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首页> 外文期刊>Transplant immunology >Host thymectomy and cyclosporine lead to unstable skin graft tolerance after class I mismatched allogeneic neonatal thymic transplantation in mice.
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Host thymectomy and cyclosporine lead to unstable skin graft tolerance after class I mismatched allogeneic neonatal thymic transplantation in mice.

机译:小鼠胸腺切除术和环孢菌素导致I类小鼠异基因新生儿胸腺移植不匹配后导致不稳定的皮肤移植耐受性。

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摘要

BACKGROUND: Our laboratory has demonstrated that xenogeneic porcine thymus tissue grafted in thymectomized (ATX) and T cell-depleted mice induces donor-specific tolerance. Recipient thymectomy is essential for the success of tolerance induction. In contrast, studies in pigs grafted with non-vascularized allogeneic class I mismatched thymus tissue under the cover of CyA have shown that removal of host thymus is detrimental to thymic graft survival. To determine the requirements for nonvascularized allogeneic class I-mismatched thymic engraftment in mice, we performed thymic allotransplantation under the cover of CyA. MATERIALS AND METHODS: Euthymic and ATX B10.MBR mice received class I mismatched B10.AKM neonatal mouse thymus (NMTHY) tissue under the kidney capsule with or without a short course of CyA. The grafts were allowed to engraft for two and a half months before exploratory laparotomy was performed to evaluate them. Three months after the thymic transplant, mice were challenged with donor-specific skin grafts to assess tolerance. One month after donor-specific skin grafting, they received third party B10.BR skin grafts. Cellular anti-donor immune responses were studied at the time of euthanasia. RESULTS: CyA-treated ATX and euthymic control mice showed good engraftment of the allogeneic thymic tissue at the time of exploratory laparotomy, whereas non-CyA-treated ATX and euthymic controls had rejected the grafts. The CyA-treated ATX B10.MBR mice accepted donor-specific skin grafts, but rejected them following a challenge with third party B10.BR skin grafts. Untreated ATX and euthymic mice and 6 of 7 CyA-treated euthymic mice rejected donor skin within 15 days. Mixed lymphocyte reactions did not show an increased anti-donor response, but CML clearly showed sensitization and increased killing activity against donor-type targets in these mice. CONCLUSION: Allogeneic thymic transplantation across a class I MHC barrier under the cover of CyA induces a metastable state of tolerance in mice. To achieve this state, ATX of the recipient is required.
机译:背景:我们的实验室已经证明,在胸腺切除(ATX)和T细胞缺失的小鼠中移植的异种猪胸腺组织可诱导供体特异性耐受。接受胸腺切除术对于成功诱导耐受至关重要。相比之下,对在CyA覆盖下移植了非血管化I类异基因胸腺组织的猪进行的研究表明,去除宿主胸腺对胸腺移植物的存活有害。为了确定小鼠中非血管化同种异基因I类不匹配胸腺移植的要求,我们在CyA的掩护下进行了胸腺同种异体移植。材料与方法:正常的和ATX的B10.MBR小鼠在肾囊下接受I类不匹配的B10.AKM新生小鼠胸腺(NMTHY)组织,伴或不伴短程CyA。在进行探索性剖腹手术以评估它们之前,让它们移植两个半月。胸腺移植后三个月,用供体特异性皮肤移植物攻击小鼠以评估耐受性。供体特异性皮肤移植后一个月,他们接受了第三方B10.BR皮肤移植。安乐死时研究了细胞抗供体的免疫反应。结果:经CyA处理的ATX和正常人对照小鼠在探索性剖腹手术时表现出良好的异体胸腺组织植入,而未经CyA处理的ATX和正常人对照则排斥了移植物。经CyA处理的ATX B10.MBR小鼠接受了供体特异性皮肤移植物,但是在受到第三方B10.BR皮肤移植物的挑战后拒绝了它们。未经治疗的ATX和正常小鼠和7只经CyA治疗的正常小鼠中有6只在15天内排斥了供体皮肤。混合淋巴细胞反应未显示出增强的抗供体反应,但CML清楚地显示了这些小鼠中对供体型靶标的致敏性和杀伤活性的增强。结论:在CyA的保护下跨I类MHC屏障进行异基因胸腺移植可诱导小鼠的亚稳态耐受。要实现此状态,需要收件人的ATX。

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