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Multilevel toxicity assessment of polypropylene microplastics and pyrene on mussels

DiRROS repository (University of Maribor) 2026
Tatjana Mijošek Pavin, Margareta Kračun-Kolarević, Stoimir Kolarević, Tatjana Simčič, Rajko Martinović, Oliver Bajt, Gabriela Kalčíková, Gabriela Kalčíková, Andreja Ramšak

Summary

Researchers assessed the combined effects of polypropylene microplastics and the pollutant pyrene on Mediterranean mussels over 14 days. They found that while each pollutant individually increased DNA damage, the combination surprisingly did not, suggesting a complex interaction between the two contaminants. However, the combined exposure compromised the mussels' physiological resilience, as shown by their slower heart rate recovery after stress, indicating that co-exposure to microplastics and pollutants can have nuanced biological effects.

Despite extensive research on microplastic pollution, combined biological effects of microplastics and associated pollutants on marine invertebrates remain unclear. We present an integrative assessment of polypropylene (PP) and pyrene, individually and in co-exposure, in mussel Mytilus galloprovincialis. Mussels were exposed to 1 mg L−1 PP (~40 μm) and 50 μg L−1 of pyrene for 7 and 14 days, representing a scenario relevant to highly polluted coastal areas. DNA damage increased significantly in mussels exposed to pyrene or PP alone, but remained at control levels under combined exposure, suggesting an interaction that may reduce genotoxic potential. Lipid peroxidation remained stable across treatments, despite significant changes in antioxidant enzymes. Catalase activity increased in pyrene and pyrene + PP treatments, with tissue-specific trends, indicating enhanced antioxidant protection. Glutathione S-transferase activity was stable in digestive glands but significantly inhibited in gills after seven days under PP exposure. ETS activity increased in pyrene-containing treatments after 14 days, reflecting elevated metabolic demand after prolonged exposure. Respiration rate declined under PP exposure. Heart rate recovery time after the hyposalinity test was the slowest in the pyrene + PP group, indicating compromised physiological resilience. These findings reveal interactive, tissue- and biomarker-specific effects of PP and pyrene. Their combination suggested attenuation of genotoxicity but enhanced physiological stress responses, highlighting the complexity of pollutant interactions and importance of evaluating multiple biomarkers, tissues and pollutants. Presented data provide the first ever biomarker-based evaluation of PP and pyrene co-exposure, offering novel insights into microplastic-pollutant interactions and potential ecological consequences for marine invertebrates.

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