Cadmium at a non-toxic dose alters gene expression in mouse testes

The testes are important targets of cadmium (Cd)-induced toxicity and carcinogenicity in rodents. Exposure to Cd at environmentally relevant low levels is a significant human health concern, but the effects of Cd on the rodent testes at doses that do not cause overt lesions are poorly defined. We us...

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Published inToxicology letters Vol. 154; no. 3; pp. 191 - 200
Main Authors Zhou, Tong, Jia, Xiaodong, Chapin, Robert E., Maronpot, Robert R., Harris, Martha W., Liu, Jie, Waalkes, Michael P., Eddy, Edward M.
Format Journal Article
LanguageEnglish
Published Shannon Elsevier Ireland Ltd 30.12.2004
Amsterdam Elsevier Science
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Abstract The testes are important targets of cadmium (Cd)-induced toxicity and carcinogenicity in rodents. Exposure to Cd at environmentally relevant low levels is a significant human health concern, but the effects of Cd on the rodent testes at doses that do not cause overt lesions are poorly defined. We used cDNA microarray and quantitative real-time RT-PCR assays to determine gene expression profiles in the testes of CD-1 mice 12–72 h after a single s.c. injection of 5 μmol/kg CdCl 2. This dose of Cd did not produce overt histopathological changes, but clearly altered the expression of some genes that are likely to be important in toxicity responses. The most significant changes in gene expression occurred 24 h after treatment, corresponding to when the highest level of Cd was detected in the testes. Increased expression of the C- myc and Egr1 genes strongly suggests acute stress responses. Repressed expression of cell cycle-regulated cyclin B1 and CDC2 proteins indicates a potential for causing G2/M arrest and disturbance of meiosis. Decreased expression of pro-apoptotic genes, particularly Casp3, and DNA repair genes possibly contributes to Cd-induced carcinogenesis. These results indicate that changes in gene expression occur well before overt effects of Cd-induced testicular toxicity and carcinogenicity are apparent.
AbstractList The testes are important targets of cadmium (Cd)-induced toxicity and carcinogenicity in rodents. Exposure to Cd at environmentally relevant low levels is a significant human health concern, but the effects of Cd on the rodent testes at doses that do not cause overt lesions are poorly defined. We used cDNA microarray and quantitative real-time RT-PCR assays to determine gene expression profiles in the testes of CD-1 mice 12–72 h after a single s.c. injection of 5 μmol/kg CdCl 2. This dose of Cd did not produce overt histopathological changes, but clearly altered the expression of some genes that are likely to be important in toxicity responses. The most significant changes in gene expression occurred 24 h after treatment, corresponding to when the highest level of Cd was detected in the testes. Increased expression of the C- myc and Egr1 genes strongly suggests acute stress responses. Repressed expression of cell cycle-regulated cyclin B1 and CDC2 proteins indicates a potential for causing G2/M arrest and disturbance of meiosis. Decreased expression of pro-apoptotic genes, particularly Casp3, and DNA repair genes possibly contributes to Cd-induced carcinogenesis. These results indicate that changes in gene expression occur well before overt effects of Cd-induced testicular toxicity and carcinogenicity are apparent.
The testes are important targets of cadmium (Cd)-induced toxicity and carcinogenicity in rodents. Exposure to Cd at environmentally relevant low levels is a significant human health concern, but the effects of Cd on the rodent testes at doses that do not cause overt lesions are poorly defined. We used cDNA microarray and quantitative real-time RT-PCR assays to determine gene expression profiles in the testes of CD-1 mice 12-72 h after a single s.c. injection of 5 mu mol/kg CdCl sub(2). This dose of Cd did not produce overt histopathological changes, but clearly altered the expression of some genes that are likely to be important in toxicity responses. The most significant changes in gene expression occurred 24 h after treatment, corresponding to when the highest level of Cd was detected in the testes. Increased expression of the C-myc and Egr1 genes strongly suggests acute stress responses. Repressed expression of cell cycle-regulated cyclin B1 and CDC2 proteins indicates a potential for causing G2/M arrest and disturbance of meiosis. Decreased expression of pro-apoptotic genes, particularly Casp3, and DNA repair genes possibly contributes to Cd-induced carcinogenesis. These results indicate that changes in gene expression occur well before overt effects of Cd- induced testicular toxicity and carcinogenicity are apparent.
The testes are important targets of cadmium (Cd)-induced toxicity and carcinogenicity in rodents. Exposure to Cd at environmentally relevant low levels is a significant human health concern, but the effects of Cd on the rodent testes at doses that do not cause overt lesions are poorly defined. We used cDNA microarray and quantitative real-time RT-PCR assays to determine gene expression profiles in the testes of CD-1 mice 12-72 h after a single s.c. injection of 5 micromol/kg CdCl2. This dose of Cd did not produce overt histopathological changes, but clearly altered the expression of some genes that are likely to be important in toxicity responses. The most significant changes in gene expression occurred 24 h after treatment, corresponding to when the highest level of Cd was detected in the testes. Increased expression of the C-myc and Egr1 genes strongly suggests acute stress responses. Repressed expression of cell cycle-regulated cyclin B1 and CDC2 proteins indicates a potential for causing G2/M arrest and disturbance of meiosis. Decreased expression of pro-apoptotic genes, particularly Casp3, and DNA repair genes possibly contributes to Cd-induced carcinogenesis. These results indicate that changes in gene expression occur well before overt effects of Cd-induced testicular toxicity and carcinogenicity are apparent.
Author Liu, Jie
Jia, Xiaodong
Chapin, Robert E.
Harris, Martha W.
Maronpot, Robert R.
Zhou, Tong
Waalkes, Michael P.
Eddy, Edward M.
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  fullname: Eddy, Edward M.
  email: eddy@niehs.nih.gov
  organization: Gamete Biology Section, Laboratory of Reproductive and Developmental Toxicology, National Institute of Environmental Health Sciences, National Institutes of Health, Research Triangle Park, NC 27709, USA
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Issue 3
Keywords Real-time RT-PCR
Cadmium
Mouse
Microarray
Testes
RNA-directed DNA polymerase
Enzyme
Toxicity
Transferases
Rodentia
DNA chip
Gene expression
Real time
Testicle
Male genital system
Heavy metal
Nucleotidyltransferases
Vertebrata
Mammalia
Animal
Dose
Reverse transcription polymerase chain reaction
Language English
License CC BY 4.0
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Snippet The testes are important targets of cadmium (Cd)-induced toxicity and carcinogenicity in rodents. Exposure to Cd at environmentally relevant low levels is a...
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SubjectTerms Animals
Apoptosis - drug effects
Biological and medical sciences
Cadmium
Cadmium - pharmacokinetics
Cadmium - toxicity
Cell Cycle - drug effects
Cell Proliferation - drug effects
Chemical and industrial products toxicology. Toxic occupational diseases
DNA Damage - drug effects
DNA Repair - drug effects
Gene Expression Profiling
Gene Expression Regulation - drug effects
Male
Medical sciences
Metals and various inorganic compounds
Mice
Microarray
Mouse
Oligonucleotide Array Sequence Analysis
Real-time RT-PCR
Testes
Testis - drug effects
Testis - metabolism
Testis - pathology
Toxicology
Title Cadmium at a non-toxic dose alters gene expression in mouse testes
URI https://dx.doi.org/10.1016/j.toxlet.2004.07.015
https://www.ncbi.nlm.nih.gov/pubmed/15501611
https://search.proquest.com/docview/18066499
Volume 154
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