细胞外基质同种异体移植对小鼠前十字韧带损伤后膝关节炎症的影响

Caroline Bice, Peyton Estes, Benjamin E. Loflin, Roufael Hanna, Stephen Schlecht
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摘要

背景与假设:一种人胎盘细胞外基质(ECM)同种异体移植物先前已被开发出来,生产商表示该产品可减轻组织炎症并加速修复。为了评估该产品对减少前交叉韧带(ACL)损伤后炎症的疗效,我们使用了一种新型小鼠体内前交叉韧带损伤模型。此前已有研究表明,该模型可在前交叉韧带损伤后两周内诱发明显的滑膜炎、髌下脂肪垫(IFP)纤维化和关节软骨(AC)退化。我们假设,在关节内注射同种异体移植物后,滑膜炎、纤维化和关节软骨退化会相应减轻。实验设计或项目方法:将十周大的 C57BL/6J 小鼠随机分为四组(n=10/组)。所有小鼠的右前交叉韧带均已断裂。一组为假对照组,在损伤后 24 小时进行单次关节内注射生理盐水。其余三组分别在损伤后 24 小时开始注射 1、2 和 6 次同种异体移植物。小鼠在受伤 14 天后安乐死。安乐死后,对IFP纤维化程度、膝关节滑膜炎和AC降解进行组织病理学评估。结果:到目前为止,每组分析了 5 只小鼠。在这些小鼠中,注射 6 次的小鼠滑膜炎评分(p < 0.01)明显高于假体组。1次注射组(p < 0.01)、2次注射组(p = 0.16)和6次注射组(p = 0.03)的IFP纤维化程度均高于假体组。各组间的交流变性无明显差异。结论和潜在影响:在对其余小鼠进行分析后,如果目前的结果成立,那么这种特殊的正生物制品可能不适合用于减少小鼠 ACL 损伤后的炎症反应。然而,这项试验性研究还存在一些局限性,首先需要考虑到这些局限性,以确认所发现的疗效不足。
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The Effects of Extracellular Matrix Allograft Administration on Knee Inflammation Following an Anterior Cruciate Ligament Injury in Mice
Background and Hypothesis:A human placental-derived extracellular matrix (ECM) allograft has previously been developed and is indicated by the manufacturer for reducing tissue inflammation and accelerated repair. To evaluate the efficacy of this product for reducing post-anterior cruciate ligament (ACL) injury inflammation, we used a novel murine in vivo ACL injury model. This model has previously been shown to induce significant synovitis, infrapatellar fat pad (IFP) fibrosis, and articular cartilage (AC) degradation within 2 weeks following an ACL injury. We hypothesized that intra-articular injections of the allograft would correspond with a decrease in synovitis, fibrosis, and articular cartilage degradation. Experimental Design or Project Methods:Ten-week-old C57BL/6J mice were randomly placed into 4 groups (n=10/group). For all mice, the right ACL was ruptured. One group served as sham controls, with a single intra-articular saline injection 24-hours following injury. The remaining three groups received 1, 2, and 6 allograft injections respectively beginning 24-hours after injury. Mice were euthanized 14 days after injury. Following euthanasia, the degree of IFP fibrosis, knee synovitis, and AC degradation were histopathologically evaluated. Results:Thus far, 5 mice per group have been analyzed. Within this subset of mice, those that received 6 injections demonstrated a significantly higher synovitis score (p < 0.01) than the sham group. The 1-injection (p < 0.01), 2-injection (p = 0.16), and 6-injection (p = 0.03) groups each displayed greater IFP fibrosis, relative to sham. No significant differences were found in AC degeneration across groups. Conclusion and Potential Impact:If the current results hold, following the analyses of the remaining mice, then this particular orthobiologic may not be suitable for reducing the post-ACL injury inflammatory response in mice. However, there are several limitations to this pilot study that will first need to be accounted for to confirm the lack of efficacy found.
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