Nrf2介导的生精细胞铁凋亡参与了聚苯乙烯纳米塑料对小鼠雄性生殖毒性的诱导。

Xufeng Fu, Hang Han, Hong Yang, Bo Xu, Wenjie Dai, Ling Liu, Tiantian He, Xing Du, Xiuying Pei
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摘要

由于大量的塑料垃圾和一次性口罩,微塑料(MPs)和纳米塑料(NPs)已成为有害物质,但它们对健康的具体影响仍不确定。本研究将荧光标记的聚苯乙烯 NPs(PS-NPs)注入小鼠的循环系统,以确定 NPs 在体内的分布和潜在毒性效应。有趣的是,全身成像发现 PS-NPs 在小鼠睾丸中聚集。因此,研究人员探讨了 PS-NPs 对雄性小鼠生殖系统和精母细胞系的毒性作用及其机制。口服 PS-NPs 后,小鼠的精子发生受到影响,生精细胞受损。将精母细胞系 GC-2 暴露于 PS-NPs 后,利用 RNA 测序(RNA-seq)分析其毒性机制;发现暴露于 PS-NPs 后存在铁突变途径。研究还发现核因子红细胞2相关因子2(Nrf2)在PS-NPs诱导的生精细胞铁突变中发挥了重要作用。最后,在体内证实了 Nrf2 的这一机制在 PS-NPs 诱导的男性生殖毒性中发挥了保护作用。本研究证明,PS-NPs通过引起依赖于Nrf2的生精细胞铁凋亡而诱导小鼠雄性生殖功能障碍。
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Nrf2-mediated ferroptosis of spermatogenic cells involved in male reproductive toxicity induced by polystyrene nanoplastics in mice.
Microplastics (MPs) and nanoplastics (NPs) have become hazardous materials due to the massive amount of plastic waste and disposable masks, but their specific health effects remain uncertain. In this study, fluorescence-labeled polystyrene NPs (PS-NPs) were injected into the circulatory systems of mice to determine the distribution and potential toxic effects of NPs in vivo. Interestingly, whole-body imaging found that PS-NPs accumulated in the testes of mice. Therefore, the toxic effects of PS-NPs on the reproduction systems and the spermatocytes cell line of male mice, and their mechanisms, were investigated. After oral exposure to PS-NPs, their spermatogenesis was affected and the spermatogenic cells were damaged. The spermatocyte cell line GC-2 was exposed to PS-NPs and analyzed using RNA sequencing (RNA-seq) to determine the toxic mechanisms; a ferroptosis pathway was found after PS-NP exposure. The phenomena and indicators of ferroptosis were then determined and verified by ferroptosis inhibitor ferrostatin-1 (Fer-1), and it was also found that nuclear factor erythroid 2-related factor 2 (Nrf2) played an important role in spermatogenic cell ferroptosis induced by PS-NPs. Finally, it was confirmed in vivo that this mechanism of Nrf2 played a protective role in PS-NPs-induced male reproductive toxicity. This study demonstrated that PS-NPs induce male reproductive dysfunction in mice by causing spermatogenic cell ferroptosis dependent on Nrf2.
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