Elisabeth A. Lemmon , Kevin G. Burt , Sung Yeon Kim , Bryan Kwok , Lorielle Laforest , Rui Xiao , Lin Han , Carla R. Scanzello , Robert L. Mauck , Kimberly A. Agnello
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Additional samples (n = 5/group) were subjected to RNA-sequencing to define the transcriptional response to injury. Finally, synovial tissue samples from injured animals (n = 6 (IL1) or n = 8 (IL6)/group) were assessed in vitro for response to therapeutic molecules directed against interleukin (IL) signaling (IL1 or IL6).</p></div><div><h3>Results</h3><p>Cruciate injury resulted in increased synovial fibrosis, vascularity, inflammatory cell infiltration, and intimal hyperplasia. Additionally, the stiffness of both the intima and subintima regions were higher in diseased compared to healthy tissue. Differential gene expression analysis showed that diseased synovium had an upregulation of immune response and cell adhesion pathways and a downregulation of Rho protein transduction pathways. In vitro application of small molecule therapeutics targeting IL1 (anakinra) or IL6 (tocilizumab) dampened expression of inflammatory and matrix deposition mediators.</p></div><div><h3>Conclusion</h3><p>Spontaneous cruciate ligament injury in canines is associated with synovial inflammation and fibrosis in a relevant model for testing emerging intra-articular treatments. Small molecule therapeutics targeting IL pathways may be ideal interventions for delivery to the joint space after injury.</p></div>","PeriodicalId":19654,"journal":{"name":"Osteoarthritis and Cartilage","volume":"32 10","pages":"Pages 1295-1307"},"PeriodicalIF":7.2000,"publicationDate":"2024-07-14","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Interleukin receptor therapeutics attenuate inflammation in canine synovium following cruciate ligament injury\",\"authors\":\"Elisabeth A. Lemmon , Kevin G. 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引用次数: 0
摘要
目的:膝关节韧带损伤后的滑膜纤维化与渐进性关节疼痛和僵硬有关。本研究旨在评估犬自然发生十字韧带损伤后滑膜结构、机械性能和转录特征的变化,并测试针对滑膜炎症和纤维化驱动因素的潜在疗法:设计:通过组织学(n=10/组)和微机械测试(n=5/组)评估犬自发性十字韧带撕裂的滑膜和健康膝关节的滑膜,以确定组织结构和硬度的变化。对其他样本(5 个/组)进行 RNA 测序,以确定转录对损伤的反应。最后,对受伤动物的滑膜组织样本(n=6(IL1)或n=8(IL6)/组)进行体外评估,以确定其对针对白细胞介素(IL)信号传导的治疗分子(IL1或IL6)的反应:结果:十字韧带损伤导致滑膜纤维化、血管扩张、炎性细胞浸润和内膜增生加剧。此外,与健康组织相比,病变组织内膜和内膜下区域的硬度更高。差异基因表达分析表明,病变滑膜的免疫反应和细胞粘附通路上调,Rho蛋白转导通路下调。体外应用靶向IL1(anakinra)或IL6(tocilizumab)的小分子疗法抑制了炎症和基质沉积介质的表达:结论:犬自发性十字韧带损伤与滑膜炎症和纤维化有关,是测试新出现的关节内治疗方法的相关模型。针对 IL 通路的小分子疗法可能是损伤后向关节间隙输送药物的理想干预措施。
Interleukin receptor therapeutics attenuate inflammation in canine synovium following cruciate ligament injury
Objective
In the knee, synovial fibrosis after ligamentous injury is linked to progressive joint pain and stiffness. The objective of this study was to evaluate changes in synovial architecture, mechanical properties, and transcriptional profiles following naturally occurring cruciate ligament injury in canines and to test potential therapeutics that target drivers of synovial inflammation and fibrosis.
Design
Synovia from canines with spontaneous cruciate ligament tears and from healthy knees were assessed via histology (n = 10/group) and micromechanical testing (n = 5/group) to identify changes in tissue architecture and stiffness. Additional samples (n = 5/group) were subjected to RNA-sequencing to define the transcriptional response to injury. Finally, synovial tissue samples from injured animals (n = 6 (IL1) or n = 8 (IL6)/group) were assessed in vitro for response to therapeutic molecules directed against interleukin (IL) signaling (IL1 or IL6).
Results
Cruciate injury resulted in increased synovial fibrosis, vascularity, inflammatory cell infiltration, and intimal hyperplasia. Additionally, the stiffness of both the intima and subintima regions were higher in diseased compared to healthy tissue. Differential gene expression analysis showed that diseased synovium had an upregulation of immune response and cell adhesion pathways and a downregulation of Rho protein transduction pathways. In vitro application of small molecule therapeutics targeting IL1 (anakinra) or IL6 (tocilizumab) dampened expression of inflammatory and matrix deposition mediators.
Conclusion
Spontaneous cruciate ligament injury in canines is associated with synovial inflammation and fibrosis in a relevant model for testing emerging intra-articular treatments. Small molecule therapeutics targeting IL pathways may be ideal interventions for delivery to the joint space after injury.
期刊介绍:
Osteoarthritis and Cartilage is the official journal of the Osteoarthritis Research Society International.
It is an international, multidisciplinary journal that disseminates information for the many kinds of specialists and practitioners concerned with osteoarthritis.