αβ和γδ T细胞在同种异体供体骨髓植入、嵌合状态及移植物抗宿主病中的作用。
The role of alphabeta- and gammadelta-T cells in allogenic donor marrow on engraftment, chimerism, and graft-versus-host disease.
作者信息
Huang Y, Cramer D E, Ray M B, Chilton P M, Que X, Ildstad S T
机构信息
Institute for Cellular Therapeutics, University of Louisville, 570 South Preston Street, Suite 404, Louisville, KY 40202, USA.
出版信息
Transplantation. 2001 Dec 27;72(12):1907-14. doi: 10.1097/00007890-200112270-00007.
BACKGROUND
We previously characterized a facilitating cell (FC) in mouse marrow that enables engraftment of allogeneic hematopoietic stem cells (HSCs) without causing graft-versus-host disease (GVHD). The FC shares some cell surface molecules with T cells (Thy1+, CD3epsilon+, CD8+, CD5+, and CD2+) but is T-cell receptor (TCR) negative. Historically, depletion of CD3+ or CD8+ cells from rat marrow was associated with an increased rate of failure of engraftment. In this study, we evaluated whether depletion of alphabeta- and gammadelta-TCR(+) T cells from donor marrow would retain engraftment potential yet avoid GVHD.
METHODS
Wistar-Furth rats were conditioned with 950 cGy of total body irradiation and transplanted with ACI bone marrow processed to remove either alphabeta-TCR(+), gammadelta-TCR(+), or alphabeta- plus gammadelta-TCR(+) T cells. Recipients were typed for chimerism at 28 days and monthly thereafter.
RESULTS
Recipients of marrow depleted of alphabeta- (group A), gammadelta- (group B), or alphabeta- and gammadelta-TCR(+) T cells (group C) engrafted and had an average chimerism level of 73.0+/-8.3%, 92.3+/-9.2%, and 46.3+/-32.8%, respectively. Aggressive T-cell depletion did not remove the FC population (CD8+/CD3+/TCR(-)). Group A and group B both developed GVHD, with a higher incidence of GVHD in group B compared to group A. None of the recipients in group C developed GVHD.
CONCLUSIONS
These data demonstrate that depletion of T cells from rat marrow does not impair engraftment of HSCs, indirectly supporting the existence of FCs in rat marrow. Moreover, donor alphabeta- and gammadelta-TCR(+) T cells contribute to GVHD in a nonredundant fashion, although alphabeta-TCR(+) T cells are more potent as the effector cells. Finally, the level of donor chimerism is influenced by the composition of the graft, because recipients of marrow that contain alphabeta-TCR(+) T cells exhibited significantly higher donor chimerism compared to recipients of marrow depleted of both alphabeta- and gammadelta-TCR(+) T cells.
背景
我们之前鉴定了小鼠骨髓中的一种促进细胞(FC),它能使异基因造血干细胞(HSC)植入,而不会引发移植物抗宿主病(GVHD)。FC与T细胞共享一些细胞表面分子(Thy1 +、CD3ε +、CD8 +、CD5 +和CD2 +),但为T细胞受体(TCR)阴性。从历史上看,从大鼠骨髓中去除CD3 +或CD8 +细胞与植入失败率增加有关。在本研究中,我们评估了从供体骨髓中去除αβ - 和γδ - TCR(+)T细胞是否会保留植入潜力,同时避免GVHD。
方法
用950 cGy全身照射对Wistar - Furth大鼠进行预处理,然后移植经处理以去除αβ - TCR(+)、γδ - TCR(+)或αβ - 和γδ - TCR(+)T细胞的ACI骨髓。在28天时对受体进行嵌合分型,此后每月进行一次。
结果
接受去除αβ - (A组)、γδ - (B组)或αβ - 和γδ - TCR(+)T细胞(C组)的骨髓移植的受体均成功植入,平均嵌合水平分别为73.0±8.3%、92.3±9.2%和46.3±32.8%。积极的T细胞去除并未清除FC群体(CD8 + / CD3 + / TCR( - ))。A组和B组均发生了GVHD,B组的GVHD发生率高于A组。C组的受体均未发生GVHD。
结论
这些数据表明,从大鼠骨髓中去除T细胞不会损害HSC的植入,间接支持了大鼠骨髓中FC的存在。此外,供体αβ - 和γδ - TCR(+)T细胞以非冗余方式促成GVHD,尽管αβ - TCR(+)T细胞作为效应细胞更具效力。最后,供体嵌合水平受移植物组成的影响,因为含有αβ - TCR(+)T细胞的骨髓移植受体与去除αβ - 和γδ - TCR(+)T细胞的骨髓移植受体相比,表现出显著更高的供体嵌合率。
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