| Literature DB >> 30793848 |
Dekai Xia1, Dawei Jin1, Qian Wang2, Manchen Gao1, Jialing Zhang1, Hengyi Zhang1, Jie Bai1, Bei Feng1,3, Maolin Chen1, Yanhui Huang4, Yumin Zhong2, Nevin Witman5, Wei Wang1, Zhiwei Xu1, Haibo Zhang1, Meng Yin1, Wei Fu1,3,6.
Abstract
Traditional treatment therapies for tracheal stenosis often cause severe post-operative complications. To solve the current difficulties, novel and more suitable long-term treatments are needed. A whole-segment tissue-engineered trachea (TET) representing the native goat trachea was 3D printed using a poly(caprolactone) (PCL) scaffold engineered with autologous auricular cartilage cells. The TET underwent mechanical analysis followed by in vivo implantations in order to evaluate the clinical feasibility and potential. The 3D-printed scaffolds were successfully cellularized, as observed by scanning electron microscopy. Mechanical force compression studies revealed that both PCL scaffolds and TETs have a more robust compressive strength than does the native trachea. In vivo implantation of TETs in the experimental group resulted in significantly higher mean post-operative survival times, 65.00 ± 24.01 days (n = 5), when compared with the control group, which received autologous trachea grafts, 17.60 ± 3.51 days (n = 5). Although tracheal narrowing was confirmed by bronchoscopy and computed tomography examination in the experimental group, tissue necrosis was only observed in the control group. Furthermore, an encouraging epithelial-like tissue formation was observed in the TETs after transplantation. This large animal study provides potential preclinical evidence around the employment of an orthotopic transplantation of a whole 3D-printed TET.Entities:
Keywords: 3D-printed; PCL; goat; large animal experiment; tissue-engineered trachea; trachea transplantation
Mesh:
Year: 2019 PMID: 30793848 DOI: 10.1002/term.2828
Source DB: PubMed Journal: J Tissue Eng Regen Med ISSN: 1932-6254 Impact factor: 3.963