在非清髓性且无辐照预处理治疗下，阻断CD40/CD154通路可增强去除T细胞的异基因骨髓植入。

Blockade of the CD40/CD154 pathway enhances T-cell-depleted allogeneic bone marrow engraftment under nonmyeloablative and irradiation-free conditioning therapy.

作者信息

Pan Yisheng, Luo Bin, Sozen Haken, Kalscheuer Hannes, Blazar Bruce R, Sutherland David E R, Hering Benhard J, Guo Zhiguang

机构信息

Department of Surgery and Diabetes, Institute for Immunology and Transplantation, University of Minnesota, Minneapolis, MN 55455, USA.

出版信息

Transplantation. 2003 Jul 15;76(1):216-24. doi: 10.1097/01.TP.0000069602.30162.A1.

DOI:10.1097/01.TP.0000069602.30162.A1

PMID:12865813

Abstract

BACKGROUND

T-cell-depleted bone marrow transplantation (TDBMT) can prevent graft-versus-host disease (GvHD). However, depleting T cells from allogeneic bone marrow often results in failure of bone marrow engraftment under irradiation conditioning. It is not know whether donor T cells are essential for bone marrow engraftment and whether blocking the CD40/CD154 pathway promotes allogeneic TDBM engraftment under nonmyeloablative and irradiation-free fludarabine phosphate and cyclophosphamide conditioning therapy.

METHODS

Using fully major histocompatibility complex (MHC)-matched mouse models, we investigated whether donor T cells are essential for bone marrow engraftment under fludarabine phosphate and cyclophosphamide conditioning therapy. We also determined whether the barrier of allogeneic TDBM could be overcome by blocking the CD40/CD154 pathway. Donor chimerism was detected by flow cytometric analysis. Donor-specific tolerance through establishing mixed chimerism was tested in vivo by skin transplantation and in vitro by mixed leukocyte reaction and enzyme-linked immunospot (ELISPOT) assay.

RESULTS

Compared with unmodified bone marrow, TDBM resulted in poor engraftment when fully MHC-mismatched donors were used. However, anti-CD154 monoclonal antibody (mAb) treatment significantly enhanced donor TDBM engraftment. TDBM engraftment was also seen in CD154 knockout mice. A stable and high level of multilinage donor chimerism was achieved. Recovery of host CD3 T cells was suppressed, and recovery of donor CD3 T cells was promoted, after TDBMT and anti-CD154 mAb treatment. Donor chimerism was established by TDBMT induced donor-specific tolerance in vivo and in vitro.

CONCLUSION

Donor T cells facilitate bone marrow engraftment under nonmyeloablative and irradiation-free conditioning therapy, and the blocking the CD40/CD154 pathway can replace donor T cells to promote TDBM engraftment.

摘要

背景

去除T细胞的骨髓移植（TDBMT）可预防移植物抗宿主病（GvHD）。然而，在照射预处理条件下，从异基因骨髓中去除T细胞常导致骨髓植入失败。目前尚不清楚供体T细胞对于骨髓植入是否必不可少，以及在非清髓性且无照射的磷酸氟达拉滨和环磷酰胺预处理治疗下，阻断CD40/CD154途径是否能促进异基因TDBM植入。

方法

使用完全主要组织相容性复合体（MHC）匹配的小鼠模型，我们研究了在磷酸氟达拉滨和环磷酰胺预处理治疗下，供体T细胞对于骨髓植入是否必不可少。我们还确定了阻断CD40/CD154途径是否能克服异基因TDBM的植入障碍。通过流式细胞术分析检测供体嵌合情况。通过皮肤移植在体内以及通过混合淋巴细胞反应和酶联免疫斑点（ELISPOT）试验在体外测试通过建立混合嵌合实现的供体特异性耐受。

结果

与未修饰的骨髓相比，当使用完全MHC不匹配的供体时，TDBM导致植入不佳。然而，抗CD154单克隆抗体（mAb）治疗显著增强了供体TDBM植入。在CD154基因敲除小鼠中也观察到了TDBM植入。实现了稳定且高水平的多谱系供体嵌合。在TDBMT和抗CD154 mAb治疗后，宿主CD3 T细胞的恢复受到抑制，而供体CD3 T细胞的恢复得到促进。通过TDBMT建立了供体嵌合，在体内和体外诱导了供体特异性耐受。