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一种临床可行的方法,可诱导先前接受过肾或血管化复合组织同种异体移植的受者产生延迟性耐受。

A clinically feasible approach to induce delayed tolerance in recipients of prior kidney or vascularized composite allotransplants.

机构信息

Institute for Cellular Therapeutics, University of Louisville, Louisville, KY, USA.

出版信息

Transplantation. 2012 Oct 15;94(7):671-8. doi: 10.1097/TP.0b013e318264fbc1.

Abstract

BACKGROUND

Mixed chimerism induces donor-specific tolerance to kidney and vascularized composite allotransplants (VCA). However, simultaneous kidney or VCA and bone marrow transplantation (BMT) is problematic because of the combined risk and time required for conditioning. Here, we developed a delayed tolerance induction strategy with mixed chimerism through BMT in prior kidney or VCA recipients.

METHODS

Wistar Furth rats that received kidney transplantation (KTx) or VCA from allogeneic August-Copenhagen Irish donors were maintained on immunosuppression (IS) for 8 weeks. These recipients were then conditioned with anti-αβ-T-cell receptor and anti-CD8 monoclonal antibodies, total body irradiation, cyclosporine A and mycophenolate mofetil (12 doses), and antilymphocyte serum (one dose); and transplanted with T-cell-depleted donor marrow. All IS was discontinued on day 11 after BMT.

RESULTS

Cyclosporine A monotherapy prevented acute rejection of KTx or VCA. However, all allografts were rejected after IS withdrawal in KTx or VCA recipients who were conditioned but did not receive BMT. After delayed BMT, mixed chimerism was initially achieved in all KTx or VCA recipients with 200-, 300-, and 400-cGy total body irradiation. Long-term tolerance to KTx or VCA was achieved in most of these recipients with total IS withdrawal. The tolerance achieved with delayed BMT was donor specific as confirmed by acceptance of donor skin and rejection of third-party skin graft.

CONCLUSIONS

IS-free donor-specific tolerance can be successfully induced with delayed BMT to previous recipients of kidney transplantation or VCA. These findings have significant clinical implications for transplant recipients who receive an organ from either a living donor or a deceased donor with frozen bone marrow cells available.

摘要

背景

嵌合状态可诱导对肾和血管化复合组织移植(VCA)的供者特异性耐受。然而,由于联合风险和调理所需的时间,同时进行肾或 VCA 和骨髓移植(BMT)是有问题的。在这里,我们通过先前接受过肾或 VCA 移植的受者的 BMT 开发了一种延迟嵌合状态诱导的耐受策略。

方法

接受来自同种异体 August-Copenhagen Irish 供体的肾移植(KTx)或 VCA 的 Wistar Furth 大鼠接受免疫抑制(IS)治疗 8 周。然后,这些受者接受抗-αβ-T 细胞受体和抗-CD8 单克隆抗体、全身照射、环孢素 A 和霉酚酸酯(12 剂)和抗淋巴细胞血清(1 剂)预处理,并接受 T 细胞耗竭的供者骨髓移植。BMT 后第 11 天停用所有 IS。

结果

环孢素 A 单药治疗可预防 KTx 或 VCA 的急性排斥反应。然而,在接受调理但未接受 BMT 的 KTx 或 VCA 受者中,IS 停药后所有同种异体移植物均被排斥。在延迟 BMT 后,所有 KTx 或 VCA 受者均在接受 200、300 和 400-cGy 全身照射后最初实现嵌合状态。在这些受者中,大多数在完全停用 IS 后实现了对 KTx 或 VCA 的长期耐受。通过接受供体皮肤和排斥第三方皮肤移植物证实,延迟 BMT 获得的耐受是供者特异性的。

结论

通过延迟 BMT 成功诱导对先前接受肾移植或 VCA 治疗的受者进行无 IS 的供者特异性耐受。这些发现对接受来自活体供者或有冷冻骨髓细胞的已故供者的器官的移植受者具有重要的临床意义。

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