Abstract

Although creating a tracheal tube de novo might appear straightforward, the first clinical applications have shown that reconstruction of long-segment tracheal defects remains challenging. In this study, the authors aimed to refine the baseline requirements of successful trachea transplantation by means of three proof-of-concept models in the rabbit. In each model, one characteristic of a perfect tracheal transplant was eliminated. The first model was developed to map out the immunologic response of vascularized allogenic trachea, transplanted without immunosuppression (n = 6). The second model studied (1) the need for wrapping the transplant with a highly vascularized flap and (2) the source of angiogenesis after autologous trachea transplantation (n = 18). In the third model, the authors examined the importance of an inner epithelial covering (n = 12). All models were compared to a control group of heterotopically transplanted vascularized autologous tracheae (n = 6). Embedded in an avascular matrix, allogenic chondrocytes were protected from an overt immune response. Orthotopic transplantation without additional external vascular wrap was successful in a well-vascularized environment. Nonetheless, an external vascular source was essential to maintain viability of the construct. Epithelial covering was necessary to prevent secondary healing. Epithelial migration from the anastomoses or graft was not sufficient to cover long-segment defects. These experiments provided ample evidence of the importance of baseline requirements when designing a tracheal transplant study. This study confirmed that different tracheal cell types possess different immunologic sensitivities. External revascularization, preferably in a two-stage procedure, and fast reepithelialization were both paramount to successful transplantation.

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