丝裂霉素诱导的血细胞与环孢素A的短期治疗相结合可延长血管化复合异体移植中同种异体移植物的存活时间。

The combination of mitomycin-induced blood cells with a temporary treatment of ciclosporin A prolongs allograft survival in vascularized composite allotransplantation.

作者信息

Radu Christian Andreas, Fischer Sebastian, Diehm Yannick, Hetzel Otto, Neubrech Florian, Dittmar Laura, Kleist Christian, Gebhard Martha Maria, Terness Peter, Kneser Ulrich, Kiefer Jurij

机构信息

Department of Hand, Plastic and Reconstructive Surgery, Burn Center, BG Trauma Center Ludwigshafen, Plastic- and Hand Surgery, University of Heidelberg, Ludwig-Guttmann-Str. 13, D-67071, Ludwigshafen, Germany.

Transplantation Immunology, Institute for Immunology, University of Heidelberg, Heidelberg, Germany.

出版信息

Langenbecks Arch Surg. 2018 Feb;403(1):83-92. doi: 10.1007/s00423-017-1616-3. Epub 2017 Aug 19.

DOI:10.1007/s00423-017-1616-3

PMID:28823033

Abstract

BACKGROUND

Vascularized composite allotransplantation (VCA) is a rapidly expanding field of transplantation and provides a potential treatment for complex tissue defects. Peripheral blood mononuclear cells (PBMCs) shortly incubated with the antibiotic and chemotherapeutic agent mitomycin C (MMC) can suppress allogeneic T cell response and control allograft rejection in various organ transplantation models. MMC-incubated PBMCs (MICs) are currently being tested in a phase I clinical trial in kidney transplant patients. Previous studies with MICs in a complex VCA model showed the immunomodulatory potential of these cells. The aim of this study is to optimize and evaluate the use of MICs in combination with a standard immunosuppressive drug in VCA.

METHODS

Fully mismatched rats were used as hind limb donors [Lewis (RT1)] and recipients [Brown-Norway (RT1)]. Sixty allogeneic hind limb transplantations were performed in six groups. Group A received donor-derived MICs combined with a temporary ciclosporin A (CsA) treatment. Group B received MICs in combination with a temporarily administered reduced dose of CsA. Group C served as a control and received a standard CsA dose temporarily without an additional administration of MICs, whereas Group D was solely medicated with a reduced CsA dose. Group E received no immunosuppressive therapy, neither CsA nor MICs. Group F was given a continuous standard immunosuppressive regimen consisting of CsA and prednisolone. The endpoint of the study was the onset of allograft rejection which was assessed clinically and histologically.

RESULTS

In group A and B, the rejection-free interval of the allograft was significantly prolonged to an average of 23.1 ± 1.7 and 24.7 ± 1.8 days compared to the corresponding control groups (p < 0.01). Rejection in groups C, D, and E was noted after 14.3 ± 1.1, 7.8 ± 0.7, and 6.9 ± 0.6 days. No rejection occurred in control group F during the follow-up period of 100 days. No adverse events have been noted.

CONCLUSION

The findings of this study show that the combination of MICs with a temporary CsA treatment significantly prolongs the rejection-free interval in a complex VCA model. The combination of MICs with CsA showed no adverse events such as graft-versus-host disease. MICs, which are generated by a simple and reliable in vitro technique, represent a potential therapeutic tool for prolonging allograft survival through immunomodulation.

摘要

背景

血管化复合组织异体移植（VCA）是一个快速发展的移植领域，为复杂组织缺损提供了一种潜在的治疗方法。与抗生素及化疗药物丝裂霉素C（MMC）短期孵育的外周血单个核细胞（PBMC）可抑制同种异体T细胞反应，并在各种器官移植模型中控制移植排斥反应。MMC孵育的PBMC（MIC）目前正在肾移植患者的I期临床试验中进行测试。先前在复杂VCA模型中对MIC的研究显示了这些细胞的免疫调节潜力。本研究的目的是优化和评估MIC与标准免疫抑制药物联合用于VCA的效果。

方法

完全不匹配的大鼠用作后肢供体[刘易斯大鼠（RT1）]和受体[布朗 - 挪威大鼠（RT1）]。在六组中进行了60次同种异体后肢移植。A组接受供体来源的MIC联合临时环孢素A（CsA）治疗。B组接受MIC联合临时给予的降低剂量的CsA。C组作为对照组，临时接受标准剂量的CsA且不额外给予MIC，而D组仅给予降低剂量的CsA。E组未接受免疫抑制治疗，既未使用CsA也未使用MIC。F组接受由CsA和泼尼松龙组成的持续标准免疫抑制方案。研究的终点是移植排斥反应的发生，通过临床和组织学评估。