Polystyrene Microplastics Postpone APAP-Induced Liver Injury through Impeding Macrophage Polarization

Polystyrene microplastics (PS MPs) are micrometer-scale items degraded from plastics and have been detected in various organisms. PS MPs have been identified as causing cognitive, cardiac, intestinal, and hepatic damage. However, their role in liver regeneration under drug-induced liver injury remains unknown. Thus, the current study aims to evaluate the impact of PS MPs on liver repair during APAP hepatotoxicity. PS MPs pretreatment exacerbates mice mortality and hepatocyte apoptosis, suppresses hepatic cell proliferation, and disturbs the inflammatory response in the APAP-induced damage model. Further mechanism exploration uncovers that prior PS MPs administration is sufficient to recruit neutrophils and macrophages, which are necessary for tissue recovery in the acute liver injury model. However, the polarization capacity of macrophages to anti-inflammatory sub-type is significantly delayed in PS MPs plus APAP group compared to the single APAP group, which is the leading cause of tissue repair suppression. Overall, the current study supports a new insight to realize the toxicity of PS MPs in acute liver injury, which should be considered in health risk assessment.

Automated summary

This study explores the impact of polystyrene microplastics (PS MPs) on liver repair during acute liver injury. The results show that pre-treatment with PS MPs exacerbates mortality and hepatocyte apoptosis in mice, suppresses hepatic cell proliferation, and disrupts the inflammatory response. Additionally, PS MPs delay the polarization capacity of macrophages to anti-inflammatory sub-type, leading to tissue repair suppression.