Li Lexiang, Zhu Jun, Chen Yi, Li Haobo, Han Yaguang, Zhang Lei, Wang Bo
Department of Joint Surgery and Orthopedic Medicine, Shanghai Changzheng Hospital (The Second Affiliated Hospital of Naval Medical University), Shanghai, China.
J Gene Med. 2025 Jan;27(1):e70005. doi: 10.1002/jgm.70005.
Osteoarthritis (OA) is characterized by progressive cartilage degeneration mediated by various molecular pathways, including inflammatory and autophagic processes. SET domain-containing lysine methyltransferase 7 (SETD7), a methyltransferase, has been implicated in OA pathology. This study investigates the expression pattern of SETD7 in OA and its role in promoting interleukin-1 beta (IL-1β)-induced chondrocyte injury through modulation of autophagy and inflammation.
The expression of SETD7 in cartilage tissues from OA patients and healthy controls was quantified using quantitative reverse transcription PCR and Western blot analysis. Small interfering RNA targeting SETD7 (si-SETD7) was transfected into human articular chondrocytes (HACs) treated with IL-1β to examine its impact on cellular viability, apoptosis, inflammatory responses, and autophagy. Functional assays including Cell Counting Kit-8, flow cytometry, enzyme-linked immunosorbent assay, and commercial kits were employed to assess biochemical changes. Interaction between YTH N6-methyladenosine RNA binding protein 2 (YTHDF2) and SETD7 was explored using RNA immunoprecipitation and co-immunoprecipitation assays.
SETD7 was overexpressed in OA cartilage compared with controls and increased further upon IL-1β treatment. Knockdown of SETD7 in IL-1β-treated HACs improved cellular viability, decreased apoptosis, and reversed the adverse effects on lactate dehydrogenase release and inflammatory markers (tumor necrosis factor-alpha and interleukin-6) while enhancing antioxidant enzymes (catalase, malondialdehyde, and superoxide dismutase). Additionally, autophagy was restored, as evidenced by changes in the levels of autophagy related 5, Beclin1, and sequestosome 1. Interfering with autophagy using chloroquine negated the protective effects of SETD7 knockdown. Furthermore, YTHDF2 was found to stabilize SETD7 mRNA, influencing its expression and enhancing IL-1β-induced chondrocyte injury.
SETD7 plays a critical role in the pathogenesis of OA by modulating chondrocyte survival, apoptosis, inflammation, and autophagy. The interaction between YTHDF2 and SETD7 exacerbates chondrocyte injury under inflammatory conditions, highlighting potential therapeutic targets for OA treatment. The YTHDF2/SETD7 axis offers a novel insight into the molecular mechanisms governing cartilage degeneration in OA.
骨关节炎(OA)的特征是由多种分子途径介导的进行性软骨退变,包括炎症和自噬过程。含SET结构域的赖氨酸甲基转移酶7(SETD7)作为一种甲基转移酶,与OA病理过程有关。本研究调查了SETD7在OA中的表达模式及其通过调节自噬和炎症促进白细胞介素-1β(IL-1β)诱导的软骨细胞损伤中的作用。
使用定量逆转录PCR和蛋白质免疫印迹分析对OA患者和健康对照者软骨组织中SETD7的表达进行定量。将靶向SETD7的小干扰RNA(si-SETD7)转染到用IL-1β处理的人关节软骨细胞(HACs)中,以检查其对细胞活力、凋亡、炎症反应和自噬的影响。采用包括细胞计数试剂盒-8、流式细胞术、酶联免疫吸附测定和商业试剂盒在内的功能测定法来评估生化变化。使用RNA免疫沉淀和免疫共沉淀测定法探索YTH N6-甲基腺苷RNA结合蛋白2(YTHDF2)与SETD7之间的相互作用。
与对照组相比,SETD7在OA软骨中过表达,并且在IL-1β处理后进一步增加。在IL-1β处理的HACs中敲低SETD7可提高细胞活力,减少凋亡,并逆转对乳酸脱氢酶释放和炎症标志物(肿瘤坏死因子-α和白细胞介素-6)的不利影响,同时增强抗氧化酶(过氧化氢酶、丙二醛和超氧化物歧化酶)。此外,自噬得以恢复,这通过自噬相关5、Beclin1和聚集体蛋白1水平的变化得以证明。使用氯喹干扰自噬可消除SETD7敲低的保护作用。此外,发现YTHDF2可稳定SETD7 mRNA,影响其表达并增强IL-1β诱导的软骨细胞损伤。
SETD7通过调节软骨细胞存活、凋亡、炎症和自噬在OA发病机制中起关键作用。YTHDF2与SETD7之间的相互作用在炎症条件下加剧软骨细胞损伤,突出了OA治疗的潜在靶点。YTHDF2/SETD7轴为OA中软骨退变的分子机制提供了新的见解。
