Chondroitin sulfate A-selenium nanoparticles protect chondrocytes from T-2 toxin-induced oxidative stress and mitochondrial dysfunction through activating autophagy by the SIRT1-AMPK-FOXO3 pathway

IF 6.1 2区环境科学与生态学 Q1 ENVIRONMENTAL SCIENCES

Ecotoxicology and Environmental Safety Pub Date : 2025-08-04 DOI:10.1016/j.ecoenv.2025.118797

Huan Deng , Jinyan Lin , Yude Jiang , Abebe Feyissa Amhare , Lichun Qiao , Jun Wang , Jing Han

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引用次数: 0

Abstract

T-2 toxin is known to cause tissue and cellular damage, with chondrocytes being particularly vulnerable. In contrast, chondroitin sulfate A-selenium nanoparticles (CSA-SeNP) have shown cartilage-protective properties, although the precise molecular mechanism remains incompletely elucidated. This study used T-2 toxin and CSA-SeNP to treat human C28/I2 chondrocytes, and studied their effects on SIRT1-AMPK-FOXO3 pathway and oxidative damage, mitochondrial dysfunction, impaired autophagy, and apoptosis. Autophagy was evaluated by acridine orange (AO) and dansylcadaverine (MDC) staining, transmission electron microscopy observation, and mRFP-GFP-LC3 adenovirus. Oxidative stress (ROS, MDA, SOD, CAT, T-AOC) and mitochondrial function (ATP, SDH, ATPases, membrane potential) were assessed. Western blotting analyzed the expression level of the SIRT1-AMPK-FOXO3 pathway, autophagy markers, and apoptosis. We found that 4-hour exposure to 5 and 20 ng/mL, as well as 12-hour exposure to 5 ng/mL of T-2 toxin, activated the SIRT1-AMPK-FOXO3 pathway compensatively, inducing autophagy but inhibiting degradation of autolysosome, leading to oxidative damage, mitochondrial dysfunction, and increased apoptosis. 12-hour exposure to 20 ng/mL T-2 toxin inhibited this pathway and autophagy, causing serious damage to chondrocytes. CSA-SeNP alleviated the inhibition of the SIRT1-AMPK-FOXO3 pathway induced by T-2 toxin, reducing oxidative damage, mitochondrial dysfunction and apoptosis, thereby restoring autophagy to protect chondrocytes. In summary, T-2 toxin's effects on chondrocyte autophagy were dose- and time-dependent. CSA-SeNP protected against T-2 toxin by activating the SIRT1-AMPK-FOXO3 pathway, suggesting its potential for chondrocyte protection. This study may provide new insights into the development of T-2 toxin detoxification strategies and the method for prevention and treatment of chondrocyte damage.

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硫酸软骨素a -硒纳米颗粒通过SIRT1-AMPK-FOXO3途径激活自噬，保护软骨细胞免受T-2毒素诱导的氧化应激和线粒体功能障碍

已知T-2毒素会导致组织和细胞损伤，软骨细胞尤其脆弱。相比之下，硫酸软骨素a -硒纳米颗粒（CSA-SeNP）显示出软骨保护特性，尽管其精确的分子机制尚未完全阐明。本研究采用T-2毒素和CSA-SeNP处理人C28/I2软骨细胞，研究其对SIRT1-AMPK-FOXO3通路及氧化损伤、线粒体功能障碍、自噬受损和凋亡的影响。采用吖啶橙（AO）和丹西尸碱（MDC）染色、透射电镜观察和mRFP-GFP-LC3腺病毒检测自噬情况。评估氧化应激（ROS、MDA、SOD、CAT、T-AOC）和线粒体功能（ATP、SDH、ATPases、膜电位）。Western blotting分析SIRT1-AMPK-FOXO3通路、自噬标志物和凋亡的表达水平。我们发现，暴露于5和20 ng/mL 4小时以及暴露于5 ng/mL的T-2毒素12小时可代偿激活SIRT1-AMPK-FOXO3途径，诱导自噬，但抑制自噬酶体的降解，导致氧化损伤、线粒体功能障碍和细胞凋亡增加。暴露于20 ng/mL的T-2毒素中12小时可抑制该途径和自噬，导致软骨细胞严重损伤。CSA-SeNP可减轻T-2毒素对SIRT1-AMPK-FOXO3通路的抑制，减轻氧化损伤、线粒体功能障碍和细胞凋亡，从而恢复自噬，保护软骨细胞。总之，T-2毒素对软骨细胞自噬的影响是剂量和时间依赖性的。CSA-SeNP通过激活SIRT1-AMPK-FOXO3通路保护T-2毒素，提示其潜在的软骨细胞保护作用。该研究可能为T-2毒素解毒策略的发展以及预防和治疗软骨细胞损伤的方法提供新的见解。

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来源期刊

Ecotoxicology and Environmental Safety 环境科学-毒理学

CiteScore

12.10

自引率

5.90%

发文量

1234

审稿时长

88 days

期刊介绍： Ecotoxicology and Environmental Safety is a multi-disciplinary journal that focuses on understanding the exposure and effects of environmental contamination on organisms including human health. The scope of the journal covers three main themes. The topics within these themes, indicated below, include (but are not limited to) the following: Ecotoxicology、Environmental Chemistry、Environmental Safety etc.