maresin 1-LGR6轴可减轻小鼠前交叉韧带横断后的炎症反应和创伤后骨关节炎。
Maresin 1-LGR6 axis mitigates inflammation and posttraumatic osteoarthritis after transection of the anterior cruciate ligament in mice.
作者信息
Leite Chilan B G, Fricke Hannah P, Tavares Luciana P, Nshimiyimana Robert, Mekhail Julie, Kilgallen Elliott, Killick Felix, Whalen Janey D, Lehoczky Jessica A, Serhan Charles N, Charles Julia F, Lattermann Christian
机构信息
Department of Orthopedic Surgery, Brigham and Women's Hospital, Harvard Medical School, Boston, MA, USA.
Division of Pulmonary and Critical Care Medicine, Department of Medicine, Brigham and Women's Hospital, Harvard Medical School, Boston, MA, USA.
出版信息
Osteoarthritis Cartilage. 2025 Jul;33(7):861-873. doi: 10.1016/j.joca.2025.03.005. Epub 2025 Mar 24.
OBJECTIVE
Anterior cruciate ligament (ACL) tears frequently cause chronic inflammation and posttraumatic osteoarthritis (PTOA), with therapies failing to resolve persistent post-injury inflammation. Specialized pro-resolving mediators (SPMs), including Maresin1 (MaR1), show promise in resolving inflammation and promoting tissue repair. However, their role in PTOA remains underexplored. This study investigated inflammatory markers and MaR1 dynamics post-ACL injury, the role of the MaR1 receptor Leucine-rich Repeat-containing G protein-coupled receptor 6 (LGR6) in PTOA, and MaR1's therapeutic potential in a mouse ACL transection (ACLT) model.
DESIGN
Eight-week-old C57BL6/J male mice underwent ACLT, and synovial fluid, periarticular tissue, and tibiofemoral joints were collected at various time points post-surgery for analysis. LGR6-deficient mice were utilized to investigate the role of MaR1 signaling in inflammation resolution. Additionally, the effect of intraarticular MaR1 administration on PTOA progression was assessed.
RESULTS
ACLT induced joint inflammation with leukocyte infiltration and elevated pro-inflammatory cytokines. MaR1 levels peaked early post-injury and were associated with a six-fold increase in LGR6 expression. LGR6 deficiency worsened inflammation and PTOA severity with higher histological Osteoarthritis Research Society International (OARSI) scores (mean difference 5.6[95%CI: 2.5-8.6], p<0.001) and microCT OA severity scores (mean difference 4.3[95%CI: 0.7-7.9], p=0.018). Intraarticular MaR1 treatment reduced leukocyte recruitment, suppressed pro-inflammatory gene expression, and ameliorated PTOA development, improving histological OARSI scores (mean difference -3.9[95%CI: -6.9 to -1.0], p=0.012) and microCT scores (mean difference -6.7[95%CI: -10.3 to -3.0], p=0.012).
CONCLUSION
This study suggests a critical role of MaR1 in resolving inflammation post-ACL injury and mitigating PTOA in mice. Targeting SPM pathways, particularly MaR1 and/or MaR1 mimetics, offers a promising strategy to prevent chronic joint inflammation and degeneration after ACL injury.
目的
前交叉韧带(ACL)撕裂常导致慢性炎症和创伤后骨关节炎(PTOA),现有治疗方法无法解决损伤后持续存在的炎症。包括玛瑞辛1(MaR1)在内的特异性促消退介质(SPM)在解决炎症和促进组织修复方面显示出前景。然而,它们在PTOA中的作用仍未得到充分研究。本研究调查了ACL损伤后炎症标志物和MaR1的动态变化、MaR1受体富含亮氨酸重复序列的G蛋白偶联受体6(LGR6)在PTOA中的作用,以及MaR1在小鼠ACL横断(ACLT)模型中的治疗潜力。
设计
8周龄C57BL6/J雄性小鼠接受ACLT手术,在术后不同时间点收集滑液、关节周围组织和胫股关节进行分析。利用LGR6基因缺陷小鼠研究MaR1信号在炎症消退中的作用。此外,评估关节内注射MaR1对PTOA进展的影响。
结果
ACLT诱导关节炎症,伴有白细胞浸润和促炎细胞因子升高。MaR1水平在损伤后早期达到峰值,并与LGR6表达增加6倍相关。LGR6缺陷使炎症和PTOA严重程度恶化,组织学国际骨关节炎研究学会(OARSI)评分更高(平均差异5.6[95%CI:2.5 - 8.6],p<0.001),微CT骨关节炎严重程度评分更高(平均差异4.3[95%CI:0.7 - 7.9],p = 0.018)。关节内注射MaR1治疗减少了白细胞募集,抑制了促炎基因表达,并改善了PTOA的发展,提高了组织学OARSI评分(平均差异 - 3.9[95%CI: - 6.9至 - 1.0],p = 0.012)和微CT评分(平均差异 - 6.7[95%CI: - 10.3至 - 3.0],p = 0.012)。
结论
本研究表明MaR1在解决ACL损伤后的炎症和减轻小鼠PTOA方面起关键作用。靶向SPM途径,特别是MaR1和/或MaR1模拟物,为预防ACL损伤后慢性关节炎症和退变提供了一种有前景的策略。
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