Endoplasmic reticulum stress participates in the pathophysiology of mercury-caused acute kidney injury

Acute exposure to mercury chloride (HgCl 2 ) causes acute kidney injury (AKI). Some metals interfere with protein folding, leading to endoplasmic reticulum stress (ERS), and the activation of cell death mechanisms, but in the case of mercury, there is no knowledge about whether the ERS mediates tubu...

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Bibliographic Details
Published in:Renal failure 2019-01, Vol.41 (1), p.1001-1010
Main Authors: Rojas-Franco, Plácido, Franco-Colín, Margarita, Torres-Manzo, Alejandra Paola, Blas-Valdivia, Vanessa, Thompson-Bonilla, María del Rocio, Kandir, Sinan, Cano-Europa, Edgar
Format: Article
Language:English
Subjects:
acute kidney injury
Acute Kidney Injury - chemically induced
Acute Kidney Injury - pathology
Animals
Antioxidants
Apoptosis
Bioaccumulation
Caspase-12
Caspase-3
Cell activation
Cell Death
Endoplasmic reticulum
Endoplasmic Reticulum Stress
Glutathione
Heavy metals
Kidney - pathology
Kidneys
Laboratory Study
Male
Mercuric chloride
mercury chloride
Mercury nephrotoxicity
Mercury Poisoning - etiology
Mercury Poisoning - pathology
Mice
Oxidative Stress
Protein folding
Renal function
unfolded protein response
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Summary:Acute exposure to mercury chloride (HgCl 2 ) causes acute kidney injury (AKI). Some metals interfere with protein folding, leading to endoplasmic reticulum stress (ERS), and the activation of cell death mechanisms, but in the case of mercury, there is no knowledge about whether the ERS mediates tubular damage. This study aimed to determinate if HgCl 2 causes an AKI course with temporary activation of ERS and if this mechanism is involved in kidney cell death. Male mice were intoxicated with 5 mg/kg HgCl 2 and sacrificed after 24, 48, 72, and 96 h of mercury administration. The kidneys of euthanized mice were used to assess the renal function, oxidative stress, redox environment, antioxidant enzymatic system, cell death, and reticulum stress markers (PERK, ATF-6, and IRE1α pathways). The results indicate temporary-dependent renal dysfunction, oxidative stress, and an increase of glutathione-dependent enzymes involved in the bioaccumulation process of mercury, as well as the enhancement of caspase 3 activity along with IRE1a, GADD-153, and caspase 12 expressions. Mercury activates the PERK/eIF2α branch during the first 48 h. Meanwhile, the activation of PERK/ATF-4 branch allowed for ATF-4, ATF-6, and IRE1α pathways to enhance GADD-153. It led to the activation of caspases 12 and 3, which mediated the deaths of the tubular and glomerular cells. This study revealed temporary-dependent ERS present during AKI caused by HgCl 2 , as well as how it plays a pivotal role in kidney cell damage.
ISSN:0886-022X
1525-6049
DOI:10.1080/0886022X.2019.1686019