Literature DB >> 22166497

Current understanding of the mechanism of benzene-induced leukemia in humans: implications for risk assessment.

Cliona M McHale1, Luoping Zhang, Martyn T Smith.   

Abstract

Benzene causes acute myeloid leukemia and probably other hematological malignancies. As benzene also causes hematotoxicity even in workers exposed to levels below the US permissible occupational exposure limit of 1 part per million, further assessment of the health risks associated with its exposure, particularly at low levels, is needed. Here, we describe the probable mechanism by which benzene induces leukemia involving the targeting of critical genes and pathways through the induction of genetic, chromosomal or epigenetic abnormalities and genomic instability, in a hematopoietic stem cell (HSC); stromal cell dysregulation; apoptosis of HSCs and stromal cells and altered proliferation and differentiation of HSCs. These effects modulated by benzene-induced oxidative stress, aryl hydrocarbon receptor dysregulation and reduced immunosurveillance, lead to the generation of leukemic stem cells and subsequent clonal evolution to leukemia. A mode of action (MOA) approach to the risk assessment of benzene was recently proposed. This approach is limited, however, by the challenges of defining a simple stochastic MOA of benzene-induced leukemogenesis and of identifying relevant and quantifiable parameters associated with potential key events. An alternative risk assessment approach is the application of toxicogenomics and systems biology in human populations, animals and in vitro models of the HSC stem cell niche, exposed to a range of levels of benzene. These approaches will inform our understanding of the mechanisms of benzene toxicity and identify additional biomarkers of exposure, early effect and susceptibility useful for risk assessment.

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Year:  2011        PMID: 22166497      PMCID: PMC3271273          DOI: 10.1093/carcin/bgr297

Source DB:  PubMed          Journal:  Carcinogenesis        ISSN: 0143-3334            Impact factor:   4.944


  206 in total

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10.  Genetic polymorphisms in hMTH1, hOGG1 and hMYH and risk of chronic benzene poisoning in a Chinese occupational population.

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  80 in total

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Review 4.  The evolving role of the aryl hydrocarbon receptor (AHR) in the normophysiology of hematopoiesis.

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Journal:  Stem Cell Rev Rep       Date:  2012-12       Impact factor: 5.739

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Review 6.  Redox Signaling by Reactive Electrophiles and Oxidants.

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8.  Mapping Proteome-Wide Targets of Environmental Chemicals Using Reactivity-Based Chemoproteomic Platforms.

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Review 10.  Application of toxicogenomic profiling to evaluate effects of benzene and formaldehyde: from yeast to human.

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