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首页> 外文期刊>Xenotransplantation >Xenogeneic skin graft rejection in M-CSF/macrophage deficient osteopetrotic mice.
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Xenogeneic skin graft rejection in M-CSF/macrophage deficient osteopetrotic mice.

机译:M-CSF /巨噬细胞缺陷性骨营养不良小鼠的异种皮肤移植排斥反应。

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Zhao Y, Xiong W, Yang T, Prall A, Baxter BT, Langnas AN. Xenogeneic skin graft rejection in M-CSF/macrophage deficient osteopetrotic mice. Xenotransplantation 2003; 10: 232-239. Copyright Blackwell Munksgaard, 2003 Background: The cellular infiltrate in xenografts suggests that macrophages may be involved in xenograft rejection. However, the precise role of macrophages in xenograft rejection has not yet been fully addressed. Methods: Xenogeneic rat skin grafts were transplanted to macrophage colony stimulating factor (M-CSF)/macrophage-deficient osteopetrotic ([OP]-/-) and wild-type control mice. Skin graft survival and antidonor rat humoral responses were quantified. Results: Xenogeneic rat skin grafts survived 13 days in wild-type control mice, survival of rat skin grafts was significantly prolonged to 24 days in [OP]-/- mice (P<0.01). Similar results were observed in sensitized [OP]-/- and control mouse recipients, showing markedly prolonged rat skin graft survival in [OP]-/- mice. Levels of T-cell-dependent antirat antibodies [immunoglobulin G (IgG)2a and IgG3] in sera of [OP]-/- mice were significantly lower than that of control mice 2 weeks post-rat skin grafting. The proliferative responses to xenogeneic rats not to allogeneic mouse stimulation of T cells from [OP]-/- mice were significantly lower than that of wild-type mice. However, neutrilization of M-CSF by anti-M-CSF monoclonal antibody (mAb) or the addition of M-CSF to the in vitro culture systems of wild-type or [OP]-/- mouse T-responder cells, respectively, did not significantly change proliferative responses and cytolytic function against xenogeneic rat targets of wild-type or [OP]-/- mouse T-responder cells. Conclusions: The in vitro data indicate that M-CSF does not directly regulate cellular immune responses to xenoantigens. The present studies indicate that macrophages may play an important role in immune rejection of xenografts. The precise role of macrophages in xenograft rejection should be further investigated.
机译:Zhao Y,熊W,Yang T,Prall A,Baxter BT,Langnas AN。 M-CSF /巨噬细胞缺陷性骨营养不良小鼠的异种皮肤移植排斥反应。异种移植2003; 10:232-239。版权所有Blackwell Munksgaard,2003年背景:异种移植物中的细胞浸润提示巨噬细胞可能与异种移植排斥有关。然而,巨噬细胞在异种移植排斥中的确切作用尚未完全解决。方法:将异种大鼠皮肤移植到巨噬细胞集落刺激因子(M-CSF)/巨噬细胞缺陷型骨质疏松症([OP]-/-)和野生型对照小鼠中。量化皮肤移植物存活和抗供体大鼠的体液反应。结果:异种大鼠皮肤移植物在野生型对照小鼠中存活13天,在[OP]-/-小鼠中大鼠皮肤移植物存活显着延长至24天(P <0.01)。在致敏的[OP]-/-和对照组小鼠中观察到了相似的结果,表明[OP]-/-小鼠中大鼠皮肤移植物的存活期显着延长。在大鼠皮肤移植后2周,[OP]-/-小鼠血清中T细胞依赖性抗大鼠抗体[免疫球蛋白G(IgG)2a和IgG3]的水平显着低于对照组小鼠。异种小鼠对来自[OP]-/-小鼠的T细胞的同种异体小鼠刺激的增殖反应显着低于野生型小鼠。但是,分别通过抗M-CSF单克隆抗体(mAb)中和M-CSF或将M-CSF加入野生型或[OP]-/-小鼠T应答细胞的体外培养系统,不会明显改变针对野生型或[OP]-/-小鼠T应答细胞异种大鼠靶标的增殖反应和细胞溶解功能。结论:体外数据表明,M-CSF不能直接调节细胞对异种抗原的免疫反应。本研究表明巨噬细胞可能在异种移植物的免疫排斥中起重要作用。巨噬细胞在异种移植排斥中的确切作用应进一步研究。

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