Hess A D, Horwitz L R, Laulis M K, Fuchs E
Bone Marrow Transplant Unit, Johns Hopkins University, Baltimore, Maryland 21287-8985.
Clin Immunol Immunopathol. 1993 Dec;69(3):341-50. doi: 10.1006/clin.1993.1190.
Administration of cyclosporine (CsA) following syngeneic/autologous bone marrow transplantation (BMT) elicits a T lymphocyte-dependent autoimmune disease resembling graft-vs-host disease (syngeneic GVHD). This autoaggression syndrome appears to be due to the autorecognition of self-MHC class II antigens by CD8+ cytolytic T cells and a CD4+ autoreactive T cell subset. The syngeneic GVHD model was used to assess the effectiveness of treatment with monoclonal antibodies to the alpha/beta T cell receptor (TCR) and the CD4 or CD8 determinants on the prevention of autoimmune disease. Nylon wool nonadherent splenic T cells (50 x 10(6)) from Lewis strain rats with active syngeneic GVHD were adoptively transferred into irradiated (1050 rad syngeneic recipients reconstituted with normal marrow (60 x 10(6) cells). Monoclonal antibody (McAb) to the alpha/beta TCR, the CD4 determinant, or the CD8 determinant was administered to secondary recipients on Days 0, 3, 6, 9, and 12 at a dose of 0.1 ml of ascites fluid. Control animals received normal mouse serum on the same schedule. Animals treated with either saline or normal mouse serum developed syngeneic GVHD within 16-20 days. Comparatively, syngeneic GVHD developed much later in the secondary recipients treated with anti-CD4 McAb (onset of syngeneic GVHD, 28-32 days) and was less severe compared to the control group. On the other hand, the recipients treated with McAb's to the alpha/beta TCR or to the CD8 determinant did not develop syngeneic GVHD (monitored over 10 weeks post-therapy). Peripheral blood lymphocytes from these recipients also were analyzed for T cell subsets by phenotypic analysis. There was a pronounced reduction of the total number of cells expressing the alpha/beta TCR and the CD8 determinant after treatment of the recipients with the McAb's to the alpha/beta TCR and to the CD8 determinant, respectively. Recovery to normal levels began to occur 6 weeks after the last dose of McAb. There was a significant reduction of the CD4+ subset after treatment with anti-CD4 McAb, but it was not long lasting with recovery coinciding with the onset of syngeneic GVHD. Studies were also performed to evaluate McAb therapy of established syngeneic GVHD. The McAb's were found to be largely ineffective due in part to pulmonary toxicity. Furthermore, this model was utilized to evaluate the efficacy of treatment with McAb to the target antigen of syngeneic GVHD. Infusion of McAb to a public determinant on class II MHC molecules prevented or significantly delayed the onset of syngeneic GVHD after adoptive transfer of effector cells.(ABSTRACT TRUNCATED AT 400 WORDS)
在同基因/自体骨髓移植(BMT)后给予环孢素(CsA)会引发一种类似于移植物抗宿主病(同基因GVHD)的T淋巴细胞依赖性自身免疫性疾病。这种自身攻击综合征似乎是由于CD8 + 细胞毒性T细胞和CD4 + 自身反应性T细胞亚群对自身MHC II类抗原的自身识别所致。同基因GVHD模型用于评估针对α/β T细胞受体(TCR)以及CD4或CD8决定簇的单克隆抗体治疗对预防自身免疫性疾病的有效性。将来自患有活动性同基因GVHD的Lewis品系大鼠的尼龙毛非黏附性脾T细胞(50×10⁶)过继转移到经照射(1050拉德)的同基因受体中,这些受体用正常骨髓(60×10⁶个细胞)进行重建。在第0、3、6、9和12天,以0.1毫升腹水的剂量向二级受体给予针对α/β TCR、CD4决定簇或CD8决定簇的单克隆抗体(McAb)。对照动物按相同时间表接受正常小鼠血清。用盐水或正常小鼠血清治疗的动物在16 - 20天内发生同基因GVHD。相比之下,用抗CD4 McAb治疗的二级受体中同基因GVHD出现得要晚得多(同基因GVHD的发病时间为28 - 32天),并且与对照组相比病情较轻。另一方面,用针对α/β TCR或CD8决定簇的McAb治疗的受体未发生同基因GVHD(在治疗后10周内进行监测)。还通过表型分析对这些受体的外周血淋巴细胞进行T细胞亚群分析。在用针对α/β TCR和CD8决定簇的McAb分别治疗受体后,表达α/β TCR和CD8决定簇的细胞总数明显减少。在最后一剂McAb后6周开始恢复到正常水平。用抗CD4 McAb治疗后CD4 + 亚群显著减少,但持续时间不长,恢复与同基因GVHD的发病同时发生。还进行了研究以评估已确立的同基因GVHD的McAb治疗。发现McAb在很大程度上无效,部分原因是肺部毒性。此外,该模型用于评估用针对同基因GVHD靶抗原的McAb治疗的疗效。向II类MHC分子上的一个公共决定簇输注McAb可预防或显著延迟效应细胞过继转移后同基因GVHD的发病。(摘要截于400字)
