathione content (an important antioxidant) and higher protein oxidation (Fig. 2B) (Tapia et al 1997, 2006, Valencia et al 2004, Fernandez et al 2005, 2007a. Conversely, another study found that T 3 inhibited STAT3 signalling in macrophages after LPS or IL-6 stimulation and had no effect on TNFα induction and NFκB activation in vitro (Contreras-Jurado et al 2016).…”

Section: Thyroid Hormone Metabolism In Tissue-resident Macrophagesmentioning

confidence: 96%

“…Several studies by the same group have analysed the effect of TH administration on rat liver and the role of Kupffer cells in this process. T 3 administration induces oxidative stress in the liver (Tapia et al 1997, 2006, 2010, Valencia et al 2004, Fernandez et al 2005, 2007a,b, 2008. This is thought to be mediated via Kupffer cells, which demonstrate hyperplasia, increased phagocytic capacity, increased ROS generation and tumour necrosis factor α (TNFα) production in response to T 3 administration in vivo (Fig.…”

Section: Thyroid Hormone Metabolism In Tissue-resident Macrophagesmentioning

confidence: 99%

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Thyroid hormone metabolism in innate immune cells

Spek

Fliers

Boelen

2017

Journal of Endocrinology

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Thyroid hormone (TH) metabolism and thyroid status have been linked to various aspects of the immune response. There is extensive literature available on the effects of thyroid hormone on innate immune cells. However, only recently have authors begun to study the mechanisms behind these effects and the role of intracellular TH metabolism in innate immune cell function during inflammation. This review provides an overview of the molecular machinery of intracellular TH metabolism present in neutrophils, macrophages and dendritic cells and the role and effects of intracellular TH metabolism in these cells. Circulating TH levels have a profound effect on neutrophil, macrophage and dendritic cell function. In general, increased TH levels result in an amplification of the pro-inflammatory response of these cells. The mechanisms behind these effects include both genomic and non-genomic effects of TH. Besides a pro-inflammatory effect induced by extracellular TH, the cellular response to pro-inflammatory stimuli appears to be dependent on functional intracellular TH metabolism. This is illustrated by the fact that the deiodinase enzymes and in some cell types also thyroid hormone receptors appear to be crucial for adequate innate immune cell function. This overview of the literature suggests that TH metabolism plays an important role in the host defence against infection through the modulation of innate immune cell function.

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“…However, prolonged stress may cause an elevation in cortisol concentrations as the adrenal glands respond to the stress. The high cortisol levels inhibit the conversion of T4 to T3 [41]. On the other hand, loss of thyroid-binding protein in urine under the effects of oxidative stress could be another cause of decrease in serum T3 and T4 levels.…”

Section: Discussionmentioning

confidence: 99%

Changes in the hemodynamic and thyroid functions of rats treated by opium

Mustafa¹,

Othman²,

Othman³

et al. 2017

DJPS

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Opioids are perhaps the most efficacious analgesic agents influencing a large number of body functions. The objective of this study is to observe changes in hemodynamic, electrolytes, and kidney and thyroid functions of opium treatment in rats. Thirty male rats were randomly distributed into three groups. Group 1 regarded as control, while in group 2 and 3, the animals were daily injected intraperitoneally with opium for seven successive days. Intraperitoneal opium injection caused a dose-deponent increase in serum calcium (Ca +2 )and phosphate (PO4 -) levels, whereas the nitric oxide (NO), triiodothyronine (T3) and thyroxine (T4) levels were significantly decreased in both doses. The significant decrease in serum (NO )level and increase serum (Ca 2+ ) and (PO4 -) levels resulted in significant elevation of systolic blood pressure (SBP) accompanied by elevation of serum bilirubin and urea. Our finding suggests that opium causes hypertension, kidney and thyroid function abnormalities mostly in concentration dependent manner.

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Thyroid hormone preconditioning: Protection against ischemia-reperfusion liver injury in the rat

Cited by 74 publications

References 40 publications

Hormetic responses of thyroid hormone calorigenesis in the liver: Association with oxidative stress

Hormetic responses of thyroid hormone calorigenesis in the liver: Association with oxidative stress

Thyroid hormone metabolism in innate immune cells

Changes in the hemodynamic and thyroid functions of rats treated by opium

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