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Polystyrene nanoplastics induce profound metabolic shift in human cells as revealed by integrated proteomic and metabolomic analysis

Environment International 2022 64 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.
Lei Wang Lei Wang Lei Wang Lei Wang Hua Wang, Lei Wang Lei Wang Lei Wang Xu Zhang, Xuelian Shi, Lei Wang Lei Wang Xuelian Shi, Xuelian Shi, Lei Wang Xuelian Shi, Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Yan Gao, Hua Wang, Lei Wang Lei Wang Lei Wang Xiangyang Zhang, Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Xu Zhang, Xu Zhang, Lei Wang Lei Wang Lei Wang Xiangyang Zhang, Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Hongzhi Zhao, Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Hongzhi Zhao, Hongzhi Zhao, Lei Wang Xu Zhang, Lei Wang Lei Wang Hua Wang, Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Ruibing Chen, Lei Wang Lei Wang Lei Wang Xu Zhang, Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Xu Zhang, Lei Wang Lei Wang Lei Wang Lei Wang Lei Wang Ruibing Chen, Lei Wang Lei Wang Lei Wang Lei Wang

Summary

Researchers used integrated proteomic and metabolomic analysis to study how polystyrene nanoplastics affect human kidney and liver cell lines. The study quantified changes in thousands of proteins and hundreds of metabolites, revealing that nanoplastic exposure induced a profound metabolic shift in human cells. Evidence indicates that nanoplastics can be internalized by human cells and trigger significant biological changes at the molecular level.

Polymers
Body Systems

Nanoplastics (NPLs) are widespread in our environment. However, their impacts on human health and precise toxicity mechanisms remain poorly understood. Here we studied the internalization, release, and cytotoxicity of polystyrene nanoplastics (PSNPs) using the renal tubular epithelial cell line HKC and human derived liver cell line HL-7702. We also employed an integrated proteomic and metabolomic approach to investigate the potential biological effects of PSNPs on HKC cells. The abundances of 4770 proteins and 100 metabolites were quantified, with 785 proteins and 17 metabolites detected with altered levels in response to PSNPs. Most of the differential proteins and metabolites were enriched in a variety of metabolic pathways, for example, glycolysis, citrate cycle, oxidative phosphorylation, and amino acid metabolism, suggesting the potential effects of NPLs on global cellular metabolism shift in human cells. The altered energy metabolism induced by PSNPs was further confirmed by a Seahorse analysis. Moreover, lysosomal distribution study and western blotting showed that mTORC1 signaling, a central regulator of cellular metabolism, was inhibited upon nanoplastic exposure, likely serving as the link between lysosome dysfunction and metabolic defects. Taken together, our findings systematically mapped the key molecular changes induced by PSNPs in human cells and provide comprehensive biological insights for the risk estimation of NPLs contamination.

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