Characterization of<i>Hprt</i>mutations in cDNA and genomic DNA of T‐cell mutants from control and 1,3‐butadiene‐exposed male B6C3F1 mice and F344 rats

Meng, Quanxin; Walker, Dale M.; Scott, Bobby R.; Seilkop, Steve K.; Aden, James K; Walker, Vernon E.

doi:10.1002/em.20002

Cited by 19 publications

(17 citation statements)

References 43 publications

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“…Our results are in agreement with the data from Ma et al (2000) , Burkhart-Schultz and Jones (1997) , and Burkhart-Schultz et al (1996) . Analysis of the in vitro mutational spectra of DEB- and EB-induced mutants in a study by Steen et al (1997a , 1997b) clearly revealed that a decrease in the proportion of single-base substitutions was associated with an increase in the proportion of large deletion mutations Our data and similar findings by Meng et al (2004) indicate that it is not necessary to invoke the formation of DEB as the sole source of large exon deletions; rather, HPRT spectra data from rats indicate that EB-diol is a likely source of deletion mutations.…”

Section: Discussionsupporting

confidence: 78%

“…The authors identified a lower frequency of single-base substitutions, a higher proportion of A:T → T:A transversions and ± 1 frameshift mutations in BD-exposed workers. These changes were also confirmed by Meng et al (2004) in mice and rats. In the future, we plan to analyze more population samples and molecular mutational spectrums in order to elucidate the molecular mutational spectrum associated with butadiene exposure.…”

Section: Discussionsupporting

confidence: 59%

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HPRT Mutations in Lymphocytes from 1,3-Butadiene-Exposed Workers in China

Liu

Du³

et al. 2008

Environ Health Perspect

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Background1,3-Butadiene (BD) is an important industrial chemical and an environmental and occupational pollutant. The carcinogenicity of BD in rodents has been proved, but its carcinogenic and mutagenic molecular mechanism(s) are not fully elucidated in humans.ObjectivesIn the present study, we compared the mutation frequencies and exon deletions of BD-exposed workers with that of control subjects in China to identify the characteristic mutations associated with BD exposure in the human HPRT (hypoxanthine–guanine–phosphoribosyltransferase) gene.MethodsSeventy-four workers exposed to BD via inhalation and 157 matched controls were evaluated in Nanjing, China. Molecular analysis of HPRT mutant T lymphocytes from BD-exposed workers and nonexposed control subjects was conducted to identify changes in the structure of the HPRT gene. A total of 783 HPRT mutants were analyzed by multiplex polymerase chain reaction, in which 368 HPRT mutants were isolated from BD-exposed workers and 415 mutants from control subjects.ResultsThe BD-exposed workers showed a higher mutation frequency (18.2 ± 9.4 × 10−6) than the control subjects (12.7 ± 7.3 × 10−6), but the difference was not significant (p > 0.05). The frequency of exon deletions in BD-exposed workers (27.4%) was significantly higher than that in control subjects (12.5%) (p < 0.05), which mainly included multiplex exon deletions (2–8 exons).ConclusionsThe results of the present study suggest that BD should increase the frequency of large deletions of HPRT gene in human lymphocytes This change confirms and supports the previous findings in BD-exposed workers.

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Section: Discussionsupporting

confidence: 78%

Section: Discussionsupporting

confidence: 59%

HPRT Mutations in Lymphocytes from 1,3-Butadiene-Exposed Workers in China

Liu

Du³

et al. 2008

Environ Health Perspect

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“…Chromosomal alterations (structural and numerical changes) and gene mutations 2-AAF, EO, and DMBA: transgenes (e.g., Lac I); benzene: bone marrow cytogenetics, FISH for translocations, HPRT (in vivo); CPP: bone marrow cytogenetics Chen et al, 2001;Meng et al, 2004;Mittelstaedt et al, 1998;Monroe et al, 1998;Recio et al, 2004;Recio et al, 2001 4. Mutations in critical genes in replicating target cell.…”

Section: Biomarkers Of Exposure and Effect And Bioindicators Of Cancermentioning

confidence: 99%

Creating context for the use of DNA adduct data in cancer risk assessment: I. Data organization

Jarabek

Pottenger

Andrews

et al. 2009

Critical Reviews in Toxicology

115

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The assessment of human cancer risk from chemical exposure requires the integration of diverse types of data. Such data involve effects at the cell and tissue levels. This report focuses on the specific utility of one type of data, namely DNA adducts. Emphasis is placed on the appreciation that such DNA adduct data cannot be used in isolation in the risk assessment process but must be used in an integrated fashion with other information. As emerging technologies provide even more sensitive quantitative measurements of DNA adducts, integration that establishes links between DNA adducts and accepted outcome measures becomes critical for risk assessment. The present report proposes an organizational approach for the assessment of DNA adduct data (e.g., type of adduct, frequency, persistence, type of repair process) in concert with other relevant data, such as dosimetry, toxicity, mutagenicity, genotoxicity, and tumor incidence, to inform characterization of the mode of action. DNA adducts are considered biomarkers of exposure, whereas gene mutations and chromosomal alterations are often biomarkers of early biological effects and also can be bioindicators of the carcinogenic process.

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“…These include alkylated bases, predominantly purines, and interstrand crosslinks Elfarra, 1996, 1999;Tretyakova et al, 1998;Koc et al, 1999;Koivisto et al, 1999;Solomon, 1999;Park and Tretyakova, 2004;Zhang and Elfarra, 2004]. Mutational spectra in cultured cells, as well as mice and humans exposed to BD or BD-epoxides, reveal increases in specific point mutations (A/T?T/A transversions and A/T?G/C transitions) and deletions ranging from simple frameshifts to entire gene regions Recio et al, 2001;Meng et al, 2004]. Studies examining the mutagenicity of synthesized lesions in vitro indicate that *Correspondence to: Jeffrey K. Wickliffe.…”

Section: Introductionmentioning

confidence: 98%

3,4‐Epoxy‐1‐butene, a reactive metabolite of 1,3‐butadiene, induces somatic mutations in Xpc‐null mice

Wickliffe

Galbert

Ammenheuser

et al. 2005

Environ and Mol Mutagen

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Xpc-null (Xpc-/-) mice, deficient in the global genome repair subpathway of nucleotide excision repair (NER-GGR), were exposed by intraperitoneal (i.p.) injection to a 300 mg/kg mutagenic dose of 3,4-epoxy-1-butene (EB), to investigate NER's potential role in repairing butadiene (BD) epoxide DNA lesions. Mutagenic sensitivity was assessed using the Hprt assay. Xpc-/- mice were significantly more sensitive to EB exposure, exhibiting an average 2.8-fold increase in Hprt mutant frequency (MF) relative to those of exposed Xpc+/+ (wild-type) mice. As a positive control for NER-GGR, additional mice were exposed by i.p. injection to a 150 mg/kg mutagenic dose of benzo[a]pyrene (B[a]P). The Xpc-/- mice had MFs 2.9-fold higher than those of exposed Xpc+/+ mice. These results suggest that NER-GGR plays a role in recognizing and repairing some of the DNA adducts formed following in vivo exposure to EB. Additional research is needed to examine the response of Xpc-/- mice, as well as other NER-deficient strains, to inhaled BD. Furthermore, it is likely that alternative DNA repair pathways also are involved in restoring genomic integrity compromised by BD-epoxide DNA damage. Collaborative studies are currently underway to address these critical issues.

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Characterization ofHprtmutations in cDNA and genomic DNA of T‐cell mutants from control and 1,3‐butadiene‐exposed male B6C3F1 mice and F344 rats

Cited by 19 publications

References 43 publications

HPRT Mutations in Lymphocytes from 1,3-Butadiene-Exposed Workers in China

HPRT Mutations in Lymphocytes from 1,3-Butadiene-Exposed Workers in China

Creating context for the use of DNA adduct data in cancer risk assessment: I. Data organization

3,4‐Epoxy‐1‐butene, a reactive metabolite of 1,3‐butadiene, induces somatic mutations in Xpc‐null mice

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