Xu Weiran, Geng Fei, Zhang Kaihui, Wang Yinhuan
School of Basic Medicine Sciences, North China University of Science and Technology, Tangshan, China.
Department of Minimally Invasive Spine Surgery, Tianjin Hospital, Tianjin University, Tianjin, China.
Orthop Surg. 2025 Aug 25. doi: 10.1111/os.70150.
Intervertebral disc degeneration (IVDD) has been closely associated with ferroptosis in nucleus pulposus cells (NPCs), the underlying regulatory mechanisms and therapeutic strategies remain poorly defined. This study aims to delineate how ginsenoside Rg3 mitigates IVDD progression through ferroptosis suppression, providing a basis for clinical translation.
An erastin-induced nucleus pulposus cell ferroptosis model was established. Suitable Erastin concentrations (0-20 μM) were screened via CCK-8, qRT-PCR, and Western blotting based on viability, extracellular matrix (COL2A1/ACAN/ADAMTS5/MMP3) and ferroptosis markers (GPX4/FTH-1/ACSL4), followed by determination of optimal Rg3 concentrations (0-150 μM) using identical methods. Key targets of Rg3 were predicted through network pharmacology and verified by qRT-PCR and Western blotting. After establishing a rat tail puncture-induced IVDD model, local injection of Rg3 was administered. Therapeutic efficacy was evaluated by MRI assessment of nucleus pulposus status and disc height, alongside histological and immunohistochemical analyses of Rg3's role in delaying disc degeneration.
5 μM Erastin effectively induced ferroptosis in nucleus pulposus cells, reducing cell viability, suppressing expression of extracellular matrix anabolic proteins (COL2A1, ACAN), while promoting catabolic factors (MMP3, ADAMTS5) and downregulating ferroptosis inhibitors (GPX4, FTH-1). These alterations were significantly reversed by 100 μM Rg3. Integrated network pharmacology and molecular biological validation identified PRKAA2 as the key target mediating Rg3's anti-degenerative effects. In vivo rat experiments demonstrated that Rg3 treatment preserved disc height and attenuated disc degeneration, with histological and immunohistochemical analyses further confirming its therapeutic efficacy and PRKAA2-targeted regulation.
This study elucidates the therapeutic mechanism of Rg3 in delaying IVDD progression via PRKAA2-mediated ferroptosis inhibition, providing substantial experimental evidence for its clinical translation as a potential disease-modifying agent.
椎间盘退变(IVDD)与髓核细胞(NPCs)的铁死亡密切相关,但其潜在的调控机制和治疗策略仍不清楚。本研究旨在阐明人参皂苷Rg3如何通过抑制铁死亡来减轻IVDD进展,为临床转化提供依据。
建立了erastin诱导的髓核细胞铁死亡模型。基于细胞活力、细胞外基质(COL2A1/ACAN/ADAMTS5/MMP3)和铁死亡标志物(GPX4/FTH-1/ACSL4),通过CCK-8、qRT-PCR和蛋白质印迹法筛选合适的erastin浓度(0-20μM),然后使用相同方法确定最佳Rg3浓度(0-150μM)。通过网络药理学预测Rg3的关键靶点,并通过qRT-PCR和蛋白质印迹法进行验证。在建立大鼠尾部穿刺诱导的IVDD模型后,进行Rg3局部注射。通过MRI评估髓核状态和椎间盘高度来评估治疗效果,并通过组织学和免疫组织化学分析Rg3在延缓椎间盘退变中的作用。
5μM erastin可有效诱导髓核细胞铁死亡,降低细胞活力,抑制细胞外基质合成蛋白(COL2A1、ACAN)的表达,同时促进分解代谢因子(MMP3、ADAMTS5)并下调铁死亡抑制剂(GPX4、FTH-1)。100μM Rg3可显著逆转这些变化。综合网络药理学和分子生物学验证确定PRKAA2是介导Rg3抗退变作用的关键靶点。体内大鼠实验表明,Rg3治疗可保持椎间盘高度并减轻椎间盘退变,组织学和免疫组织化学分析进一步证实了其治疗效果和PRKAA2靶向调节作用。
本研究阐明了Rg3通过PRKAA2介导的铁死亡抑制作用延缓IVDD进展的治疗机制,为其作为潜在疾病修饰剂的临床转化提供了大量实验证据。
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