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免疫球蛋白或Fc受体γ缺陷小鼠中猪胰岛样细胞簇的异种移植排斥反应

Xenograft rejection of porcine islet-like cell clusters in immunoglobulin- or Fc-receptor gamma-deficient mice.

作者信息

Benda B, Karlsson-Parra A, Ridderstad A, Korsgren O

机构信息

Department of Clinical Immunology, Uppsala University, Sweden.

出版信息

Transplantation. 1996 Nov 15;62(9):1207-11. doi: 10.1097/00007890-199611150-00003.

Abstract

The aim of the present study was to evaluate the role of xenoreactive antibodies in islet-like cell cluster (ICC) xenograft rejection. For this purpose, normal mice, mice with a targeted disruption of the Fc-receptor (FcR) gamma-chain, or the membrane exon of the immunoglobulin mu-chain gene, were transplanted with fetal porcine ICC under the kidney capsule. Mice lacking the FcR gamma have no functional FcR for IgG or IgE. Mice with disruption of the immunoglobulin mu-chain cannot produce antibodies, because B cell development is arrested at the stage of preB cells. All animals, irrespective of recipient group, readily rejected the ICC xenograft. Analyses of the pattern of cellular infiltration revealed only minor dissimilarities between the different experimental groups. Xenograft destruction was evident on day 6 after transplantation, and a large number of mononuclear cells were found to be evenly distributed throughout the ICC graft. The majority of the infiltrating cells were large, macrophage-like cells expressing the macrophage-specific phenotype marker F4/80. CD3-positive T lymphocytes were found to be mainly accumulated in the peripheral parts of the ICC xenograft. This study has demonstrated that xenoreactive antibodies are not crucial to ICC xenograft rejection in the pig-to-mouse model.

摘要

本研究的目的是评估异种反应性抗体在胰岛样细胞簇(ICC)异种移植排斥反应中的作用。为此,将正常小鼠、Fc受体(FcR)γ链或免疫球蛋白μ链基因膜外显子靶向破坏的小鼠在肾包膜下移植胎猪ICC。缺乏FcRγ的小鼠没有针对IgG或IgE的功能性FcR。免疫球蛋白μ链破坏的小鼠不能产生抗体,因为B细胞发育在preB细胞阶段停滞。所有动物,无论受体组如何,均迅速排斥ICC异种移植。细胞浸润模式分析显示不同实验组之间仅有微小差异。移植后第6天异种移植破坏明显,发现大量单核细胞均匀分布于整个ICC移植物中。大多数浸润细胞是表达巨噬细胞特异性表型标志物F4/80的大的巨噬样细胞。发现CD3阳性T淋巴细胞主要聚集在ICC异种移植的周边部分。本研究表明,在猪到小鼠模型中,异种反应性抗体对ICC异种移植排斥反应并不关键。

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