Benzene poisoning, a risk factor for hematological malignancy, is associated with the NQO1 super(609)C arrow right T mutation and rapid fractional excretion of chlorzoxazone

Benzene is a ubiquitous occupational hematotoxin and leukemogen, but people vary in their response to this toxic agent. To evaluate the impact of interindividual variation in enzymes that activate (i.e., CYP2E1) and detoxify (i.e., NQO1) benzene and its metabolites, we carried out a case-control stu...

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Published inCancer research (Chicago, Ill.) Vol. 57; no. 14; pp. 2839 - 2842
Main Authors Rothman, N, Smith, M T, Hayes, R B, Traver, R D, Hoener, B, Campleman, S, Li, Gui-Lan, Dosemeci, M, Linet, M, Zhang, Luoping
Format Journal Article
LanguageEnglish
Published 01.07.1997
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Abstract Benzene is a ubiquitous occupational hematotoxin and leukemogen, but people vary in their response to this toxic agent. To evaluate the impact of interindividual variation in enzymes that activate (i.e., CYP2E1) and detoxify (i.e., NQO1) benzene and its metabolites, we carried out a case-control study in Shanghai, China, of occupational benzene poisoning (BP; i.e., hematotoxicity), which we show is itself strongly associated with subsequent development of acute nonlymphocytic leukemia and the related myelodysplastic syndromes (relative risk, 70.6; 95% confidence interval, 11.4-439.3). CYP2E1 and NQO1 genotypes were determined by PCR-RFLP, and CYP2E1 enzymatic activity was estimated by the fractional excretion of chlorzoxazone (fe sub(6-OH)) for 50 cases of BP and 50 controls. Subjects with both a rapid fe sub(6-OH) and two copies of the NQO1 super(609)C arrow right T mutation had a 7.6-fold (95% confidence interval, 1.8-31.2) increased risk of BP compared to subjects with a slow fe sub(6-OH) who carried one or two wild-type NQO1 alleles. In contrast, the CYP2E1 PstI/RsaI polymorphism did not influence BP risk. This is the first report that provides evidence of human susceptibility to benzene-related disease. Further evaluation of susceptibility for hematotoxicity and hematological malignancy among workers with a history of occupational exposure to benzene is warranted.
AbstractList Benzene is a ubiquitous occupational hematotoxin and leukemogen, but people vary in their response to this toxic agent. To evaluate the impact of interindividual variation in enzymes that activate (i.e., CYP2E1) and detoxify (i.e., NQO1) benzene and its metabolites, we carried out a case-control study in Shanghai, China, of occupational benzene poisoning (BP; i.e., hematotoxicity), which we show is itself strongly associated with subsequent development of acute nonlymphocytic leukemia and the related myelodysplastic syndromes (relative risk, 70.6; 95% confidence interval, 11.4-439.3). CYP2E1 and NQO1 genotypes were determined by PCR-RFLP, and CYP2E1 enzymatic activity was estimated by the fractional excretion of chlorzoxazone (fe sub(6-OH)) for 50 cases of BP and 50 controls. Subjects with both a rapid fe sub(6-OH) and two copies of the NQO1 super(609)C arrow right T mutation had a 7.6-fold (95% confidence interval, 1.8-31.2) increased risk of BP compared to subjects with a slow fe sub(6-OH) who carried one or two wild-type NQO1 alleles. In contrast, the CYP2E1 PstI/RsaI polymorphism did not influence BP risk. This is the first report that provides evidence of human susceptibility to benzene-related disease. Further evaluation of susceptibility for hematotoxicity and hematological malignancy among workers with a history of occupational exposure to benzene is warranted.
Author Hayes, R B
Traver, R D
Campleman, S
Zhang, Luoping
Linet, M
Rothman, N
Li, Gui-Lan
Smith, M T
Hoener, B
Dosemeci, M
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Title Benzene poisoning, a risk factor for hematological malignancy, is associated with the NQO1 super(609)C arrow right T mutation and rapid fractional excretion of chlorzoxazone
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