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A new total hemiface allotransplantation model in rats

医学 同种异体移植 外科 移植
作者
Yalçın Külahçı,Selman Hakkı Altuntaş,Hüseyi̇n Karagöz,Joanna Cwykiel,Fatih Zor,Maria Siemionow
出处
期刊:Microsurgery [Wiley]
卷期号:36 (3): 230-238 被引量:9
标识
DOI:10.1002/micr.22527
摘要

Introduction Vascularized composite allotransplantation (VCA), a new reconstructive option for patients suffering from extensive facial defects leads to superior functional and aesthetic outcomes compared to the standard autologous reconstruction. Among VCA recipients, each case involves different facial structures and tissues depending on the patient's injury, thus drawing conclusions on the mechanism of immune interactions between the donor and recipient is challenging. This study introduces a new total hemiface VCA model, including scalp, external ear, mystacial pad, premaxilla, upper/lower lids, nose, and upper/lower lips to evaluate the effect of transplantation of multitissue VCA on the recipient's immune response. Material and Methods Ten hemiface allotransplantations were performed in two groups between Lewis–Lewis (isograft) and LBN‐Lewis (allograft) rats. Cyclosporine A (CsA) monotherapy was applied in the allograft group to prevent rejection. Results All flaps survived up to 100 days post‐transplant. The mean warm ischemia time was 45 minutes. Histological analysis revealed normal bone, cartilage (ear and nose), conjunctiva, palpebra, and eyelashes. Flow cytometry confirmed donor‐specific chimerism for T cells (CD4/RT1 n and CD8/RT1 n ) and B cells (CD45RA/RT1 n ) in the peripheral blood of all rats in the allotransplantation group. At post‐transplant day 7, chimerism levels were at 1.68% for CD4/RT1 n , 0.46% for CD8/RT1 n and 0.64% for CD45RA/RT1 n . However, chimerism levels for CD4/RT1 n , CD8/RT1 n , and CD45RA/RT1 n populations decreased at long‐term follow‐up (at post‐transplant day 100) to 0.08%, 0.04%, and 0.23%, respectively. Conclusion The feasibility and long‐term survival of the new hemiface VCA transplantation model was confirmed, donor‐specific chimerism and post‐transplant tissue changes were evaluated. © 2016 Wiley Periodicals, Inc. Microsurgery 36:230–238, 2016.

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