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用于膝关节和颞下颌关节移植的全猪半月板的可行玻璃体移植物。

Viable Vitreous Grafts of Whole Porcine Menisci for Transplant in the Knee and Temporomandibular Joints.

机构信息

Department of Bioengineering, Clemson University, Clemson, SC, 29634, USA.

Department of Oral Health Sciences, Medical University of South Carolina, Charleston, SC, 29425, USA.

出版信息

Adv Healthc Mater. 2024 Sep;13(22):e2303706. doi: 10.1002/adhm.202303706. Epub 2024 Apr 2.

Abstract

The shortage of suitable donor meniscus grafts from the knee and temporomandibular joint (TMJ) impedes treatments for millions of patients. Vitrification offers a promising solution by transitioning these tissues into a vitreous state at cryogenic temperatures, protecting them from ice crystal damage using high concentrations of cryoprotectant agents (CPAs). However, vitrification's success is hindered for larger tissues (>3 mL) due to challenges in CPA penetration. Dense avascular meniscus tissues require extended CPA exposure for adequate penetration; however, prolonged exposure becomes cytotoxic. Balancing penetration and reducing cell toxicity is required. To overcome this hurdle, a simulation-based optimization approach is developed by combining computational modeling with microcomputed tomography (µCT) imaging to predict 3D CPA distributions within tissues over time accurately. This approach minimizes CPA exposure time, resulting in 85% viability in 4-mL meniscal specimens, 70% in 10-mL whole knee menisci, and 85% in 15-mL whole TMJ menisci (i.e., TMJ disc) post-vitrification, outperforming slow-freezing methods (20%-40%), in a pig model. The extracellular matrix (ECM) structure and biomechanical strength of vitreous tissues remain largely intact. Vitreous meniscus grafts demonstrate clinical-level viability (≥70%), closely resembling the material properties of native tissues, with long-term availability for transplantation. The enhanced vitrification technology opens new possibilities for other avascular grafts.

摘要

膝关节和颞下颌关节(TMJ)合适供体半月板移植物的短缺阻碍了数百万患者的治疗。玻璃化提供了一个有前途的解决方案,通过将这些组织在低温下转变为玻璃体状态,使用高浓度的冷冻保护剂(CPAs)来防止冰晶损伤。然而,由于较大组织(>3 毫升)中 CPAs 渗透的挑战,玻璃化的成功受到阻碍。致密的无血管半月板组织需要延长 CPA 暴露时间以充分渗透;然而,长时间暴露会产生细胞毒性。需要平衡渗透和降低细胞毒性。为了克服这一障碍,通过将计算建模与微计算机断层扫描(µCT)成像相结合,开发了一种基于模拟的优化方法,以准确预测组织中 3D CPA 分布随时间的变化。该方法最大限度地减少了 CPA 的暴露时间,结果表明,在玻璃化后,4 毫升半月板标本的存活率为 85%,10 毫升全膝半月板的存活率为 70%,15 毫升全 TMJ 半月板(即 TMJ 盘)的存活率为 85%,优于慢冻法(20%-40%),在猪模型中。玻璃化组织的细胞外基质(ECM)结构和生物力学强度基本保持完整。玻璃化半月板移植物具有临床水平的存活率(≥70%),与天然组织的材料特性非常相似,具有长期移植可用性。增强的玻璃化技术为其他无血管移植物开辟了新的可能性。

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