Literature DB >> 7871536

Sensitivity to cadmium-induced genotoxicity in rat testicular cells is associated with minimal expression of the metallothionein gene.

N Shiraishi1, J F Hochadel, T P Coogan, J Koropatnick, M P Waalkes.   

Abstract

Cadmium is a carcinogenic metal. Although the mechanism of tumor induction is unknown, DNA/metal interactions may be involved. Metallothionein can protect against cadmium toxicity in our previous work it was shown to reduce cadmium genotoxicity in cultured cells. To extend these results, the genotoxicity of cadmium was studied in R2C cells, a rat testicular Leydig cell line. The R2C cells were very sensitive to cadmium-induced single-strand DNA damage (SSD), as measured by alkaline elution. SSD occurred in R2C cells after treatment with 25 and 50 microM CdCl2 for 2 hr. Prior work showed other cells required much higher levels of cadmium (approximately 500 microM) to induce genotoxicity. The genotoxic levels of cadmium (25-50 microM) were not cytotoxic in R2C cells as assessed by a metabolic activity (MTT) assay. Pretreatment of R2C cells with a low cadmium dose (2 microM, 24 hr) had no effect on cadmium-induced SSD, in contrast to prior work in other cells where such pretreatments reduced SSD through metallothionein gene activation. In fact, cadmium or zinc treatments resulted in little or no increase in metallothionein gene expression in R2C cells as determined by Northern blot analysis for metallothionein mRNA using cDNA or oligonucleotide probes and radioimmunoassay for metallothionein protein production. Basal metallothionein mRNA was essentially nondetectable. Induction of a cadmium-binding protein in R2C cells did occur, as determined by Cd-heme assay, but did not induce tolerance to SSD. In vivo, the Leydig cell is a target for cadmium carcinogenicity and its cadmium-binding protein is thought not to be a true metallothionein. These results indicate that R2C cells are sensitive to cadmium-induced genotoxicity and that this sensitivity is associated with minimal expression of the metallothionein gene.

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Year:  1995        PMID: 7871536     DOI: 10.1006/taap.1995.1028

Source DB:  PubMed          Journal:  Toxicol Appl Pharmacol        ISSN: 0041-008X            Impact factor:   4.219


  8 in total

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Authors:  C Q Zhao; M R Young; B A Diwan; T P Coogan; M P Waalkes
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Review 2.  Cadmium-induced testicular injury.

Authors:  Erica R Siu; Dolores D Mruk; Catarina S Porto; C Yan Cheng
Journal:  Toxicol Appl Pharmacol       Date:  2009-02-21       Impact factor: 4.219

3.  Expression of metallothionein gene at different time in testicular interstitial cells and liver of rats treated with cadmium.

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Journal:  World J Gastroenterol       Date:  2003-07       Impact factor: 5.742

4.  Metallothionein blocks oxidative DNA damage in vitro.

Authors:  Wei Qu; Jingbo Pi; Michael P Waalkes
Journal:  Arch Toxicol       Date:  2012-08-23       Impact factor: 5.153

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6.  Exposure of human proximal tubule cells to cd2+, zn2+, and Cu2+ induces metallothionein protein accumulation but not metallothionein isoform 2 mRNA.

Authors:  S H Garrett; S Somji; J H Todd; D A Sens
Journal:  Environ Health Perspect       Date:  1998-09       Impact factor: 9.031

7.  Variation of Metallothionein I and II Gene Expression in the Bank Vole (Clethrionomys glareolus) Under Environmental Zinc and Cadmium Exposure.

Authors:  Magdalena Mikowska; Barbara Dziublińska; Renata Świergosz-Kowalewska
Journal:  Arch Environ Contam Toxicol       Date:  2017-12-16       Impact factor: 2.804

8.  Role of metallothionein-like cadmium-binding protein (MTLCdBP) in the protective mechanism against cadmium toxicity in the testis.

Authors:  Hisayoshi Ohta; Yonggang Qi; Kenichi Ohba; Tatsushi Toyooka; Rui-Sheng Wang
Journal:  Ind Health       Date:  2018-12-29       Impact factor: 2.179

  8 in total

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