细胞因子受体样因子 1 (CRLF1) 在面关节骨关节炎发病机制中的作用。

Pengfei Xue , Huricha Jin , Xiaogang Zhou , Zhiming Cui , Daoran Cui
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引用次数: 0

摘要

背景:面关节骨关节炎(FJOA)是导致腰背痛的一种常见疾病,尤其是在老年人群中。本研究旨在探讨细胞因子受体样因子 1(CRLF1)在 FJOA 发病机制中的潜在作用及其治疗意义:方法:利用生物信息学分析确定 CRLF1 为靶基因,然后利用免疫组化技术(IHC)量化 CRLF1 的表达水平和关节退化程度。在原代软骨细胞中,用 siRNA 抑制 CRLF1 的表达,并进行 Western 印迹分析,以评估细胞外基质和 MAPK/ERK 信号通路的参与情况。流式细胞术用于评估软骨细胞的凋亡率,免疫荧光(IF)用于评估CRLF1、裂解-caspase3、MMP13、COL2A1和ERK的定位:结果:与正常组织相比,FJOA 组织中 CRLF1 的表达明显升高。通过功能缺失试验,确定 CRLF1 不仅能提高软骨细胞的凋亡率,还能促进体外细胞外基质的降解。此外,研究还发现 CRLF1 能激活 ERK1/2 通路。在软骨细胞中使用 MEK 抑制剂 U0126 可减轻 CRLF1 引发的促关节炎效应:这些结果表明,CRLF1 可促进 FJOA 中软骨细胞的凋亡和细胞外基质的降解,因此可能成为 FJOA 的潜在治疗靶点。
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The role of cytokine receptor-like factor 1 (CRLF1) in facet joint osteoarthritis pathogenesis

Background

Facet joint osteoarthritis (FJOA) is a prevalent condition contributing to low back pain, particularly in the elderly population. This study aimed to investigate the potential role of Cytokine Receptor-like Factor 1 (CRLF1) in FJOA pathogenesis and its therapeutic implications.

Methods

Bioinformatics analysis was utilized to identify CRLF1 as the target gene, followed by quantification of CRLF1 expression levels and joint degeneration degree using immunohistochemistry (IHC). In primary chondrocytes, the inhibition of CRLF1 expression by siRNA was performed, and Western blot analysis was conducted to evaluate the involvement of the extracellular matrix and MAPK/ERK signaling pathway. Flow cytometry was employed to assess the apoptosis rate of chondrocytes, while immunofluorescence (IF) was utilized to evaluate the localization of CRLF1, cleaved-caspase3, MMP13, COL2A1, and ERK.

Results

The expression of CRLF1 was found to be significantly elevated in FJOA tissues compared to normal tissues. Through the use of loss-of-function assays, it was determined that CRLF1 not only enhanced the rate of apoptosis in chondrocytes, but also facilitated the degradation of the extracellular matrix in vitro. Furthermore, CRLF1 was found to activate the ERK1/2 pathways. The pro-arthritic effects elicited by CRLF1 were mitigated by treatment with the MEK inhibitor U0126 in chondrocytes.

Conclusion

These results suggest that CRLF1 enhances chondrocytes apoptosis and extracellular matrix degration in FJOA and thus may therefore be a potential therapeutic target for FJOA.

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来源期刊
Experimental gerontology
Experimental gerontology Ageing, Biochemistry, Geriatrics and Gerontology
CiteScore
6.70
自引率
0.00%
发文量
0
审稿时长
66 days
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