4.7 Article

Ingested Polystyrene Nanospheres Translocate to Placenta and Fetal Tissues in Pregnant Rats: Potential Health Implications

Journal

NANOMATERIALS
Volume 13, Issue 4, Pages -

Publisher

MDPI
DOI: 10.3390/nano13040720

Keywords

plastics; nanoplastics; rat; translocation; placenta; fetus

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Recent studies have found that oral exposure to micro- and nano-plastics during pregnancy can have adverse effects on outcomes and progeny. This study examined the translocation of ingested nanoscale polystyrene MNPs to the placenta and fetal tissues in pregnant rats, and found that these MNPs can breach the intestinal and placental barriers to access the fetal circulation and all fetal tissues. Further research is needed to understand the mechanisms and potential adverse effects of this translocation.
Recent studies in experimental animals found that oral exposure to micro- and nano-plastics (MNPs) during pregnancy had multiple adverse effects on outcomes and progeny, although no study has yet identified the translocation of ingested MNPs to the placenta or fetal tissues, which might account for those effects. We therefore assessed the placental and fetal translocation of ingested nanoscale polystyrene MNPs in pregnant rats. Sprague Dawley rats (N = 5) were gavaged on gestational day 19 with 10 mL/kg of 250 mu g/mL 25 nm carboxylated polystyrene spheres (PS25C) and sacrificed after 24 h. Hyperspectral imaging of harvested placental and fetal tissues identified abundant PS25C within the placenta and in all fetal tissues examined, including liver, kidney, heart, lung and brain, where they appeared in 10-25 mu m clusters. These findings demonstrate that ingested nanoscale polystyrene MNPs can breach the intestinal barrier and subsequently the maternal-fetal barrier of the placenta to access the fetal circulation and all fetal tissues. Further studies are needed to assess the mechanisms of MNP translocation across the intestinal and placental barriers, the effects of MNP polymer, size and other physicochemical properties on translocation, as well as the potential adverse effects of MNP translocation on the developing fetus.

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