Long-term environmental metal exposure is associated with hypomethylation of CpG sites in NFKB1 and other genes related to oncogenesis
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Abstract
Background
Long-term environmental exposure to metals leads to epigenetic changes and may increase risks
to human health. The relationship between the type and level of metal exposure and epigenetic changes in subjects
exposed to high concentrations of metals in the environment is not yet clear. The aim of our study is to fnd the pos sible association of environmental long-term exposure to metals with DNA methylation changes of genes related
to immune response and carcinogenesis. We investigated the association of plasma levels of 21 essential and non essential metals detected by ICP-MS and the methylation level of 654 CpG sites located on NFKB1, CDKN2A, ESR1,
APOA5, IGF2 and H19 genes assessed by targeted bisulfte sequencing in a cohort of 40 subjects living near metal
mining area and 40 unexposed subjects. Linear regression was conducted to fnd diferentially methylated positions
with adjustment for gender, age, BMI class, smoking and metal concentration.
Results
In the metal-exposed group, fve CpGs in the NFKB1 promoter region were hypomethylated compared
to unexposed group. Four diferentially methylated positions (DMPs) were associated with multiple metals, two
of them are located on NFKB1 gene, and one each on CDKN2A gene and ESR1 gene. Two DMPs located on NFKB1
(chr4:102500951, associated with Be) and IGF2 (chr11:2134198, associated with U) are associated with specifc metal
levels. The methylation status of the seven CpGs located on NFKB1 (3), ESR1 (2) and CDKN2A (2) positively correlated
with plasma levels of seven metals (As, Sb, Zn, Ni, U, I and Mn).
Conclusions
Our study revealed methylation changes in NFKB1, CDKN2A, IGF2 and ESR1 genes in individuals
with long-term human exposure to metals. Further studies are needed to clarify the efect of environmental metal
exposure on epigenetic mechanisms and pathways involved.
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Subject(s)
toxic metal, environmental exposure, DNA methylation, NFKB1, CDKN2A, IGF2, ESR1, uranium
Citation
Clinical Epigenetics. 2023, vol. 15, issue 1, art. no. 126.