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环孢素A加供体特异性输血预处理可诱导特异性B细胞耐受:延长I类主要组织相容性复合体不同的心脏同种异体移植物的存活时间。

Specific B cell tolerance is induced by cyclosporin A plus donor-specific blood transfusion pretreatment: prolonged survival of MHC class I disparate cardiac allografts.

作者信息

Yang C P, Shittu E, Bell E B

机构信息

Immunology Research Group, Biological Sciences, Medical School, Manchester, United Kingdom.

出版信息

J Immunol. 2000 Mar 1;164(5):2427-32. doi: 10.4049/jimmunol.164.5.2427.

DOI:10.4049/jimmunol.164.5.2427
PMID:10679079
Abstract

Donor-specific blood transfusion (DST), designed to prolong allograft survival, sensitized recipients of the high-responder PVG-RT1u strain, resulting in accelerated rejection of MHC-class I mismatched (PVG-R8) allografts. Rejection was found to be mediated by anti-MHC class I (Aa) alloantibody. By pretreating recipients 4 wk before grafting with cyclosporin A (CsA) daily (x7), combined with once weekly (x4) DST, rejection was prevented. The investigation explores the mechanism for this induced unresponsiveness. CD4 T cells purified from the thoracic duct of CsA/DST-pretreated RT1u rats induced rejection when transferred to R8 heart-grafted RT1u athymic nude recipients, indicating that CD4 T cells were not tolerized by the pretreatment. To determine whether B cells were affected, nude recipients were pretreated, in the absence of T cells, with CsA/DST (or CsA/third party blood) 4 wk before grafting. The subsequent transfer of normal CD4 T cells induced acute rejection of R8 cardiac allografts in third party- but not DST-pretreated recipients; prolonged allograft survival was reversed by the cotransfer of B cells with the CD4 T cells. Graft survival correlated with reduced production of anti-MHC class I (Aa) cytotoxic alloantibody. The results indicated that the combined pretransplant treatment of CsA and DST induced tolerance in allospecific B cells independently of T cells. The resulting suppression of allospecific cytotoxic Ab correlated with the survival of MHC class I mismatched allografts. The induction of B cell tolerance by CsA has important implications for clinical transplantation.

摘要

供者特异性输血(DST)旨在延长同种异体移植物存活时间,但却使高反应性PVG - RT1u品系的受者致敏,导致MHC - I类错配(PVG - R8)同种异体移植物加速排斥。发现这种排斥是由抗MHC - I类(Aa)同种异体抗体介导的。通过在移植前4周每天用环孢素A(CsA)预处理受者(共7次),并结合每周一次(共4次)的DST,可预防排斥反应。本研究探讨了这种诱导性无反应性的机制。从经CsA/DST预处理的RT1u大鼠胸导管中纯化的CD4 T细胞,转移至接受R8心脏移植的RT1u无胸腺裸鼠受者时会诱导排斥反应,这表明预处理并未使CD4 T细胞产生耐受。为确定B细胞是否受到影响,在无T细胞的情况下,于移植前4周用CsA/DST(或CsA/第三方血液)预处理裸鼠受者。随后转移正常CD4 T细胞,可诱导第三方预处理但非DST预处理的受者发生R8心脏同种异体移植物的急性排斥反应;B细胞与CD4 T细胞共转移可逆转同种异体移植物的长期存活。移植物存活与抗MHC - I类(Aa)细胞毒性同种异体抗体产生减少相关。结果表明,移植前联合使用CsA和DST的治疗可独立于T细胞诱导同种特异性B细胞产生耐受。由此产生的同种特异性细胞毒性抗体的抑制与MHC - I类错配同种异体移植物的存活相关。CsA诱导B细胞耐受对临床移植具有重要意义。

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Specific B cell tolerance is induced by cyclosporin A plus donor-specific blood transfusion pretreatment: prolonged survival of MHC class I disparate cardiac allografts.环孢素A加供体特异性输血预处理可诱导特异性B细胞耐受:延长I类主要组织相容性复合体不同的心脏同种异体移植物的存活时间。
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