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Tracheobronchial transplantation with a stem-cell-seeded bioartificial nanocomposite: a proof-of-concept study.

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Authors
Jungebluth, Philipp
Alici, Evren
Baiguera, Silvia
Le Blanc, Katarina
Blomberg, Pontus
Bozóky, Béla
Crowley, Claire
Einarsson, Oskar
Grinnemo, Karl-Henrik
Gudbjartsson, Tomas
Le Guyader, Sylvie
Henriksson, Gert
Hermanson, Ola
Juto, Jan Erik
Leidner, Bertil
Lilja, Tobias
Liska, Jan
Luedde, Tom
Lundin, Vanessa
Moll, Guido
Nilsson, Bo
Roderburg, Christoph
Strömblad, Staffan
Sutlu, Tolga
Teixeira, Ana Isabel
Watz, Emma
Seifalian, Alexander
Macchiarini, Paolo
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Issue Date
2011-12-10

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Lancet 2011, 378(9808):1997-2004
Abstract
BACKGROUND: Tracheal tumours can be surgically resected but most are an inoperable size at the time of diagnosis; therefore, new therapeutic options are needed. We report the clinical transplantation of the tracheobronchial airway with a stem-cell-seeded bioartificial nanocomposite. METHODS: A 36-year-old male patient, previously treated with debulking surgery and radiation therapy, presented with recurrent primary cancer of the distal trachea and main bronchi. After complete tumour resection, the airway was replaced with a tailored bioartificial nanocomposite previously seeded with autologous bone-marrow mononuclear cells via a bioreactor for 36 h. Postoperative granulocyte colony-stimulating factor filgrastim (10 μg/kg) and epoetin beta (40,000 UI) were given over 14 days. We undertook flow cytometry, scanning electron microscopy, confocal microscopy epigenetics, multiplex, miRNA, and gene expression analyses. FINDINGS: We noted an extracellular matrix-like coating and proliferating cells including a CD105+ subpopulation in the scaffold after the reseeding and bioreactor process. There were no major complications, and the patient was asymptomatic and tumour free 5 months after transplantation. The bioartificial nanocomposite has patent anastomoses, lined with a vascularised neomucosa, and was partly covered by nearly healthy epithelium. Postoperatively, we detected a mobilisation of peripheral cells displaying increased mesenchymal stromal cell phenotype, and upregulation of epoetin receptors, antiapoptotic genes, and miR-34 and miR-449 biomarkers. These findings, together with increased levels of regenerative-associated plasma factors, strongly suggest stem-cell homing and cell-mediated wound repair, extracellular matrix remodelling, and neovascularisation of the graft. INTERPRETATION: Tailor-made bioartificial scaffolds can be used to replace complex airway defects. The bioreactor reseeding process and pharmacological-induced site-specific and graft-specific regeneration and tissue protection are key factors for successful clinical outcome
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http://dx.doi.org/10.1016/S0140-6736(11)61715-7
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Archived with thanks to Lancet
ae974a485f413a2113503eed53cd6c53
10.1016/S0140-6736(11)61715-7
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