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在灵长类动物肾移植慢性而非急性排斥反应中,血管性血友病因子的肾小球沉积物增加。

Increased glomerular deposits of von Willebrand factor in chronic, but not acute, rejection of primate renal allografts.

作者信息

Lagoo A S, Buckley P J, Burchell L J, Peters D, Fechner J H, Tsuchida M, Dong Y, Hong X, Brunner K G, Oberley T D, Hamawy M M, Knechtle S J

机构信息

Department of Surgery, University of Wisconsin, Madison 53792-7375, USA.

出版信息

Transplantation. 2000 Sep 27;70(6):877-86. doi: 10.1097/00007890-200009270-00005.

Abstract

BACKGROUND

In our previously described primate renal allograft model, T cell ablation leads to long-term graft survival. The role of endothelial cell alteration in chronic rejection was examined in our model.

METHODS

Renal transplants were performed in rhesus monkeys using a T cell- depleting immunotoxin, FN18-CRM9. Sections from 10 rejected kidneys (5 acute and 7 chronic rejection) were examined after immunohistochemical staining for expression of endothelium-related proteins [von Willebrand factor (vWF), CD62P, and CD31], fibrinogen, and a macrophage marker (CD68). Glomerular staining for each antigen was graded on a semiquantitative scale.

RESULTS

Intense staining for vWF was consistently observed in glomerular endothelium, subendothelium, and mesangium in all kidneys removed due to chronic rejection. vWF staining was weak in kidneys showing acute rejection. The difference in glomerular staining was statistically significant. Staining for vWF in extraglomerular vessels was nearly identical in kidneys showing acute and chronic rejection. Expression of CD62P was increased in extraglomerular vessels in allografts with chronic rejection, but the glomeruli showed little or no staining. There was no significant difference in the glomerular staining for CD62P or CD31 in organs showing acute and chronic rejection. Fibrinogen staining of glomerular mesangium was seen in kidneys with chronic rejection. Macrophages (CD68+) infiltrating glomeruli were more numerous in kidneys showing chronic rejection.

CONCLUSION

Increased glomerular deposition of vWF in renal allografts showing chronic rejection, without increased staining for CD62P or CD31, suggests increased constitutive secretion of vWF from endothelial cells as a component of the mechanism of chronic rejection in our model.

摘要

背景

在我们之前描述的灵长类动物肾移植模型中,T细胞消融可导致移植物长期存活。在我们的模型中研究了内皮细胞改变在慢性排斥反应中的作用。

方法

使用T细胞清除免疫毒素FN18-CRM9对恒河猴进行肾移植。对10个排斥肾(5个急性排斥和7个慢性排斥)的切片进行免疫组织化学染色,检测内皮相关蛋白[血管性血友病因子(vWF)、CD62P和CD31]、纤维蛋白原和巨噬细胞标志物(CD68)的表达。对每种抗原的肾小球染色进行半定量评分。

结果

在因慢性排斥而切除的所有肾脏中,肾小球内皮、内皮下和系膜中均持续观察到vWF的强烈染色。在表现为急性排斥的肾脏中,vWF染色较弱。肾小球染色的差异具有统计学意义。在表现为急性和慢性排斥的肾脏中,肾外血管中vWF的染色几乎相同。在慢性排斥的同种异体移植物中,肾外血管中CD62P的表达增加,但肾小球几乎没有染色或无染色。在表现为急性和慢性排斥的器官中,肾小球CD62P或CD31染色无显著差异。在慢性排斥的肾脏中可见肾小球系膜的纤维蛋白原染色。在表现为慢性排斥的肾脏中,浸润肾小球的巨噬细胞(CD68+)更多。

结论

在表现为慢性排斥的肾移植中,vWF在肾小球的沉积增加,而CD62P或CD31染色未增加,提示内皮细胞组成性分泌vWF增加是我们模型中慢性排斥反应机制的一个组成部分。

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