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Terms: benzene
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Stem cell and benzene-induced malignancy and hematotoxicity.
Authors
Wang-L; He-X; Bi-Y; Ma-Q
Source
Chem Res Toxicol 2012 Jul; 25(7):1303-1315
Link
http://dx.doi.org/10.1021/tx3001169 
NIOSHTIC No.
20041132 
Abstract
The biological effect of benzene on the hematopoietic system has been known for over a century. The rapid advancement in understanding the biology of hematopoietic stem cells (HSCs) and cancer stem cells (CSCs) in recent years has renewed interest in investigating the role of stem cells in benzene-induced malignancy and bone marrow depression. The interplay between benzene and stem cells is complex involving the stem cell, progenitor, and HSC niche compartments of the bone marrow. In this prospect, benzene metabolites formed through metabolism in the liver and bone marrow cause damage in hematopoietic cells via multiple mechanisms that, in addition to traditionally recognized chromosomal aberration and covalent binding, incorporate oxidative stress, alteration of gene expression, apoptosis, error-prone DNA repair, epigenetic regulation, and disruption of tumor surveillance. However, benzene-exposed individuals exhibit variable susceptibility to benzene effect that arises, in part, from genetic variations in benzene metabolism, DNA repair, genomic stability, and immune function. These new studies of benzene leukemogenesis and hematotoxicity are expected to provide insights into how environmental and occupational chemicals affect stem cells to cause cancer and toxicity, which impact the risk assessment, permissible level, and therapy of benzene exposure.
Keywords
Benzenes; Biological-effects; Hematopoietic-system; Cancer; Cell-biology; Cell-function; Cellular-function; Malignancy; Bone-marrow; Liver; Chromosome-damage; Tumors; Surveillance-programs; Genes; Immune-reaction; Leukemogenesis
Contact
Qiang Ma, Health Effects Laboratory Division, National Institute for Occupational Safety and Health, 1095 Willowdale Road, Mail Stop 3014, Morgantown, West Virginia 26505
CODEN
CRTOEC
CAS No.
71-43-2
Publication Date
20120701
Document Type
Journal Article
Email Address
qam1@cdc.gov
Fiscal Year
2012
NTIS Accession No.
NTIS Price
Identifying No.
B08012012
Issue of Publication
7
ISSN
0893-228X
NIOSH Division
HELD
Priority Area
Manufacturing
Source Name
Chemical Research in Toxicology
State
WV
Page 8 of 574

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