Proximal tubular transport of Metallothionein-Mercury complexes and protection against nephrotoxicity

[Display omitted] •Overexpression of metallothionein (MT) alters the corporal distribution of mercury (Hg)•Hg-MT complexes are taken up at the apical and basolateral membranes of proximal tubular cells.•Overexpression of MT reduces Hg-induced nephrotoxicity. Mercury (Hg) is an important environmenta...

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Published in:Current research in toxicology 2023-01, Vol.5, p.100132-100132, Article 100132
Main Authors: Dave, Aditi, Joshee, Lucy, Barfuss, Delon W., Brownlee, Ryan, Surani, Roha, Anis Ali, Sahar, Ford IV, Earl G., Pittman, Elizabeth G., Caroland, Anasalea V.G., Barkin, Jennifer, Bridges, Christy C.
Format: Article
Language:English
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from the special issue on Invite 2023 edited by Thomas Knudsen
Heavy metals
Kidney
Mercury
Metallothionein
Nephrotoxicity
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Summary:[Display omitted] •Overexpression of metallothionein (MT) alters the corporal distribution of mercury (Hg)•Hg-MT complexes are taken up at the apical and basolateral membranes of proximal tubular cells.•Overexpression of MT reduces Hg-induced nephrotoxicity. Mercury (Hg) is an important environmental toxicant to which humans are exposed on a regular basis. Mercuric ions within biological systems do not exist as free ions. Rather, they are bound to free sulfhydryl groups (thiols) on biological molecules. Metallothionein (MT) is a cysteine-rich, metal-binding protein that has been shown to bind to heavy metals and reduce their toxic effects in target cells and organs. Little is known about the effect of MT on the handing and disposition of Hg. Therefore, the current study was designed to test the hypothesis that overexpression of MT alters the corporal disposition of Hg and reduces its nephrotoxicity. Furthermore, the current study examined the transport of Hg-MT complexes in isolated proximal tubules. Rats were treated with saline or Zn followed by injection with a non-nephrotoxic (0.5 µmol kg−1), moderately nephrotoxic (1.5 µmol kg−1), or significantly nephrotoxic (2.25 µmol kg−1) dose of HgCl2 (containing radioactive Hg). Pretreatment with Zn increased mRNA expression of MT and enhanced accumulation of Hg in the renal cortex of male and female rats. In addition, injection with Zn also protected animals from Hg-induced nephrotoxicity. Studies using isolated proximal tubules from rabbit kidney demonstrated that Hg-MT is taken up rapidly at the apical and basolateral membranes. The current findings suggest that at least part of this uptake occurs through an endocytic process. This study is the first to examine the uptake of Hg-MT complexes in isolated proximal tubules. Overall, the findings of this study suggest that supplementation with Zn may be a viable strategy for reducing the risk of Hg intoxication in at-risk populations.
ISSN:2666-027X
2666-027X
DOI:10.1016/j.crtox.2023.100132