二苯甲酮-3通过调节软骨细胞衰老驱动骨关节炎发病。

IF 5.4 2区医学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY

Chemico-Biological Interactions Pub Date : 2025-09-30 DOI:10.1016/j.cbi.2025.111757

Zhenyu Zhu , Chunyan Wang , Shasha Wei , Runtao Wu , Wenxia Zhao , Xinyuan Zhao , Yingjun Li , Ye Yang

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引用次数: 0

摘要

二苯甲酮-3 （BP-3）是一种广泛使用的紫外线吸收剂，其潜在的健康风险日益受到人们的关注。最近的流行病学研究已经确定了BP-3暴露与骨关节炎（OA）患病率之间的联系，但其在OA发病机制中的具体作用仍不完全清楚。本研究表明，BP-3长期暴露可诱导大鼠oa样关节软骨变性，表现为结构紊乱、蛋白聚糖耗竭和细胞外基质（ECM）稳态严重失调，这可以通过基质金属蛋白酶（MMPs）上调和II型胶原蛋白（Col2a1）下调来证明。值得注意的是，在人C28/I2软骨细胞中，BP-3显著破坏ECM平衡，表现为MMPs增加和Col2a1含量降低，这与体内研究结果一致。在机制上，转录组分析发现BP-3暴露组中与衰老相关的基因表达改变。随后的实验证实，BP-3诱导软骨细胞衰老，表现为衰老相关β-半乳糖苷酶（SA-β-gal）活性升高，p16、p21和p53水平上调。随后的细胞转录组学进一步揭示了BP-3暴露后丝裂原活化蛋白激酶（MAPK）信号通路的显著变化。至关重要的是，在软骨细胞中，BP-3暴露选择性地激活了ERK1/2通路，而不是MAPK级联中的p38或JNK通路。进一步研究证实BP-3通过双重ERK依赖机制驱动p21转录：p53 Ser15位点磷酸化和下游ERK效应因子ets样转录因子1 （Elk-1）的磷酸化/核易位。引人注目的是，ERK特异性抑制剂PD98059有效地阻断了bp -3诱导的ERK活化、Elk-1磷酸化、软骨细胞衰老和ECM降解。总的来说，这些发现建立了BP-3作为环境骨关节炎危害的新机制，其中BP-3通过特异性激活ERK通路触发软骨细胞衰老并促进OA发病。

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Benzophenone-3 drives osteoarthritis pathogenesis by regulating chondrocyte senescence

Benzophenone-3 (BP-3), a widely used UV absorber, is of increasing concern due to its potential health risks. Recent epidemiological studies have identified a link between BP-3 exposure and osteoarthritis (OA) prevalence, yet its specific role in OA pathogenesis remains incompletely understood. This study reveals that prolonged BP-3 exposure induces OA-like articular cartilage degeneration in rats, marked by structural disorganization, proteoglycan depletion, and critical dysregulation of extracellular matrix (ECM) homeostasis evidenced by up-regulated matrix metalloproteinases (MMPs) and down-regulated type II collagen (Col2a1). Notably, in human C28/I2 chondrocytes, BP-3 significantly disrupted ECM balance evidenced by increased MMPs and decreased Col2a1 content, which corroborates in vivo findings. Mechanistically, transcriptome analysis identified altered expression of genes associated with senescence in BP-3 exposure groups. Subsequent experiments confirmed that BP-3 induced chondrocyte senescence evidenced by elevated Senescence-Associated β-Galactosidase (SA-β-gal) activity and up-regulated p16, p21, and p53. Subsequent cellular transcriptomics further revealed significant changes in Mitogen-activated protein kinase (MAPK) signaling pathways following BP-3 exposure. Crucially, in chondrocytes, BP-3 exposure selectively activated ERK1/2 pathway but not p38 or JNK pathways within the MAPK cascade. Further investigation established that BP-3 drove p21 transcription via dual ERK-dependent mechanism: p53 phosphorylation at Ser15 and phosphorylation/nuclear translocation of the downstream ERK effector Ets-like transcription factor 1 (Elk-1). Strikingly, the ERK-specific inhibitor PD98059 effectively blocked BP-3-induced ERK activation, Elk-1 phosphorylation, chondrocyte senescence, and ECM degradation. Collectively, these findings establish a novel mechanism for BP-3 as an environmental osteoarthritic hazard, in which it triggers chondrocyte senescence and promotes OA pathogenesis through the specific activation of the ERK pathway.

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来源期刊

Chemico-Biological Interactions 生物-毒理学

CiteScore

7.70

自引率

3.90%

发文量

410

审稿时长

36 days

期刊介绍： Chemico-Biological Interactions publishes research reports and review articles that examine the molecular, cellular, and/or biochemical basis of toxicologically relevant outcomes. Special emphasis is placed on toxicological mechanisms associated with interactions between chemicals and biological systems. Outcomes may include all traditional endpoints caused by synthetic or naturally occurring chemicals, both in vivo and in vitro. Endpoints of interest include, but are not limited to carcinogenesis, mutagenesis, respiratory toxicology, neurotoxicology, reproductive and developmental toxicology, and immunotoxicology.