Deconstructing Tissue Engineered Trachea: Assessing the Role of Synthetic Scaffolds, Segmental Replacement and Cell Seeding on Graft Performance

Sayali Dharmadhikari, Lumei Liu, K. Shontz, Matthew G. Wiet, A. White, A. Goins, Himani Akula, Jed Johnson, S. Reynolds, C. Breuer, Tendy Chiang
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引用次数: 25

Abstract

The ideal construct for tracheal replacement remains elusive in the management of long segment airway defects. Tissue engineered tracheal grafts (TETG) have been limited by the development of graft stenosis or collapse, infection, or lack of an epithelial lining. We applied a mouse model of orthotopic airway surgery to assess the impact of three critical barriers encountered in clinical applications: the scaffold, the extent of intervention, and the impact of cell seeding and characterized their impact on graft performance. First, synthetic tracheal scaffolds electrospun from polyethylene terephthalate / polyurethane (PET/PU) were orthotopically implanted in anterior tracheal defects of C57BL/6 mice. Scaffolds demonstrated complete coverage with ciliated respiratory epithelium by 2 weeks. Epithelial migration was accompanied by macrophage infiltration which persisted at long term (>6 weeks) time points. We then assessed the impact of segmental tracheal implantation using syngeneic trachea as a surrogate for the ideal tracheal replacement. Graft recovery involved local upregulation of epithelial progenitor populations and there was no evidence of graft stenosis or necrosis. Implantation of electrospun synthetic tracheal scaffold for segmental replacement resulted in respiratory distress and required euthanasia at an early time point. There was limited epithelial coverage of the scaffold with and without seeded bone marrow-derived mononuclear cells (BM-MNCs). We conclude that synthetic scaffolds support re-epithelialization in orthotopic patch implantation, syngeneic graft integration occurs with focal repair mechanisms, however epithelialization in segmental synthetic scaffolds is limited and is not influenced by cell seeding.
解构组织工程气管:评估合成支架、节段置换和细胞播种对移植物性能的作用
在长段气道缺损的治疗中,理想的气管置换术结构仍然是难以捉摸的。组织工程气管移植物(TETG)一直受到移植物狭窄或塌陷、感染或缺乏上皮衬里的限制。我们应用小鼠气道原位手术模型来评估临床应用中遇到的三个关键障碍的影响:支架、干预程度和细胞播种的影响,并表征它们对移植物性能的影响。首先,将涤纶/聚氨酯(PET/PU)静电纺丝合成气管支架原位植入C57BL/6小鼠气管前路缺损。支架在2周内被纤毛呼吸道上皮完全覆盖。上皮细胞的迁移伴随着巨噬细胞的浸润,并在长时间(>6周)持续存在。然后,我们评估了使用同种气管作为理想气管替代物的节段性气管植入的影响。移植物恢复涉及上皮祖细胞群体的局部上调,没有移植物狭窄或坏死的证据。人工合成气管支架植入术后出现呼吸窘迫,需尽早实施安乐死。有或没有植入骨髓源性单核细胞(BM-MNCs)的支架上皮覆盖有限。我们得出的结论是,人工合成支架支持原位补片植入的再上皮化,同源移植物整合发生在局灶修复机制中,然而,部分合成支架的上皮化是有限的,不受细胞播种的影响。
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