生长因子独立1通过MAPK信号通路失活抑制软骨细胞铁下垂改善骨关节炎

IF 5.9 1区医学 Q1 ORTHOPEDICS

Journal of Orthopaedic Translation Pub Date : 2025-07-29 DOI:10.1016/j.jot.2025.07.003

Xiaoyu Jin , Xunhao Wang , Siyu Xu , Nuo Xu , Ziwei Wang , Chunqing Hu , Wei Liu , Zhaofeng Zhang , Xiyu Liu , Jingjing Fan , Ruiyang Jiang , Rui Wu , Zhongyang Lv , Dongquan Shi

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引用次数: 0

摘要

骨关节炎（OA）是最常见的退行性关节疾病，以软骨退化为特征，与软骨细胞铁下垂密切相关。本研究旨在探讨生长因子独立1 （growth factor independence 1, Gfi1）基因在软骨细胞铁下垂中的作用及机制，以期为骨性关节炎提供新的治疗靶点。方法分析人、小鼠OA软骨和过氧化氢叔丁基（TBHP）诱导的原代软骨细胞中嗜铁标记物和Gfi1的表达。利用小干扰RNA或过表达质粒敲低或过表达Gfi1，探讨其在软骨细胞铁凋亡和代谢中的作用。然后，在关节内注射过表达Gfi1的腺相关病毒（AAV-Gfi1）或不注射Gfi1的情况下，研究Gfi1在内侧半月板（DMM）手术诱导的小鼠OA模型失稳中的作用。此外，我们通过RNA测序分析揭示了Gfi1在软骨细胞铁下垂中发挥作用的关键下游途径。结果在人和DMM手术诱导的小鼠OA软骨损伤中，Gfi1的表达显著降低，而典型脂质过氧化产物4-HNE的表达显著升高。与此一致的是，Gfi1在tbhp诱导的嗜铁软骨细胞中显著下调。此外，Gfi1敲低通过提高总ROS、脂质ROS和Fe2+积累等铁致下沉标志物水平加重了软骨细胞铁致下沉。在tbhp诱导的软骨细胞中，通过敲低Gfi1，还观察到铁致凋亡驱动因子（Cox2, Acsl4）和分解代谢标志物（Mmp13）的上调，铁致凋亡抑制因子（Gpx4, Fth1, Slc7a11）和合成代谢标志物（Col II）的下调。相反，Gfi1过表达在tbhp诱导的软骨细胞中表现出抗铁的作用。关节内注射AAV-Gfi1通过抵抗铁下垂和保持OA软骨合成代谢-分解代谢平衡，明显减轻软骨退变。软骨下骨硬化、骨赘形成、滑膜炎和行为表现的综合评估进一步验证了Gfi1过表达改善OA进展。从机制上看，MAPK信号通路被认为是Gfi1在OA中发挥抗铁稳定性作用的关键下游介质。结论在骨性关节炎中，ongfi1表达下调，其过表达通过抑制MAPK信号通路抑制软骨细胞铁下垂而改善骨性关节炎的进展。本研究确定了Gfi1作为软骨退变治疗抗铁下垂的新靶点，为临床优化OA治疗策略提供了更多线索。

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Growth factor independence 1 ameliorates osteoarthritis by inhibiting chondrocyte ferroptosis via inactivation of MAPK signaling pathway

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Growth factor independence 1 ameliorates osteoarthritis by inhibiting chondrocyte ferroptosis via inactivation of MAPK signaling pathway

Background

Osteoarthritis (OA) is the most common degenerative joint disease, characterized by cartilage deterioration, which is closely associated with chondrocyte ferroptosis. The aim of this study was to investigate the role and mechanism of previously unexplored gene, growth factor independence 1 (Gfi1) in chondrocyte ferroptosis, in order to provide a new therapeutic target for OA.

Methods

The expression of ferroptotic hallmarks and Gfi1 were analyzed in human and mice OA cartilages and tert-butyl hydroperoxide (TBHP)-induced primary chondrocytes. Small interfering RNA or overexpression plasmids were used to knock down or overexpress Gfi1 to explore its role in chondrocyte ferroptosis and metabolism. Then, the role of Gfi1 in destabilization of medial meniscus (DMM) surgery-induced mice OA model was investigated with or without the intra-articular injection of adeno-associated virus-overexpressing Gfi1 (AAV-Gfi1). Furthermore, RNA sequencing analysis was performed to reveal the key downstream pathway of Gfi1 exerting its role in chondrocyte ferroptosis.

Results

The expression of Gfi1 was significantly decreased, while 4-HNE, a typical lipid peroxidation product, was significantly increased both in damaged human and DMM surgery-induced mice OA cartilages. Consistently, Gfi1 was remarkably downregulated in TBHP-induced ferroptotic chondrocytes. Moreover, Gfi1 knockdown aggravated chondrocyte ferroptosis by elevated levels of ferroptotic hallmarks, including total ROS, lipid ROS and Fe²⁺ accumulation. The upregulation of ferroptotic driver (Cox2, Acsl4) and catabolic marker (Mmp13) and downregulation of ferroptotic suppressors (Gpx4, Fth1, Slc7a11) and anabolic marker (Col II) were also observed in TBHP-induced chondrocytes by Gfi1 knockdown. On the contrary, Gfi1 overexpression showed anti-ferroptotic effect in TBHP-induced chondrocytes. Intra-articular injection of AAV-Gfi1 evidently alleviated cartilage degeneration by resisting ferroptosis and preserving the anabolism-catabolism homeostasis in OA cartilages. Comprehensive evaluation of subchondral bone sclerosis, osteophyte formation, synovitis and behavior performance further validated that Gfi1 overexpression ameliorated OA progression. Mechanistically, MAPK signaling pathway was identified as the key downstream mediator of Gfi1 exerting anti-ferroptotic role in OA.

Conclusion

Gfi1 is downregulated in OA and its overexpression ameliorates OA progression by inhibiting chondrocyte ferroptosis via inactivation of MAPK signaling pathway.

The translational potential of this article

This study identifies Gfi1 as a novel therapeutic anti-ferroptotic target for cartilage degeneration, providing more clues for optimizing OA treatment strategies in clinical practice.

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来源期刊

Journal of Orthopaedic Translation Medicine-Orthopedics and Sports Medicine

CiteScore

11.80

自引率

13.60%

发文量

审稿时长

29 days

期刊介绍： The Journal of Orthopaedic Translation (JOT) is the official peer-reviewed, open access journal of the Chinese Speaking Orthopaedic Society (CSOS) and the International Chinese Musculoskeletal Research Society (ICMRS). It is published quarterly, in January, April, July and October, by Elsevier.