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聚苯乙烯纳米塑料通过激活自噬作用,抑制滋养层细胞迁移/侵袭和迁移小体形成,从而导致流产。

Polystyrene Nanoplastics Activate Autophagy and Suppress Trophoblast Cell Migration/Invasion and Migrasome Formation to Induce Miscarriage.

机构信息

Research Center for Environment and Female Reproductive Health, the Eighth Affiliated Hospital, Sun Yat-sen University, Shenzhen 518033, China.

Key Laboratory of Environment and Female Reproductive Health, West China School of Public Health & West China Fourth Hospital, Sichuan University, Chengdu 610041, China.

出版信息

ACS Nano. 2024 Jan 30;18(4):3733-3751. doi: 10.1021/acsnano.3c11734. Epub 2024 Jan 22.

Abstract

Nanoplastics (NPs), as emerging pollutants, have attracted global attention. Nevertheless, the adverse effects of NPs on female reproductive health, especially unexplained miscarriage, are poorly understood. Defects of trophoblast cell migration and invasion are associated with miscarriage. Migrasomes were identified as cellular organelles with largely unidentified functions. Whether NPs might affect migration, invasion, and migrasome formation and induce miscarriage has been completely unexplored. In this study, we selected polystyrene nanoplastics (PS-NPs, 50 nm) as a model of plastic particles and treated human trophoblast cells and pregnant mice with PS-NPs at doses near the actual environmental exposure doses of plastic particles in humans. We found that exposure to PS-NPs induced a pregnant mouse miscarriage. PS-NPs suppressed ROCK1-mediated migration/invasion and migrasome formation. SOX2 was identified as the transcription factor of ROCK1. PS-NPs activated autophagy and promoted the autophagy degradation of SOX2, thus suppressing SOX2-mediated ROCK1 transcription. Supplementing with murine SOX2 or ROCK1 could efficiently rescue migration/invasion and migrasome formation and alleviate miscarriage. Analysis of the protein levels of SOX2, ROCK1, TSPAN4, NDST1, P62, and LC-3BII/I in PS-NP-exposed trophoblast cells, villous tissues of unexplained miscarriage patients, and placental tissues of PS-NP-exposed mice gave consistent results. Collectively, this study revealed the reproductive toxicity of nanoplastics and their potential regulatory mechanism, indicating that NP exposure is a risk factor for female reproductive health.

摘要

纳米塑料(NPs)作为新兴污染物,引起了全球关注。然而,NPs 对女性生殖健康的不良影响,尤其是不明原因流产,尚不清楚。滋养层细胞迁移和侵袭缺陷与流产有关。迁移小体被认为是具有广泛未知功能的细胞细胞器。NPs 是否可能影响迁移、侵袭和迁移小体形成并导致流产,这一点尚未得到充分探索。在这项研究中,我们选择聚苯乙烯纳米塑料(PS-NPs,50nm)作为塑料颗粒的模型,用 PS-NPs 处理人滋养层细胞和怀孕小鼠,剂量接近人类实际环境中塑料颗粒的暴露剂量。我们发现,暴露于 PS-NPs 会导致怀孕小鼠流产。PS-NPs 抑制了 ROCK1 介导的迁移/侵袭和迁移小体形成。SOX2 被鉴定为 ROCK1 的转录因子。PS-NPs 激活自噬,并促进 SOX2 的自噬降解,从而抑制 SOX2 介导的 ROCK1 转录。补充鼠 SOX2 或 ROCK1 可以有效地挽救迁移/侵袭和迁移小体形成,并减轻流产。对 PS-NP 暴露的滋养层细胞、不明原因流产患者的绒毛组织和 PS-NP 暴露小鼠的胎盘组织中 SOX2、ROCK1、TSPAN4、NDST1、P62 和 LC-3BII/I 的蛋白质水平进行分析,结果一致。总之,这项研究揭示了纳米塑料的生殖毒性及其潜在的调节机制,表明 NP 暴露是女性生殖健康的一个风险因素。

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