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Predicting Alloreactivity in Transplantation

机译:预测移植过程中的含量

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Human leukocyte Antigen (HLA) mismatching leads to severe complications after solid-organ transplantation and hematopoietic stem-cell transplantation. The alloreactive responses underlying the posttransplantation complications include both direct recognition of allogeneic HLA by HLA-specific alloantibodies and T cells and indirect T-cell recognition. However, the immunogenicity of HLA mismatches is highly variable; some HLA mismatches lead to severe clinical B-cell- and T-cell-mediated alloreactivity, whereas others are well tolerated. Definition of the permissibility of HLA mismatches prior to transplantation allows selection of donor-recipient combinations that will have a reduced chance to develop deleterious host-versus-graft responses after solid-organ transplantation and graft-versus-host responses after hematopoietic stem-cell transplantation. Therefore, several methods have been developed to predict permissible HLA-mismatch combinations. In this review we aim to give a comprehensive overview about the current knowledge regarding HLA-directed alloreactivity and several developed in vitro and in silico tools that aim to predict direct and indirect alloreactivity.
机译:在固体器官移植和造血干细胞移植和造血干细胞移植后,人白细胞抗原(HLA)匹配导致严重的并发症。后翻透并发症的含有反应性的反应包括HLA特异性AlloAlibodies和T细胞和间接T细胞识别的同种异体HLA的直接识别。然而,HLA错配的免疫原性是高度变化的;一些HLA不匹配导致严重的临床B细胞和T细胞介导的含量,而其他HLA不匹配是良好的耐受性。移植前HLA错配的定义允许选择在造血干细胞移植后固体器官移植和移植物与宿主反应在固体器官移植和移植物 - 宿主反应后产生减少机会的供体 - 受体组合。 。因此,已经开发了几种方法来预测允许的HLA-Mismatch组合。在这篇综述中,我们的目标是全面概述关于HLA定向的含有性的目前的知识和在体外开发的几种开发,旨在预测直接和间接的占间断性的硅工具。

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