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Tracking alternative versions of the galactose gene network in the genus Saccharomyces and their expansion after domestication
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Metadata
Document Title
Tracking alternative versions of the galactose gene network in the genus Saccharomyces and their expansion after domestication
Author
Pontes A., Para?so F., Liu Y.-C., Limtong S., Jindamorakot S., Jespersen L., Gon?alves C., Rosa C.A., Tsai I.J., Rokas A., Hittinger C.T., Gon?alves P., Sampaio J.P.
Affiliations
Occupational Health and Safety Program, Faculty of Science and Technology, Bansomdejchaopraya Rajabhat University, Bangkok, Thailand; National Center for Genetic Engineering and Biotechnology (BIOTEC), National Science and Technology Development Agency, Pathum Thani, Thailand; Nutrition Division, Faculty of Medicine Ramathibodi Hospital, Mahidol University, Bangkok, Thailand; Department of Industrial Hygiene and Safety, Faculty of Public Health, Burapha University, Chonburi, Thailand
Type
Article
Source Title
Biomarker Insights
ISSN
11772719
Year
2024
Volume
19
Open Access
All Open Access, Gold
Publisher
SAGE Publications Ltd
DOI
10.1177/11772719241259604
Abstract
Background: Research on the proteomes impact of benzene exposure in fuel station employees remains sparse, underscoring the need for detailed health impact assessments focusing on biomarker evaluation. Objectives: This investigation aimed to analyze the differences in blood parameters and serum proteomes resulting from benzene exposure between gasoline station attendants (B-GSA) and a control group. Design and methods: A cross-sectional analytical study was conducted with 96 participants, comprising 54 in the B-GSA group and 42 in the control group. The methodology employed included an interview questionnaire alongside urine and blood sample collections. The urine samples were analyzed for trans,trans-muconic acid (t,t-MA) levels, while the blood samples underwent complete blood count analysis and proteome profiling. Results: Post-shift analysis indicated that the B-GSA group exhibited significantly higher levels of t,t-MA and monocytes compared to the control group (P <.05). Proteome quantification identified 1448 proteins differentially expressed between the B-GSA and control groups. Among these, 20 proteins correlated with the levels of t,t-MA in urine. Notably, 4 proteins demonstrated more than a 2-fold down-regulation in the B-GSA group: HBS1-like, non-structural maintenance of chromosomes element 1 homolog, proprotein convertase subtilisin/kexin type 4, and zinc finger protein 658. The KEGG pathway analysis revealed associations with apoptosis, cancer pathways, p53 signaling, and the TNF signaling pathway. Conclusion: The changes in these 4 significant proteins may elucidate the molecular mechanisms underlying benzene toxicity and suggest their potential as biomarkers for benzene poisoning in future assessments. ? The Author(s) 2024.
Keyword
benzene | Biomarker | complete blood count | gasoline station attendants | Proteomes
License
CC BY-NC
Rights
Authors
Publication Source
WoS