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胶原酶处理软骨基质可促进相邻软骨融合。

Collagenase treatment of cartilaginous matrix promotes fusion of adjacent cartilage.

作者信息

Jiang Ching-Chuan, Hsieh Chang-Hsun, Liao Chun-Jen, Chang Wen-Hsiang, Liao Wei-Ju, Tsai-Wu Jyy-Jih, Chiang Hongsen

机构信息

Department of Orthopaedic Surgery, Fu Jen Catholic University Hospital, Taipei, Taiwan.

Department of Orthopaedic Surgery, National Taiwan University Hospital, Taipei, Taiwan.

出版信息

Regen Ther. 2020 Jul 28;15:97-102. doi: 10.1016/j.reth.2020.05.006. eCollection 2020 Dec.

Abstract

In articular cartilage-repair, grafts usually fuse unsatisfactorily with surrounding host cartilage. Enzymatic dissociation of cartilaginous matrix to free chondrocytes may benefit fusion. We tested such a hypothesis with human cartilage , and with porcine cartilage . Human articular cartilage was collected from knee surgeries, cut into disc-and-ring sets, and randomly distributed into three groups: disc-and-ring sets in Group 1 were left untreated; in Group 2 only discs, and in Group 3 both discs and rings were treated with enzyme. Each disc-and-ring reassembly was cultured in a perfusion system for 14 days; expression of cartilage marker proteins and genes was evaluated by immunohistochemistry and PCR. Porcine articular cartilage from knees was similarly fashioned into disc-and-ring combinations. Specimens were randomly distributed into a control group without further treatment, and an experimental group with both disc and ring treated with enzyme. Each disc-and-ring reassembly was transplanted into subcutaneous space of a nude mouse for 30 days, and retrieved to examine disc-ring interface. In study with human cartilage, a visible gap remained at disc-ring interfaces in Group 1, yet became indiscernible in Group 2 and 3. Marker genes, including type II collagen, aggrecan and Sox 9, were well expressed by chondrocytes in all specimens, indicating that chondrocytes' phenotype retained regardless of enzymatic treatment. Similar results were found in study with porcine cartilage. Enzymatic dissociation of cartilaginous matrix promotes fusion of adjacent cartilage. The clinical relevance may be a novel method to facilitate integration of repaired cartilage in joints.

摘要

在关节软骨修复中,移植物通常与周围宿主软骨融合不佳。将软骨基质酶解以释放软骨细胞可能有利于融合。我们用人软骨和猪软骨验证了这一假设。从膝关节手术中收集人关节软骨,切成圆盘 - 环组合,并随机分为三组:第1组的圆盘 - 环组合不做处理;第2组仅处理圆盘,第3组的圆盘和环均用酶处理。每个圆盘 - 环重新组装体在灌注系统中培养14天;通过免疫组织化学和PCR评估软骨标记蛋白和基因的表达。将来自猪膝关节的关节软骨同样制成圆盘 - 环组合。标本随机分为未经进一步处理的对照组和圆盘及环均用酶处理的实验组。每个圆盘 - 环重新组装体移植到裸鼠皮下空间30天,然后取出检查圆盘 - 环界面。在用人软骨进行的研究中,第1组的圆盘 - 环界面处仍可见间隙,但在第2组和第3组中变得难以分辨。包括II型胶原蛋白、聚集蛋白聚糖和Sox 9在内的标记基因在所有标本的软骨细胞中均有良好表达,表明无论酶处理如何,软骨细胞的表型得以保留。在猪软骨研究中也发现了类似结果。软骨基质的酶解促进相邻软骨的融合。其临床意义可能是一种促进关节中修复软骨整合的新方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2538/7770344/1227e1fa6ff6/gr1.jpg

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