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DLA单倍型不匹配犬移植物抗宿主病的预防以及移植后使用和不使用cG-CSF治疗时CD6缺失骨髓的造血植入

Prevention of graft-versus-host disease in DLA-haplotype mismatched dogs and hemopoietic engraftment of CD6-depleted marrow with and without cG-CSF treatment after transplantation.

作者信息

Schumm M, Günther W, Kolb H J, Rieber P, Büttner M, Voss C, Kremmer E, Reitmeier P, Thierfelder S, Wilmanns W

机构信息

GSF-Forschungszentrum für Umwelt, Ludwig-Maximilians-Universität München, Germany.

出版信息

Tissue Antigens. 1994 Mar;43(3):170-8. doi: 10.1111/j.1399-0039.1994.tb02318.x.

Abstract

Prevention of graft-versus-host disease by depletion of CD6-positive T cells was studied in the dog. Donors were DLA-homozygous, recipients DLA-heterozygous with one DLA haplotype identical to the donor. Seven control dogs received untreated marrow and died of GvHD after full hemopoietic recovery within 28 days of transplantation. For prevention of GvHD, immunomagnetic separation of T cells with a monoclonal antibody against human CD6 that crossreacted with canine T cells was evaluated. Depletion of CD6-positive cells depleted CD4-positive cells completely, but only part of CD8-positive cells and DR-positive cells. CD6-depleted marrow exhibited strong nonspecific "natural" suppression of the generation of cytotoxic T cells in vitro. Eleven dogs received CD6-depleted marrow. Only 1 dog developed GvHD and died. Sustained engraftment was seen in 8 dogs. Hemopoietic recovery was delayed and slower after transplantation of CD6-depleted marrow than after transplantation of untreated marrow. Four of these dogs were treated with G-CSF, and this accelerated the recovery of leukocytes, but did not prevent rejection. Chimerism was mixed in 7 of 10 evaluable dogs and 1 dog recovered its own hemopoiesis 2 years after transplantation. CD6 depletion prevents GvHD across a DLA-haplotype difference, but rejection and mixed chimerism may occur. Treatment with G-CSF accelerates leukocyte recovery, but cannot prevent rejection.

摘要

在犬类中研究了通过清除CD6阳性T细胞来预防移植物抗宿主病。供体为DLA纯合子,受体为DLA杂合子,其中一个DLA单倍型与供体相同。7只对照犬接受未处理的骨髓,在移植后28天内完全造血恢复后死于移植物抗宿主病。为预防移植物抗宿主病,评估了用与犬T细胞发生交叉反应的抗人CD6单克隆抗体对T细胞进行免疫磁珠分离。清除CD6阳性细胞可完全清除CD4阳性细胞,但仅部分清除CD8阳性细胞和DR阳性细胞。CD6清除的骨髓在体外对细胞毒性T细胞的产生表现出强烈的非特异性“天然”抑制作用。11只犬接受了CD6清除的骨髓。只有1只犬发生移植物抗宿主病并死亡。8只犬出现持续植入。与未处理的骨髓移植后相比,CD6清除的骨髓移植后造血恢复延迟且较慢。其中4只犬接受了粒细胞集落刺激因子治疗,这加速了白细胞的恢复,但未能防止排斥反应。在10只可评估的犬中有7只出现混合嵌合体,1只犬在移植后2年恢复了自身造血。清除CD6可预防跨越DLA单倍型差异的移植物抗宿主病,但可能会发生排斥反应和混合嵌合体。用粒细胞集落刺激因子治疗可加速白细胞恢复,但不能防止排斥反应。

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