Abstract

Leukemia incidence is increasing, especially in children, and the contribution of ubiquitous exposure to environmental leukemogens is unknown. Since mutated ras oncogene is the most frequent abnormality reported in myelodysplastic syndromes and acute myeloid leukemias in humans, we chose to use the z-globin promoted v-Ha-ras Tg.AC transgenic line to investigate the role of an inducible oncogenic ras in the induction of leukemia after exposure to benzene (BZ). Here we describe the morphological and immunophenotypic analysis as well as a spleen colony assay data, to demonstrate that repeated dermal exposure of Tg.AC mice to BZ, but not the nontransgenic parent strain FVB/N, induced a myelogenous leukemia. Profound anemia and marked neutrophilia with presence of a left shift, marked increase in the number of progenitors that differentiated to granulocytes in bone marrow, and infiltration of hematopoietic tissues by myeloid cells characterized the BZ-induced disease. Transformation of a hematopoietic cell was confirmed by transplantation experiments to isogenic, irradiated FVB/N recipients. The absence of symptoms in untreated Tg.AC, as in nontransgenic parent strain, indicated a role for the v-Ha-ras transgene message in the development of BZ-induced myelogenous leukemia. We propose that BZ-induction of the transgene occurred in a bone marrow (BM) progenitor directed toward the granulocytic lineage. By in situ hybridization (ISH) analysis, reverse transcription polymerase chain reaction (RT-PCR) assay and immunohistochemistry staining, here we demonstrated that only leukemic recipient spleen and leukemic donor spleen and liver expressed the inducible ras transgene message concomitant to mitotic activity of hematopoietic blasts. Contrary to control, none of the BZ-treated Tg.AC BM cells expressed the transgene message, possibly due to BZ metabolite toxicity for progenitors. However, recipient mice injected with normal Tg.AC BM cells that express the transgene message did not develop leukemia, suggesting that cell transformation required other mutation(s). Finally, a ribonuclease protection analysis (RPA) demonstrated that the alteration of cytokines in BZ-treated BM could promote the survival of a transformed cell. We hypothesize that the combination of v-Ha-ras activation in a progenitor and the alteration of the cytokines in BM were permissive for a clone of transformed cell to acquire new mutation(s) and the myelogenous leukemia to develop from MPD. - benzene, cancer, leukemia, transgenic, loss of heterozygosity, p53, tumor suppressor gene, ras, protooncogene

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Intramural Research (Z01)
Project #
1Z01ES021134-04
Application #
6432229
Study Section
(LECM)
Project Start
Project End
Budget Start
Budget End
Support Year
4
Fiscal Year
2000
Total Cost
Indirect Cost

  Institution

Name
U.S. National Inst of Environ Hlth Scis
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Kang-Sickel, Juei-Chuan C; Stober, Vandy P; French, John E et al. (2010) Exposure to naphthalene induces naphthyl-keratin adducts in human epidermis in vitro and in vivo. Biomarkers 15:488-97
Donehower, Lawrence A; French, John E; Hursting, Stephen D (2005) The utility of genetically altered mouse models for cancer research. Mutat Res 576:1-3
MacDonald, James; French, John E; Gerson, Ronald J et al. (2004) The utility of genetically modified mouse assays for identifying human carcinogens: a basic understanding and path forward. The Alternatives to Carcinogenicity Testing Committee ILSI HESI. Toxicol Sci 77:188-94
Martin, Keith R; Jokinen, Micheal P; Honeycutt, Hayden P et al. (2004) Tumor profile of novel p53 heterozygous Tg.AC (v-Ha-ras) bitransgenic mice treated with benzo(a)pyrene and fed dietary N-acetyl-L-cysteine (NAC). Toxicol Sci 81:293-301
Martin, Keith R; Jokinen, Michael P; Honeycutt, Hayden P et al. (2004) Tumor spectrum in the p53 heterozygous zeta globin-promoted Tg.AC (v-Ha-ras) bitransgenic mouse model. Toxicol Pathol 32:418-25
French, John E (2004) Identification and characterization of potential human carcinogens using B6.129tm1Trp53 heterozygous null mice and loss of heterozygosity at the Trp53 locus. IARC Sci Publ :271-87
Nwosu, Veronica C; Kissling, Grace E; Trempus, Carol S et al. (2004) Exposure of Tg.AC transgenic mice to benzene suppresses hematopoietic progenitor cells and alters gene expression in critical signaling pathways. Toxicol Appl Pharmacol 196:37-46
Pritchard, John B; French, John E; Davis, Barbara J et al. (2003) The role of transgenic mouse models in carcinogen identification. Environ Health Perspect 111:444-54
Boley, Scott E; Wong, Victoria A; French, John E et al. (2002) p53 heterozygosity alters the mRNA expression of p53 target genes in the bone marrow in response to inhaled benzene. Toxicol Sci 66:209-15
French, J E; Lacks, G D; Trempus, C et al. (2001) Loss of heterozygosity frequency at the Trp53 locus in p53-deficient (+/-) mouse tumors is carcinogen-and tissue-dependent. Carcinogenesis 22:99-106

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