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From cradle to grave: Deciphering sex-specific disruptions of the nervous and reproductive systems through interactions of 4-methylbenzylidene camphor and nanoplastics in adult zebrafish

Journal of Hazardous Materials 2024 26 citations ? Citation count from OpenAlex, updated daily. May differ slightly from the publisher's own count. Score: 65 ? 0–100 AI score estimating relevance to the microplastics field. Papers below 30 are filtered from public browse.
Hongyi Xian, Hongyi Xian, Zhiming Li, Ruobing Bai, Rongyi Ye, Yu Feng, Yu Feng, Yizhou Zhong, Boxuan Liang, Yuji Huang, Yuji Huang, Jie Guo, Binjie Wang, Mingzhu Dai, Shuqin Tang, Xiaohu Ren, Xueping Chen, Da Chen, Xingfen Yang, Zhenlie Huang

Summary

Adult zebrafish exposed to a common sunscreen chemical (4-MBC) combined with nanoplastics showed significant damage to both their nervous and reproductive systems, with effects that differed between males and females. The nanoplastics acted as carriers that increased the accumulation of the sunscreen chemical in brain and reproductive tissues. These combined effects were passed to the next generation, raising concerns about how cosmetic chemicals and plastic pollution together may affect long-term reproductive health.

4-methylbenzylidene camphor (4-MBC) and micro/nanoplastics (MNPs) are common in personal care and cosmetic products (PCCPs) and consumer goods; however, they have become pervasive environmental contaminants. MNPs serve as carriers of 4-MBC in both PCCPs and the environment. Our previous study demonstrated that 4-MBC induces estrogenic effects in zebrafish larvae. However, knowledge gaps remain regarding the sex- and tissue-specific accumulation and potential toxicities of chronic coexposure to 4-MBC and MNPs. Herein, adult zebrafish were exposed to environmentally realistic concentrations of 4-MBC (0, 0.4832, and 4832 μg/L), with or without polystyrene nanoplastics (PS-NPs; 50 nm, 1.0 mg/L) for 21 days. Sex-specific accumulation was observed, with higher concentrations in female brains, while males exhibited comparable accumulation in the liver, testes, and brain. Coexposure to PS-NPs intensified the 4-MBC burden in all tested tissues. Dual-omics analysis (transcriptomics and proteomics) revealed dysfunctions in neuronal differentiation, death, and reproduction. 4-MBC-co-PS-NP exposure disrupted the brain histopathology more severely than exposure to 4-MBC alone, inducing sex-specific neurotoxicity and reproductive disruptions. Female zebrafish exhibited autism spectrum disorder-like behavior and disruption of vitellogenesis and oocyte maturation, while male zebrafish showed Parkinson's-like behavior and spermatogenesis disruption. Our findings highlight that PS-NPs enhance tissue accumulation of 4-MBC, leading to sex-specific impairments in the nervous and reproductive systems of zebrafish.

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