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Reduced dietary Ca, Cu, Zn, Mn, and Mg bioavailability but increased Fe bioavailability with polyethylene microplastic ingestion in a mouse model: Changes in intestinal permeability and gut metabolites

The Science of The Total Environment 2023 16 citations ? Citation count from OpenAlex, updated daily. May differ slightly from the publisher's own count. Score: 55 ? 0–100 AI score estimating relevance to the microplastics field. Papers below 30 are filtered from public browse.
Shan Chen, Shan Chen, Shiwei Li, Shiwei Li, Xueyuan Gu, Xueyuan Gu, Dongmei Zhou, Xueyuan Gu, Xueyuan Gu, Q. Lena, Hongbo Li Dongmei Zhou, Xueyuan Gu, Dongmei Zhou, Dongmei Zhou, Q. Lena, Q. Lena, Hongbo Li Hongbo Li Dongmei Zhou, Dongmei Zhou, Dongmei Zhou, Dongmei Zhou, Xueyuan Gu, Dongmei Zhou, Hongbo Li Dongmei Zhou, Q. Lena, Dongmei Zhou, Dongmei Zhou, Dongmei Zhou, Dongmei Zhou, Q. Lena, Q. Lena, Hongbo Li Dongmei Zhou, Shiwei Li, Xueyuan Gu, Dongmei Zhou, Dongmei Zhou, Dongmei Zhou, Q. Lena, Dongmei Zhou, Hongbo Li

Summary

Researchers fed mice diets containing polyethylene microplastics of two different sizes for 35 days and measured how plastic exposure affected the absorption of essential dietary minerals. They found that microplastic ingestion significantly reduced the bioavailability of calcium, copper, zinc, manganese, and magnesium, while unexpectedly increasing iron absorption. The study suggests that chronic microplastic ingestion could interfere with nutritional mineral uptake, potentially contributing to mineral deficiencies over time.

Microplastics emerge as a new environmental and human health crisis. Minimal research exists on effects of microplastic ingestion on the oral bioavailability of minerals (Fe, Ca, Cu, Zn, Mn, and Mg) in the gastrointestinal tract via impacting intestinal permeability, mineral transcellular transporters, and gut metabolites. Here, mice were exposed to polyethylene spheres of 30 and 200 μm (PE-30 and PE-200) in diet (2, 20, and 200 μg PE g) for 35 d to determine the microplastic effects on mineral oral bioavailability. Results showed that for mice fed diet amended with PE-30 and PE-200 at 2-200 μg g, Ca, Cu, Zn, Mn, and Mg concentrations in the small intestine tissue were 43.3-68.8 %, 28.6-52.4 %, 19.3-27.1 %, 12.9-29.9 %, and 10.2-22.4 % lower compared to control mice, suggesting hampered bioavailability of these minerals. In addition, Ca and Mg concentrations in mouse femur were 10.6 % and 11.0 % lower with PE-200 at 200 μg g. In contrast, Fe bioavailability was elevated, as suggested by significantly (p < 0.05) higher Fe concentration in the intestine tissue of mice exposed to PE-200 than control mice (157-180 vs. 115 ± 7.58 μg Fe g) and significantly (p < 0.05) higher Fe concentrations in liver and kidney with PE-30 and PE-200 at 200 μg g. Following PE-200 exposure at 200 μg g, genes coding for duodenal expression of tight junction proteins (e.g., claudin 4, occludin, zona occludins 1, and cingulin) were significantly up-regulated, possibility weakening intestinal permeability to Ca, Cu, Zn, Mn, and Mg ions. The elevated Fe bioavailability was possibly related to microplastic-induced greater abundances of small peptides in the intestinal tract, which inhibited Fe precipitation and elevated Fe solubility. Results showed that microplastic ingestion may cause Ca, Cu, Zn, Mn, and Mg deficiency but Fe overload via altering intestinal permeability and gut metabolites, posing a threat to human nutrition health.

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