Exploring the associations between phthalate exposure and cardiometabolic risk factors clustering among children: The potential mediating role of insulin-resistant-related genes DNA methylation

The relationship between childhood phthalates (PAEs) exposure, DNA methylation, and cardiometabolic risk (CMR) factors is not well understood. Children were included from a longitudinal cohort 2018–2020 in Xiamen, China. A nest case-control study was additionally conducted, and methylation in lysyl...

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Published in:Journal of hazardous materials 2024-01, Vol.461, p.132578-132578, Article 132578
Main Authors: Liu, Jieyu, Song, Jieyun, Gao, Di, Li, Yanhui, Guo, Tongjun, Yuan, Wen, Chen, Manman, Chen, Li, Zhang, Yi, Ma, Qi, Cui, Mengjie, Song, Xinli, Wang, Ruolin, Jiang, Jianuo, Zou, Zhiyong, Dong, Yanhui, Ma, Jun
Format: Article
Language:English
Subjects:
Cardiometabolic risk factors
case-control studies
childhood
Children
China
DNA methylation
Epigenetic
family
longitudinal studies
nests
Phthalates
risk
solutes
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Summary:The relationship between childhood phthalates (PAEs) exposure, DNA methylation, and cardiometabolic risk (CMR) factors is not well understood. Children were included from a longitudinal cohort 2018–2020 in Xiamen, China. A nest case-control study was additionally conducted, and methylation in lysyl oxidase-like 3 (LOXL3) and solute Carrier Family 6 Member 19 (SLC6A19) were measured. Generalized linear models were used to estimate the associations between PAEs exposure and CMR factors, and mediation analyses of DNA methylation were conducted. The longitudinal study included 835 children aged 7–11 years, and the nest case-control study included 120 cases and 120 controls. Exposure to higher PAEs was correlated with increased CMR scores at baseline (β = 0.299, 95 %CI = 0.114, 0.485) and the final visit (β = 0.202, 95 %CI = 0.008, 0.397). In nest case-control study, higher mono-n-butyl phthalate (MnBP) exposure was related with elevated triglycerides (TG) (β = 0.283, 95 %CI = 0.025, 0.540). A decrement of methylation of CpG 33.34 of LOXL3 was found in response to MnBP exposure (β = −0.014, 95 %CI = −0.027, −0.001). Furthermore, increased methylation of LOXL3_CpG 33.34 and SLC6A19_CpG 11.12 was related to reduced TG. De-methylation of LOXL3_CpG 33.34 and SLC6A19_CpG 11.12 could mediate MnBP-TG pathways. Childhood exposure to PAEs was associated with increased CMR scores, and mediation of PAE exposure on childhood cardiometabolic health by LOXL3 and SLC6A19 de-methylation was observed. [Display omitted] •Childhood PAEs exposure longitudinally increased cardiometabolic risk (CMR) scores.•PAEs exposure reduced DNA methylation of insulin-resistant-related LOXL3 and SLC6A19.•LOXL3 and SLC6A19 de-methylation mediate childhood PAEs-CMR, especially TG increase.•Add epidemiological and epigenetic evidence about PAEs and cardiometabolic health.
ISSN:0304-3894
1873-3336
DOI:10.1016/j.jhazmat.2023.132578