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Morphological and biomechanical effects of annulus fibrosus injury and repair in an ovine cervical model

机译:羊颈椎纤维环损伤和修复的形态学和生物力学效应

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摘要

Tissue engineering repair of annulus fibrosus (AF) defects has the potential to prevent disability and pain from intervertebral disc (IVD) herniation and its progression to degeneration. Clinical translation of AF repair methods requires assessment in long‐term large animal models. An ovine AF injury model was developed using cervical spinal levels and a biopsy‐type AF defect to assess composite tissue engineering repair in 1‐month and 12‐month studies. The repair used a fibrin hydrogel crosslinked with genipin (FibGen) to seal defects, poly(trimethylene carbonate) (PTMC) scaffolds to replace lost AF tissue, and polyurethane membranes to prevent herniation. In the 1‐month study, PTMC scaffolds sealed with FibGen herniated with polyurethane membranes. When applied alone, FibGen integrated with the surrounding AF tissue without herniation, showing promise for long‐term studies. The 12‐month long‐term study used only FibGen which showed fibrous healing, biomaterial resorption and no obvious hydrogel‐related complications. However, the 2 mm biopsy punch injury condition also exhibited fibrotic healing at 12 months. Both untreated and FibGen treated groups showed equivalency with no detectable differences in histological grades of proteoglycans, cellular morphology, IVD structure and blood vessel formation, biomechanical properties including torque range and axial range of motion, Pfirrmann grade, IVD height, and quantitative scores of vertebral body changes from clinical computed tomography. The biopsy‐type injury caused endplate defects with a high prevalence of osteophytes in all groups and no nucleus herniation, indicating that the biopsy‐type injury requires further refinement, such as reduction to a slit‐type defect that could penetrate the full depth of the AF without damaging the endplate. Results demonstrate translational feasibility of FibGen for AF repair to seal AF defects, although future study with a more refined injury model is required to validate the efficacy of FibGen before translation.
机译:纤维环(AF)缺陷的组织工程修复具有预防椎间盘(IVD)椎间盘突出症并发展为变性的残疾和疼痛的潜力。 AF修复方法的临床翻译需要在长期大型动物模型中进行评估。在1个月和12个月的研究中,使用颈椎脊柱水平和活检类型的AF缺损建立了绵羊AF损伤模型,以评估复合组织工程修复。修复过程使用纤维蛋白水凝胶与Genipin(FibGen)交联来密封缺损,使用聚碳酸三亚甲基酯(PTMC)支架代替丢失的AF组织,并使用聚氨酯膜来防止疝。在为期1个月的研究中,用FibGen密封的PTMC支架与聚氨酯膜一起突出。当单独使用时,FibGen可以与周围的房颤组织融合而不会产生疝气,这表明它可以进行长期研究。这项为期12个月的长期研究仅使用了FibGen,其显示出纤维愈合,生物材料吸收并且没有明显的水凝胶相关并发症。然而,2毫米活检穿孔器损伤情况在12个月时也表现出纤维化愈合。未治疗组和FibGen治疗组均显示相同,蛋白聚糖的组织学等级,细胞形态,IVD结构和血管形成,生物力学特性(包括扭矩范围和轴向运动范围,Pfirrmann等级,IVD高度以及椎骨的定量评分)均无可检测的差异。从临床计算机断层扫描可以发现身体的变化。活检类型的损伤导致终板缺损,所有组中骨赘的患病率很高,且无核突出。这表明活检类型的损伤需要进一步完善,例如减少至可穿透组织的整个深度的狭缝型缺陷。自动对焦不会损坏端板。结果证明了FibGen用于AF修复以密封AF缺陷的翻译可行性,尽管还需要进一步研究以更精确的损伤模型来验证FibGen在翻译前的功效。

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