AI Article Synopsis

  • Lead (Pb) is a harmful contaminant that can affect fetal development during pregnancy, with exposure occurring through diet and maternal bone release.
  • The study explored how different variants of the Apolipoprotein E gene (APOE) in pregnant women relate to Pb levels in both maternal and cord blood, considering the sex of the fetus and the number of previous pregnancies (parity).
  • Results showed that the maternal ε2 gene variant correlated with higher Pb levels in female fetuses, while the ε4 variant correlated with lower Pb levels, highlighting the complex roles of genetics and fetal factors in Pb exposure during pregnancy.

Article Abstract

Lead (Pb) is a global contaminant associated with multiple adverse health effects. Humans are especially vulnerable during critical developmental stages. During pregnancy, exposure to Pb can occur through diet and release from maternal bones. Apolipoprotein E gene (APOE) variants (ɛ2, ɛ3, ɛ4 alleles) may influence sex steroid hormones, bone metabolism, and Pb kinetics. We examined the interplay among maternal APOE (mAPOE) genotypes, fetal sex, parity, and Pb in maternal and cord blood (mB-Pb, CB-Pb) using linear regression models. Our study involved 817 pregnant women and 772 newborns with measured adequate levels of zinc and selenium. We compared carriers of the ε2 and ε4 alleles to those with the ε3/ε3 genotype. The geometric means (range) of mB-Pb and CB-Pb were 11.1 (3.58-87.6) and 9.31 (1.82-47.0) ng/g, respectively. In cases with female fetuses, the maternal mAPOE ε2 allele was associated with higher, while the mAPOE ε4 allele was associated with lower mB-Pb and CB-Pb levels. Nulliparity increased the strength of the observed associations. These findings highlight the significance of mAPOE genetics, fetal sex, and parity in prenatal Pb kinetics. Notably, the maternal ε2 allele may increase the risk of Pb exposure.

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Source
http://dx.doi.org/10.1016/j.envres.2024.119583DOI Listing

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