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去细胞气管细胞外基质支持上皮细胞迁移、分化及功能。

Decellularized tracheal extracellular matrix supports epithelial migration, differentiation, and function.

作者信息

Kutten Johannes C, McGovern David, Hobson Christopher M, Luffy Sarah A, Nieponice Alejandro, Tobita Kimimasa, Francis Richard J, Reynolds Susan D, Isenberg Jeffrey S, Gilbert Thomas W

机构信息

1 Vascular Medicine Institute , Pittsburgh, Pennsylvania.

出版信息

Tissue Eng Part A. 2015 Jan;21(1-2):75-84. doi: 10.1089/ten.TEA.2014.0089. Epub 2014 Sep 12.

Abstract

Tracheal loss is a source of significant morbidity for affected patients with no acceptable solution. Interest in engineering tracheal transplants has created a demand for small animal models of orthotopic tracheal transplantation. Here, we examine the use of a decellularized graft in a murine model of tracheal replacement. Fresh or decellularized tracheas harvested from age-matched female donor C57BL/6 mice were transplanted into syngeneic recipients. Tracheas were decellularized using repeated washes of water, 3% Triton X-100, and 3 M NaCl under cyclic pressure changes, followed by disinfection with 0.1% peracetic acid/4% ethanol, and terminal sterilization by gamma irradiation. Tracheas were explanted for immunolabeling at 1, 4, and 8 weeks following surgery. Video microscopy and computed tomography were performed to assess function and structure. Decellularized grafts supported complete reepithelialization by 8 weeks and motile cilia were observed. Cartilaginous portions of the trachea were maintained in mice receiving fresh transplants, but repopulation of the cartilage was not seen in mice receiving decellularized transplants. We observed superior postsurgical survival, weight gain, and ciliary function in mice receiving fresh transplants compared with those receiving decellularized transplants. The murine orthotopic tracheal transplant provides an appropriate model to assess the repopulation and functional regeneration of decellularized tracheal grafts.

摘要

气管缺失对于受影响的患者来说是严重发病的一个来源,且尚无可接受的解决方案。对工程化气管移植的兴趣引发了对原位气管移植小动物模型的需求。在此,我们研究了脱细胞移植物在小鼠气管置换模型中的应用。从年龄匹配的雌性供体C57BL/6小鼠获取的新鲜或脱细胞气管被移植到同基因受体中。气管通过在循环压力变化下用去离子水、3% Triton X - 100和3 M NaCl反复冲洗进行脱细胞处理,随后用0.1%过氧乙酸/4%乙醇进行消毒,并通过伽马射线进行最终灭菌。在手术后1、4和8周取出气管进行免疫标记。进行视频显微镜检查和计算机断层扫描以评估功能和结构。脱细胞移植物在8周时支持完全重新上皮化,并且观察到了活动的纤毛。接受新鲜移植的小鼠气管的软骨部分得以保留,但接受脱细胞移植的小鼠未见到软骨的再填充。与接受脱细胞移植的小鼠相比,我们观察到接受新鲜移植的小鼠术后存活率更高、体重增加更多且纤毛功能更好。小鼠原位气管移植为评估脱细胞气管移植物的再填充和功能再生提供了一个合适的模型。

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