Cultivation of auricular chondrocytes in poly(ethylene glycol)/poly(ε-caprolactone) hydrogel for tracheal cartilage tissue engineering in a rabbit model.

IF 3.2 3区 医学 Q3 CELL & TISSUE ENGINEERING European cells & materials Pub Date : 2018-06-21 DOI:10.22203/eCM.v035a24
C S Chang, C Y Yang, H Y Hsiao, L Chen, I M Chu, M H Cheng, C H Tsao
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引用次数: 16

Abstract

Tissue engineering has the potential to overcome the limitations of tracheal reconstruction. To tissue-engineer a tracheal cartilage, auricular chondrocytes were encapsulated in a photocurable poly(ethylene glycol)/poly(ε-caprolactone) (PEG/PCL) hydrogel. Chondrogenic genes, including Sox9, Acan and Col2a1, were up-regulated in auricular chondrocytes after 2 weeks of in vitro cultivation in the PEG/PCL hydrogel. Co-cultivation of 70 % auricular chondrocytes and 30 % bone marrow mesenchymal stem cells (BMSCs) accelerated the chondrogenic genes' expression in the PEG/PCL hydrogel. Cartilaginous matrix markers, including proteoglycans and collagen type II, were detected in the chondrocytes-encapsulated PEG/PCL hydrogel after 4 weeks of in vitro cultivation. The higher expression level of cartilaginous matrix markers was observed in the PEG/PCL hydrogel with co-cultivation of 70 % chondrocytes and 30 % BMSCs. After 4 weeks of ectopic cultivation in rabbits, the cylindrical PEG/PCL structure was sustained with the use of a luminal silicon stent. However, without the stent, the construct collapsed under a compression force. No fibrosis or vessel ingrowth were found in the PEG/PCL hydrogel after 4 weeks of ectopic cultivation, whereas the auricular chondrocytes showed proteoglycans' accumulation and collagen type II production. Rabbit auricular chondrocytes could survive and retain chondrogenic ability in the PEG/PCL hydrogel under both in vitro and in vivo conditions. While the PEG/PCL hydrogel did not show sufficient mechanical properties for supporting the cylindrical shape of the construct, the high chondrogenesis level of chondrocytes in the PEG/PCL hydrogel displayed the potential of this material for tracheal tissue engineering.

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聚乙二醇/聚ε-己内酯水凝胶培养兔气管软骨组织工程模型耳廓软骨细胞。
组织工程有潜力克服气管重建的局限性。为了组织工程气管软骨,耳廓软骨细胞被包裹在光固化聚乙二醇/聚ε-己内酯(PEG/PCL)水凝胶中。在PEG/PCL水凝胶中体外培养2周后,耳廓软骨细胞中的Sox9、Acan和Col2a1等成软骨基因表达上调。70%耳廓软骨细胞与30%骨髓间充质干细胞(BMSCs)共同培养可促进成软骨基因在PEG/PCL水凝胶中的表达。体外培养4周后,在软骨细胞包膜的PEG/PCL水凝胶中检测到软骨基质标志物,包括蛋白聚糖和II型胶原。在70%软骨细胞和30%骨髓间充质干细胞共培养的PEG/PCL水凝胶中,软骨基质标志物的表达水平较高。兔异位培养4周后,使用腔内硅支架维持圆柱形PEG/PCL结构。然而,没有支架,结构在压缩力下坍塌。异位培养4周后,PEG/PCL水凝胶未见纤维化或血管长入,耳软骨细胞出现蛋白聚糖积累和II型胶原生成。体外和体内条件下,兔耳软骨细胞在PEG/PCL水凝胶中均能存活并保持成软骨能力。虽然PEG/PCL水凝胶没有表现出足够的力学性能来支持圆柱形结构,但PEG/PCL水凝胶中软骨细胞的高软骨形成水平显示了这种材料在气管组织工程中的潜力。
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来源期刊
European cells & materials
European cells & materials 生物-材料科学:生物材料
CiteScore
6.00
自引率
6.50%
发文量
55
审稿时长
1.5 months
期刊介绍: eCM provides an interdisciplinary forum for publication of preclinical research in the musculoskeletal field (Trauma, Maxillofacial (including dental), Spine and Orthopaedics). The clinical relevance of the work must be briefly mentioned within the abstract, and in more detail in the paper. Poor abstracts which do not concisely cover the paper contents will not be sent for review. Incremental steps in research will not be entertained by eCM journal.Cross-disciplinary papers that go across our scope areas are welcomed.
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