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微粉化脱水人羊膜/绒毛膜的关节腔内递送可减轻创伤后骨关节炎发病后的退行性改变。

Intra-articular delivery of micronized dehydrated human amnion/chorion membrane reduces degenerative changes after onset of post-traumatic osteoarthritis.

作者信息

Lin Angela S P, Reece David S, Thote Tanushree, Sridaran Sanjay, Stevens Hazel Y, Willett Nick J, Guldberg Robert E

机构信息

Phil and Penny Knight Campus for Accelerating Scientific Impact, University of Oregon, Eugene, OR, United States.

Wallace H. Coulter Department of Biomedical Engineering, Parker H. Petit Institute for Bioengineering and Bioscience, Georgia Institute of Technology, Atlanta, GA, United States.

出版信息

Front Bioeng Biotechnol. 2023 Sep 6;11:1224141. doi: 10.3389/fbioe.2023.1224141. eCollection 2023.

Abstract

Micronized dehydrated human amnion/chorion membrane (mdHACM) has reduced short term post-traumatic osteoarthritis (PTOA) progression in rats when delivered 24 h after medial meniscal transection (MMT) and is being investigated for clinical use as a disease modifying therapy. Much remains to be assessed, including its potential for longer-term therapeutic benefit and treatment effects after onset of joint degeneration. Characterize longer-term effects of acute treatment with mdHACM and determine whether treatment administered to joints with established PTOA could slow or reverse degeneration. Hypotheses: Acute treatment effects will be sustained for 6 weeks, and delivery of mdHACM after onset of joint degeneration will attenuate structural osteoarthritic changes. Rats underwent MMT or sham surgery (left leg). mdHACM was delivered intra-articularly 24 h or 3 weeks post-surgery ( = 5-7 per group). Six weeks post-surgery, animals were euthanized and left tibiae scanned using equilibrium partitioning of an ionic contrast agent microcomputed tomography (EPIC-µCT) to structurally quantify joint degeneration. Histology was performed to examine tibial plateau cartilage. Quantitative 3D µCT showed that cartilage structural metrics (thickness, X-ray attenuation, surface roughness, exposed bone area) for delayed mdHACM treatment limbs were significantly improved over saline treatment and not significantly different from shams. Subchondral bone mineral density and thickness for the delayed treatment group were significantly improved over acute treated, and subchondral bone thickness was not significantly different from sham. Marginal osteophyte degenerative changes were decreased with delayed mdHACM treatment compared to saline. Acute treatment (24 h post-surgery) did not reduce longer-term joint tissue degeneration compared to saline. Histology supported µCT findings and further revealed that while delayed treatment reduced cartilage damage, chondrocytes displayed qualitatively different morphologies and density compared to sham. This study provides insight into effects of intra-articular delivery timing relative to PTOA progression and the duration of therapeutic benefit of mdHACM. Results suggest that mdHACM injection into already osteoarthritic joints can improve joint health, but a single, acute mdHACM injection post-injury does not prevent long term osteoarthritis associated with meniscal instability. Further work is needed to fully characterize the durability of therapeutic benefit in stable osteoarthritic joints and the effects of repeated injections.

摘要

微粉化脱水人羊膜/绒毛膜(mdHACM)在内侧半月板横断(MMT)后24小时给药时,可减缓大鼠创伤后骨关节炎(PTOA)的短期进展,目前正作为一种疾病改善疗法进行临床研究。仍有许多方面有待评估,包括其长期治疗益处的潜力以及关节退变发生后的治疗效果。 表征mdHACM急性治疗的长期效果,并确定对已发生PTOA的关节进行治疗是否可以减缓或逆转退变。假设:急性治疗效果将持续6周,并且在关节退变发生后给予mdHACM将减轻结构性骨关节炎变化。 大鼠接受MMT或假手术(左腿)。在手术后24小时或3周关节腔内给予mdHACM(每组=5-7只)。手术后6周,对动物实施安乐死,并使用离子造影剂微计算机断层扫描(EPIC-µCT)的平衡分配法对左胫骨进行扫描,以从结构上量化关节退变。进行组织学检查以观察胫骨平台软骨。 定量三维µCT显示,延迟给予mdHACM治疗的肢体的软骨结构指标(厚度、X射线衰减、表面粗糙度、暴露骨面积)相对于生理盐水治疗有显著改善,且与假手术组无显著差异。延迟治疗组的软骨下骨矿物质密度和厚度相对于急性治疗组有显著改善,且软骨下骨厚度与假手术组无显著差异。与生理盐水相比,延迟给予mdHACM治疗可减少边缘骨赘退变变化。与生理盐水相比,急性治疗(手术后24小时)并未减少长期关节组织退变。组织学支持µCT结果,并进一步显示,虽然延迟治疗减少了软骨损伤,但与假手术组相比,软骨细胞的形态和密度在质量上有所不同。 本研究深入探讨了关节内给药时间相对于PTOA进展的影响以及mdHACM的治疗益处持续时间。结果表明,向已患骨关节炎的关节注射mdHACM可改善关节健康,但损伤后单次急性注射mdHACM并不能预防与半月板不稳定相关的长期骨关节炎。需要进一步开展工作以全面表征在稳定的骨关节炎关节中治疗益处的持久性以及重复注射的效果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/35cd/10512062/2408573fe6f2/fbioe-11-1224141-g001.jpg

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