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自体移植脾脏中增殖的改变及蛋白质合成的细微变化。

Alteration of proliferation and subtle changes of protein synthesis in autologous transplanted spleens.

作者信息

Thalhamer J, Lenglachner C, Grillenberger W, Pimpl W

机构信息

Department of Biochemistry, University of Salzburg, Austria.

出版信息

Ann Surg. 1989 Nov;210(5):630-6. doi: 10.1097/00000658-198911000-00011.

Abstract

In the case of massive splenic rupture, heterotopic autologous transplantation of splenic tissue into the omentum majus may be used to restore splenic function. Yet little is known about specific functions of the transplants compared to the normal spleen. The goal of this study was to get more information about immunologic functions and protein expression in splenic transplants. As an animal model we used the pig, whose splenic morphology and immunoarchitecture is similar to that of the human spleen. Histologic examination of transplants revealed structures that were comparable to normal spleens (consisting of red and white pulp and including germinal centers). Immunologic tests such as the hemolytic plaque assay and mitogen stimulation revealed that the number of plaque-forming cells was not changed significantly, but the stimulation index for T cells was drastically increased in the autotransplants. Electrophoresis and immunochemical methods showed differences in the protein patterns between both tissues. Several proteins were found to be produced only in the spleen, or were produced in much higher amounts in the spleen than in the splenic transplants. More information about these differences between spleen and splenic transplants is needed before we can recommend a general clinical application of autologous spleen transplantation.

摘要

在脾严重破裂的情况下,可将脾组织异位自体移植到大网膜中以恢复脾功能。然而,与正常脾脏相比,移植脾的具体功能鲜为人知。本研究的目的是获取更多关于脾移植免疫功能和蛋白质表达的信息。我们使用猪作为动物模型,其脾脏形态和免疫结构与人类脾脏相似。对移植脾的组织学检查发现其结构与正常脾脏相似(由红髓和白髓组成,包括生发中心)。溶血空斑试验和丝裂原刺激等免疫学检测显示,空斑形成细胞数量无显著变化,但自体移植脾中T细胞的刺激指数显著增加。电泳和免疫化学方法显示两种组织的蛋白质图谱存在差异。发现几种蛋白质仅在脾脏中产生,或在脾脏中的产生量远高于脾移植组织。在我们能够推荐自体脾移植的一般临床应用之前,需要更多关于脾脏与脾移植之间这些差异的信息。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/630a/1357798/79ae4ad1cba2/annsurg00177-0068-a.jpg

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