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巨噬细胞激活在同种异体移植免疫中的作用:体内研究

Role of macrophage activation in allograft immunity: in vivo studies.

作者信息

Debray-Sachs M, Dy M, Hamburger J

出版信息

Ann Immunol (Paris). 1979 Sep-Oct;130C(5):721-33.

PMID:393160
Abstract

Macrophage-rich adherent peritoneal cells from mice sensitized by two i.p. injections of allogeneic cells at days -- 12 and --2, were found non-specifically cytotoxic against (a) tumoral target cells, as evaluated by the chromium release test, and (b) normal target cells, as evaluated by a functional test based on the insulin secretion response to glucose stimulation of isolated pancreatic islet cells. This non-specific cytotoxicity was identical to that of macrophages "activated" by an in vitro incubation with supernatants of MLC between allograft donor and recipient as reported elsewhere. Moreover this cytotoxicity was not abolished by anti-theta serum treatment of adherent peritoneal cells before contact with target cells. It is concluded that an in vivo macrophage activation was obtained in our experiment. Using this same model, we found that the survival time of skin grafts from male C57BL/6 to female C57BL/6 mice was shortened if the graft was performed at the time when the recipient macrophages were found non-specifically cytotoxic (two days after the second allogeneic cell injection). The role of macrophage cytotoxicity in this accelerated allograft rejection is suggested by (a) the lack of any detectable cross-histocompatibility antigens between the immunizing cells and the skin graft, and (b) the absence of any alteration of the graft survival if the second immunizing injection two days prior to grafting is omitted (in that case only lymphocytes are found specifically cytotoxic against the strain of injected cells, while the non-specific cytotoxicity of macrophages is lacking).

摘要

在第 - 12天和第 - 2天经两次腹腔注射同种异体细胞致敏的小鼠中,富含巨噬细胞的贴壁腹膜细胞,通过铬释放试验评估发现对(a)肿瘤靶细胞具有非特异性细胞毒性,通过基于分离的胰岛细胞对葡萄糖刺激的胰岛素分泌反应的功能试验评估发现对(b)正常靶细胞具有非特异性细胞毒性。这种非特异性细胞毒性与其他地方报道的通过同种异体移植供体和受体之间的混合淋巴细胞培养上清液体外孵育“激活”的巨噬细胞的细胞毒性相同。此外,在贴壁腹膜细胞与靶细胞接触之前,用抗θ血清处理并没有消除这种细胞毒性。得出的结论是,在我们的实验中获得了体内巨噬细胞激活。使用相同的模型,我们发现,如果在受体巨噬细胞被发现具有非特异性细胞毒性时(第二次同种异体细胞注射后两天)进行移植,雄性C57BL/6小鼠到雌性C57BL/6小鼠的皮肤移植存活时间会缩短。巨噬细胞细胞毒性在这种加速的同种异体移植排斥反应中的作用体现在:(a)免疫细胞和皮肤移植之间缺乏任何可检测到交叉组织相容性抗原,以及(b)如果省略移植前两天的第二次免疫注射(在这种情况下,仅发现淋巴细胞对注射细胞的菌株具有特异性细胞毒性,而巨噬细胞的非特异性细胞毒性不存在),移植存活没有任何改变。

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Role of macrophage activation in allograft immunity: in vivo studies.巨噬细胞激活在同种异体移植免疫中的作用:体内研究
Ann Immunol (Paris). 1979 Sep-Oct;130C(5):721-33.
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