首页> 美国卫生研究院文献>The Journal of Experimental Medicine >Lethal graft-versus-host disease after bone marrow transplantation across minor histocompatibility barriers in mice. Prevention by removing mature T cells from marrow
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Lethal graft-versus-host disease after bone marrow transplantation across minor histocompatibility barriers in mice. Prevention by removing mature T cells from marrow

机译:在小鼠中通过较小的组织相容性障碍进行骨髓移植后致命的移植物抗宿主病。通过从骨髓中去除成熟的T细胞进行预防

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摘要

In two situations, transfer of normal unsensitized bone marrow cells into heavily irradiated H-2-identical allogeneic mice caused a high incidence of lethal chronic graft-versus-host disease (GVHD), i.e. mortality occuring between days of 20 and 80 postirradiation. Minor histocompatibility determinants appeared to be the main target for eliciting GVHD. Removing mature T cells from the marrow with anti-Thy 1.2 serum and complement before injection prevented GVHD. On the basis of adding purified T cells to T-cell-depleted marrow cells, it was concluded that contamination of the marrow with as few as 0.3% T cells was sufficient to cause a high incidence of lethal GVHD in certain situations. No GVHD was found with the injection of non-T cells (Thy 1.2-negative cells) or with tolerant T cells. Irradiated recipients of T-cell-depleted marrow cells remained in good health for prolonged periods. These mice showed extensive chimerism with respect to the donor marrow, normal numbers of T and B cells and were immunocompetent. The data provide no support for the view that chronic GVHD developing after bone marrow transplantation in man is the result of an attack by the progeny of the donor stem cells. The results imply that mature T cells contaminating marrow inocula are probably the main cause of GVHD seen in the clinical situation.
机译:在两种情况下,正常的未敏化骨髓细胞转移到受过强烈辐照的H-2-同种异体小鼠中会导致致死性慢性移植物抗宿主病(GVHD)的高发生,即死亡率在辐照后20到80天之间发生。较小的组织相容性决定簇似乎是引起GVHD的主要靶标。注射前用抗Thy 1.2血清和补体从骨髓中去除成熟的T细胞可预防GVHD。在向贫T细胞的骨髓细胞中添加纯化的T细胞的基础上,得出的结论是,在某些情况下,仅含0.3%T细胞的骨髓污染足以引起高致死率的GVHD。注射非T细胞(Thy 1.2阴性细胞)或耐受性T细胞均未发现GVHD。消耗T细胞的骨髓细胞接受辐照的人长期处于良好状态。这些小鼠在供体骨髓,正常T细胞和B细胞方面表现出广泛的嵌合性,并且具有免疫能力。该数据没有支持以下观点,即人骨髓移植后发生慢性GVHD是供体干细胞后代攻击的结果。结果表明,在临床情况下,成熟的T细胞污染了骨髓接种物可能是导致GVHD的主要原因。

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