A Quantitative Meta-Analysis of the Relation between Occupational Benzene Exposure and Biomarkers of Cytogenetic Damage

Bernice Scholten; Jelle Vlaanderen; Rob Stierum; Lützen Portengen; Nat Rothman; Qing Lan; Anjoeka Pronk; Roel Vermeulen

doi:10.1289/EHP6404

A Quantitative Meta-Analysis of the Relation between Occupational Benzene Exposure and Biomarkers of Cytogenetic Damage

Environ Health Perspect. 2020 Aug;128(8):87004. doi: 10.1289/EHP6404. Epub 2020 Aug 12.

Authors

Bernice Scholten^{1

2}, Jelle Vlaanderen¹, Rob Stierum², Lützen Portengen¹, Nat Rothman³, Qing Lan³, Anjoeka Pronk², Roel Vermeulen¹

Affiliations

¹ Institute for Risk Assessment Sciences, Utrecht University, Utrecht, Netherlands.
² Netherlands Organisation for Applied Scientific Research, Zeist, Netherlands.
³ Occupational and Environmental Epidemiology Branch, Division of Cancer Epidemiology and Genetics, National Cancer Institute, National Institutes of Health, Department of Health and Human Services, Rockville, Maryland, USA.

PMID: 32783535
PMCID: PMC7422719
DOI: 10.1289/EHP6404

Abstract

Background: The genotoxicity of benzene has been investigated in dozens of biomonitoring studies, mainly by studying (classical) chromosomal aberrations (CAs) or micronuclei (MN) as markers of DNA damage. Both have been shown to be predictive of future cancer risk in cohort studies and could, therefore, potentially be used for risk assessment of genotoxicity-mediated cancers.

Objectives: We sought to estimate an exposure-response curve (ERC) and quantify between-study heterogeneity using all available quantitative evidence on the cytogenetic effects of benzene exposure on CAs and MN respectively.

Methods: We carried out a systematic literature review and summarized all available data of sufficient quality using meta-analyses. We assessed the heterogeneity in slope estimates between studies and conducted additional sensitivity analyses to assess how various study characteristics impacted the estimated ERC.

Results: Sixteen CA (1,356 individuals) and $13 MN$ studies (2,097 individuals) were found to be eligible for inclusion in a meta-analysis. Studies where benzene was the primary genotoxic exposure and that had adequate assessment of both exposure and outcomes were used for the primary analysis. Estimated slope estimates were an increase of 0.27% CA [(95% CI: 0.08%, 0.47%); based on the results from 4 studies] and 0.27% MN [(95% CI: $- 0.23 %$ , 0.76%); based on the results from 7 studies] per parts-per-million benzene exposure. We observed considerable between-study heterogeneity for both end points ( $I^{2} > 90 %$ ).

Discussion: Our study provides a systematic, transparent, and quantitative summary of the literature describing the strong association between benzene exposure and accepted markers of genotoxicity in humans. The derived consensus slope can be used as a best estimate of the quantitative relationship between real-life benzene exposure and genetic damage in future risk assessment. We also quantitate the large between-study heterogeneity that exists in this literature, a factor which is crucial for the interpretation of single-study or consensus slopes. https://doi.org/10.1289/EHP6404.

Publication types

Meta-Analysis
Research Support, Non-U.S. Gov't

MeSH terms

Benzene*
Biomarkers
Cytogenetic Analysis
DNA Damage
Humans
Occupational Exposure / statistics & numerical data*

Substances

Biomarkers
Benzene