Wnt16 protects chondrocytes from lumbar facet joint osteoarthritis through the Wnt/β-catenin pathway in low back pain patients.

IF 1.3 4区 医学 Q4 NEUROSCIENCES Somatosensory and Motor Research Pub Date : 2021-12-01 Epub Date: 2021-09-23 DOI:10.1080/08990220.2021.1977267
Chunshuai Wu, Jinjuan Yu, Guanhua Xu, Guofeng Bao, Jinlong Zhang, Pengfei Xue, Jiawei Jiang, Jiajia Chen, Chu Chen, Hongxiang Hong, Zhiming Cui
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引用次数: 3

Abstract

Purpose: Low back pain (LBP) is a long-lasting and chronic symptom without any exact cause. This study attempts to propose a new staging system based on the original grading system combined with pathological results and clinical symptoms to better clarify the dynamic evolution of LBP related to cartilage degeneration during facet joint osteoarthritis (FJOA). To explore a potential target for diagnosis, treatment, and drug intervention of facet joint osteoarthritis related LBP via protecting chondrocytes.

Materials and methods: All the facet joints were divided into 4 groups according to our new degenerative staging system based on Weishaupt grade, CT and MRI. Collect the facet joint samples from patients whom suffered lumbar fusion surgery for lumbar disc herniation. Molecular biology experiments were used to explore the effect of Wnt16 on the degeneration of facet joints. Micro-CT examination and pain stimulation test checked the biological function of Wnt16 in rats.

Results: Wnt16 was significantly increased and more aggregated in the facet joint chondrocytes in the Phase III and Phase IV, which is consistent with the pathological findings of cartilage degeneration (OARSI). We found that Wnt16 participated in the regulation of FJOA via Wnt/β-catenin pathway in vitro, which was inhibited by specific inhibitor DKK1. The rats, rich expressed Wnt16, showed higher paw withdrawal thresholds and prolonged paw withdrawal latency to FJOA related LBP. Micro-CT examination for the lumbar spine of rats showed Wnt16 protected the chondrocytes from FJOA.

Conclusions: This study defined a new staging system for LBP related cartilage degeneration of facet joint based on the original grading system combined with pathological results and clinical symptoms. Wnt16 is expected to be a potential target for treatment of FJOA via protecting chondrocytes.

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腰痛患者的Wnt16通过Wnt/β-catenin通路保护腰椎小关节骨性关节炎的软骨细胞。
目的:腰痛(LBP)是一种没有确切原因的长期慢性症状。本研究试图在原有分级体系的基础上,结合病理结果和临床症状,提出一种新的分级体系,以更好地阐明小关节骨关节炎(facet joint osteoarthritis, FJOA)中与软骨退变相关的腰痛的动态演变。通过保护软骨细胞,探索小关节骨性关节炎相关腰痛的诊断、治疗和药物干预的潜在靶点。材料和方法:所有关节突关节按照我们新的基于Weishaupt分级、CT和MRI的退行性分期系统分为4组。收集腰椎融合术治疗腰椎间盘突出症患者的关节突关节标本。通过分子生物学实验探讨Wnt16在关节突关节退变中的作用。显微ct检查和疼痛刺激试验检测Wnt16在大鼠体内的生物学功能。结果:在III期和IV期,Wnt16在小关节软骨细胞中明显升高,且更多聚集,这与软骨退变(OARSI)的病理表现一致。我们发现Wnt16在体外通过Wnt/β-catenin通路参与FJOA的调控,该通路被特异性抑制剂DKK1抑制。富表达Wnt16的大鼠对FJOA相关的LBP表现出更高的足部戒断阈值和更长的足部戒断潜伏期。大鼠腰椎显微ct检查显示Wnt16对FJOA软骨细胞有保护作用。结论:本研究在原有分级体系的基础上,结合病理结果和临床症状,定义了一种新的小关节腰痛相关软骨退变分期体系。Wnt16有望成为通过保护软骨细胞治疗FJOA的潜在靶点。
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来源期刊
Somatosensory and Motor Research
Somatosensory and Motor Research 医学-神经科学
自引率
0.00%
发文量
4
审稿时长
>12 weeks
期刊介绍: Somatosensory & Motor Research publishes original, high-quality papers that encompass the entire range of investigations related to the neural bases for somatic sensation, somatic motor function, somatic motor integration, and modeling thereof. Comprising anatomical, physiological, biochemical, pharmacological, behavioural, and psychophysical studies, Somatosensory & Motor Research covers all facets of the peripheral and central processes underlying cutaneous sensation, and includes studies relating to afferent and efferent mechanisms of deep structures (e.g., viscera, muscle). Studies of motor systems at all levels of the neuraxis are covered, but reports restricted to non-neural aspects of muscle generally would belong in other journals.
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