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在次要组织相容性抗原移植物抗宿主反应期间,由于供体T细胞的选择性扩增导致B细胞发育受到抑制。

Suppression of B-cell development as a result of selective expansion of donor T cells during the minor H antigen graft-versus-host reaction.

作者信息

Garvy B A, Elia J M, Hamilton B L, Riley R L

机构信息

Department of Microbiology and Immunology, University of Miami School of Medicine, FL 33101.

出版信息

Blood. 1993 Nov 1;82(9):2758-66.

PMID:8219228
Abstract

A murine model of bone marrow (BM) transplantation in which donor (B10.D2) and recipient (BALB/c) mice were major histocompatibility complex (MHC) (H-2d) and Mls-1 identical, but incompatible at multiple non-MHC minor histocompatibility (H) antigens, and at Mls-2,3 was used to examine regeneration of B-cell development during the minor H antigen graft-versus-host reaction (GVHR). Mice that received T-cell-depleted allogeneic BM regained significant pre-B cells (sIg- 14.8+) in their BM. Mice undergoing GVHR after transplantation with allogeneic BM + T cells had less than 2% pre-B cells in their BM at day 7 and only 12% to 14% pre-B cells at days 21 and 28 compared with greater than 20% pre-B cells in the allogeneic controls. After partial recovery, the pre-B cells in the BM of GVH mice again decreased to less than 3% by day 42. This abnormal pattern of pre-B cell development in mice undergoing GVHR was associated with a reduced response to interleukin-7 (IL-7) in vitro. The delay in B-lineage cell reconstitution in mice with GVHR correlated with the expansion of donor V beta 3+ T cells in both the spleen and BM. BM T cells from mice with GVHR as well as isolated V beta 3+ T cells inhibited IL-7 colony-forming units from normal BM in co-culture assays. This inhibition could be reversed with anti-interferon gamma (IFN gamma) antibody. These data suggest that the delay in appearance and the reduction in proportion and number of pre-B cells observed early during the GVH reaction in this model is caused, in part, by the inhibitory actions of IFN gamma derived from donor V beta 3+ T cells on B-lineage cell development.

摘要

采用一种骨髓(BM)移植的小鼠模型,其中供体(B10.D2)和受体(BALB/c)小鼠主要组织相容性复合体(MHC)(H-2d)和Mls-1相同,但在多个非MHC次要组织相容性(H)抗原以及Mls-2、3方面不匹配,用于研究次要H抗原移植物抗宿主反应(GVHR)期间B细胞发育的再生情况。接受去除T细胞的同种异体骨髓的小鼠,其骨髓中重新出现了大量前B细胞(sIg- 14.8+)。移植同种异体骨髓加T细胞后发生GVHR的小鼠,在第7天时骨髓中前B细胞少于2%,在第21天和28天时仅为12%至14%,而同种异体对照中前B细胞大于20%。部分恢复后,GVH小鼠骨髓中的前B细胞在第42天时再次降至3%以下。发生GVHR的小鼠中前B细胞发育的这种异常模式与体外对白介素-7(IL-7)的反应降低有关。GVHR小鼠中B系细胞重建的延迟与脾脏和骨髓中供体Vβ3+ T细胞的扩增相关。GVHR小鼠的骨髓T细胞以及分离的Vβ3+ T细胞在共培养试验中抑制了正常骨髓的IL-7集落形成单位。这种抑制作用可用抗干扰素γ(IFNγ)抗体逆转。这些数据表明,在该模型中GVH反应早期观察到的前B细胞出现延迟、比例和数量减少,部分是由供体Vβ3+ T细胞产生的IFNγ对B系细胞发育的抑制作用所致。

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Suppression of B-cell development as a result of selective expansion of donor T cells during the minor H antigen graft-versus-host reaction.在次要组织相容性抗原移植物抗宿主反应期间,由于供体T细胞的选择性扩增导致B细胞发育受到抑制。
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