感觉神经EP4通过调节血管生成耦联的骨形成促进异位骨化。
Sensory nerve EP4 facilitates heterotopic ossification by regulating angiogenesis-coupled bone formation.
作者信息
Lin Rongmin, Lin Hancheng, Zhu Chencheng, Zeng Jieming, Hou Jiahui, Xu Ting, Tan Yihui, Zhou Xuyou, Ma Yuan, Yang Mankai, Wei Kuanhai, Yu Bin, Wu Hangtian, Cui Zhuang
机构信息
Department of Orthopaedics and Traumatology, Nanfang Hospital, Southern Medical University, Guangzhou, Guangdong, 510515, China.
Key laboratory of bone and cartilage regeneration medicine, Southern Medical University, Guangzhou, Guangdong, 510515, China.
出版信息
J Orthop Translat. 2024 Nov 5;49:325-338. doi: 10.1016/j.jot.2024.09.005. eCollection 2024 Nov.
OBJECTIVE
Heterotopic ossification (HO) refers to the abnormal development of bone in soft tissue rather than within bone itself. Previous research has shown that sensory nerve prostaglandin E2 receptor 4 (EP4) signaling not only governs pain perception but also influences bone formation. However, the relationship between sensory nerve EP4 and the pathogenesis of HO in the Achilles tendon remains unclear. This study aims to investigate this relationship and the underlying mechanisms.
METHODS
We generated sensory nerve EP4-specific knockout mice, with the genotype of Avil-CreEP4, was propagated. Transcriptome sequencing and bioinformatics analysis techniques were used to identify the potential molecular pathways involving with sensory nerve EP4. Additionally, a neurectomy mouse model was created by transecting the sciatic nerve transection, to examine the effects and mechanisms of peripheral innervation on HO in vivo. Micro-CT, immunofluorescence (IF), Hematoxylin and Eosin (H&E) Staining, Safranin O-Fast Green staining and western blotting were used to analyze changes in cellular and tissue components.
RESULTS
We here observed an increase in sensory nerve EP4 and H-type vessels during the pathogenesis of HO in both human subjects and mice. Proximal neurectomy through sciatic nerve transection or the targeted knockout of EP4 in sensory nerves hindered angiogenesis-dependent bone formation and the development of HO at the traumatic site of the Achilles tendon. Furthermore, we identified the Efnb2 (Ephrin-B2)/Dll4 (Delta-like ligand 4) axis as a potential downstream element influenced by sensory nerve EP4 in the regulation of HO. Notably, administration of an EP4 inhibitor demonstrated the ability to alleviate HO. Based on these findings, sensory nerve EP4 emerges as an innovative and promising approach for managing HO.
CONCLUSION
Our findings demonstrate that the sensory nerve EP4 promotes ectopic bone formation by modulating angiogenesis-associated osteogenesis during HO.
THE TRANSLATIONAL POTENTIAL OF THIS ARTICLE
Our results provide a mechanistic rationale for targeting sensory nerve EP4 as a promising candidate for HO therapy.
目的
异位骨化(HO)是指在软组织而非骨组织本身中出现的异常骨发育。先前的研究表明,感觉神经前列腺素E2受体4(EP4)信号传导不仅控制疼痛感知,还影响骨形成。然而,感觉神经EP4与跟腱HO发病机制之间的关系仍不清楚。本研究旨在探讨这种关系及其潜在机制。
方法
我们培育了感觉神经EP4特异性敲除小鼠,其基因型为Avil-CreEP4。采用转录组测序和生物信息学分析技术来确定与感觉神经EP4相关的潜在分子途径。此外,通过切断坐骨神经创建神经切除术小鼠模型,以研究外周神经支配对体内HO的影响及机制。使用显微CT、免疫荧光(IF)、苏木精和伊红(H&E)染色、番红O-固绿染色和蛋白质印迹法来分析细胞和组织成分的变化。
结果
我们在此观察到,在人类受试者和小鼠的HO发病过程中,感觉神经EP4和H型血管均增加。通过坐骨神经切断进行近端神经切除术或感觉神经中EP4的靶向敲除,阻碍了依赖血管生成的骨形成以及跟腱创伤部位HO的发展。此外,我们确定Efnb2(Ephrin-B2)/Dll4(Delta样配体4)轴是感觉神经EP4在HO调节中影响的潜在下游元件。值得注意的是,给予EP4抑制剂显示出减轻HO的能力。基于这些发现,感觉神经EP4成为治疗HO的一种创新且有前景的方法。
结论
我们的研究结果表明,感觉神经EP4在HO过程中通过调节与血管生成相关的成骨作用促进异位骨形成。
本文的转化潜力
我们的结果为将感觉神经EP4作为HO治疗的有前景候选靶点提供了机制依据。
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