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新型基于固相的酶联免疫吸附测定法有助于改进抗人白细胞抗原抗体的检测,并提高移植前后交叉配型的可靠性。

Novel solid phase-based ELISA assays contribute to an improved detection of anti-HLA antibodies and to an increased reliability of pre- and post-transplant crossmatching.

作者信息

Schlaf Gerald, Pollok-Kopp Beatrix, Manzke Till, Schurat Oliver, Altermann Wolfgang

机构信息

Tissue Typing Laboratory, University Hospital , University of Halle-Wittenberg , Halle , Germany.

Department of Transfusion Medicine, University Hospital , University of Göttingen , Göttingen , Germany.

出版信息

NDT Plus. 2010 Dec;3(6):527-38. doi: 10.1093/ndtplus/sfq156. Epub 2010 Sep 15.

Abstract

Antibodies directed against HLA antigens of a given organ donor represent the dominating reason for hyper-acute or acute allograft rejections. In order to select recipients without donor-specific antibodies, a standard crossmatch (CM) procedure, the complement-dependent cytotoxicity assay (CDC), was developed. This functional assay strongly depends on the availability of isolated vital lymphocytes of a given donor. However, the requirements of the donor's material may often not be fulfilled, so that the detection of the antibodies directed against HLA molecules is either impaired or becomes completely impossible. To circumvent the disadvantages of the CDC procedure, enzyme-linked immunosorbent assay (ELISA)-based and other solid phase-based ELISA-related techniques have been designed to reliably detect anti-HLA antibodies in recipients. Due to the obvious advantages of these novel technologies, when compared with the classical CDC assay, there is an urgent need to implement them as complementary methods or even as a substitution for the conventional CDC crossmatch that is currently being applied by all tissue typing laboratories.

摘要

针对特定器官供体的HLA抗原的抗体是超急性或急性同种异体移植排斥反应的主要原因。为了选择没有供体特异性抗体的受者,开发了一种标准的交叉配型(CM)程序,即补体依赖细胞毒性试验(CDC)。这种功能试验强烈依赖于特定供体分离的活淋巴细胞的可用性。然而,供体材料的要求往往无法满足,因此针对HLA分子的抗体检测要么受到损害,要么变得完全不可能。为了规避CDC程序的缺点,基于酶联免疫吸附测定(ELISA)和其他基于固相的ELISA相关技术已被设计用于可靠地检测受者中的抗HLA抗体。由于这些新技术与经典CDC试验相比具有明显优势,迫切需要将它们作为补充方法,甚至替代目前所有组织分型实验室都在应用的传统CDC交叉配型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f1a4/4421419/525e0d222ca6/sfq156fig1.jpg

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