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Polystyrene nanoplastics and microplastics can act as Trojan horse carriers of benzo(a)pyrene to mussel hemocytes in vitro

Scientific Reports 2021 92 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.
María Paula Carrillo, Alberto Katsumiti Alberto Katsumiti Alberto Katsumiti María Paula Carrillo, Alberto Katsumiti Marta Silene Ferreira Barros, Alberto Katsumiti Alberto Katsumiti Alberto Katsumiti Miren P. Cajaraville, Miren P. Cajaraville, Miren P. Cajaraville, Alberto Katsumiti Miren P. Cajaraville, Miren P. Cajaraville, Miren P. Cajaraville, Miren P. Cajaraville, Miren P. Cajaraville, Miren P. Cajaraville, Miren P. Cajaraville, Alberto Katsumiti Miren P. Cajaraville, Miren P. Cajaraville, Miren P. Cajaraville, Miren P. Cajaraville, Alberto Katsumiti Miren P. Cajaraville, Miren P. Cajaraville, Miren P. Cajaraville, Alberto Katsumiti Alberto Katsumiti Alberto Katsumiti

Summary

Researchers demonstrated that polystyrene nanoplastics and microplastics can act as carriers to transfer the carcinogenic pollutant benzo(a)pyrene into mussel immune cells in laboratory experiments. The plastic particles were internalized by the cells and found both inside and outside lysosomes, with each contaminant contributing different toxic effects. The study raises concerns that microplastics combined with environmental pollutants may pose greater risks to marine organisms than either contaminant alone.

Polymers
Study Type In vitro

In this work we studied the ability of polystyrene (PS) nanoplastics (NPs) and microplastics (MPs) to transfer benzo(a)pyrene (BaP) to mussel hemocytes and to produce toxic effects in vitro. For this, intracellular fate and toxicity of PS NPs (0.05 μm) and MPs (0.5 and 4.5 μm) alone or with BaP and of BaP alone were assessed. Particles of 0.05 and 0.5 µm largely aggregated in the exposure medium whereas presence of BaP reduced particle aggregation. Cells internalized PS NPs and MPs alone or with BaP and these were found inside and outside lysosomes, depending on their size. PS particles alone or with BaP were cytotoxic to hemocytes only at the highest concentrations tested. The same was true for most sublethal endpoints except for increased phagocytic activity provoked by NPs and 0.5 μm MPs at lower concentrations. Plastic particles appeared to be the main drivers for reduced plasma membrane integrity and increased phagocytic and lysosomal activities whereas BaP appeared to contribute more to reduced cell viability and phagocytosis and increased ROS production and genotoxicity. Overall, PS NPs and MPs can act as carriers of BaP to mussel hemocytes, rising concerns about risks plastics associated to pollutants may pose to aquatic organisms.

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