结合分子错配方法预测肾移植后第一年内的免疫事件

IF 5.9 4区 医学 Q2 CELL BIOLOGY
HLA Pub Date : 2024-11-06 DOI:10.1111/tan.15748
Cäcilia Jäger, Matthias Niemann, Gideon Hönger, Caroline Wehmeier, Helmut Hopfer, Thomas Menter, Patrizia Amico, Michael Dickenmann, Stefan Schaub
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引用次数: 0

摘要

目前有几种分子错配评估方法,但综合使用这些方法的数据有限。在这项研究中,我们的目标是在 439 例连续的免疫学标准风险移植中,根据三种分子错配评估方法(即eplet 错配计数、高免疫原性eplet 数量和 PIRCHE-II 评分)的组合来定义不同的排斥风险组。对于每种分子错配评估方法,均使用 ROC 分析来定义临界值,以便根据 Banff 2019 分类预测移植后第一年内的(亚)临床排斥反应,作为参考。如果三项评分均低于临界值,则患者被归入低风险组(19% 的患者);如果三项评分均高于临界值,则患者被归入高风险组(21% 的患者)。低风险组一年的(亚)临床排斥发生率为12%,高风险组为33%(P = 0.003)。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Combined Molecular Mismatch Approaches to Predict Immunological Events Within the First Year After Renal Transplantation

Combined Molecular Mismatch Approaches to Predict Immunological Events Within the First Year After Renal Transplantation

Several molecular mismatch assessment approaches exist, but data on their combined use are limited. In this study, we aimed to define distinct risk groups for rejection based on the combination of three molecular mismatch assessment approaches (i.e., eplet mismatch count, the number of highly immunogenic eplets and PIRCHE-II score) in 439 consecutive immunological standard risk transplantations. For each molecular mismatch assessment approach, ROC analyses were used to define cut-offs for prediction of (sub) clinical rejection according to Banff 2019 classification within the first year post-transplant as a reference. If all three scores were below the cut-off, the patient was assigned to the low-risk group (19% of patients); if all three scores were above the cut-off, the patient was assigned to the high-risk group (21% of patients). The one-year incidence of (sub) clinical rejection was 12% in the low-risk group and 33% in the high-risk group (p = 0.003). Internal validation of the assigned risk groups for prediction of other outcomes revealed a high consistency: clinical rejection (6% vs. 24%; p = 0.004), ATG-treated rejection (1% vs. 16%; p < 0.001) and development of de novo HLA-DSA at 5 years post-transplant (6% vs. 25%; p = 0.003). The molecular mismatch risk group was an independent predictor for (sub) clinical rejection (high-risk vs. low-risk: hazard ratio 3.11 [95%-CI 1.50–6.45]; p = 0.002). We conclude that combining molecular mismatch approaches allows us to distinguish low- and high-risk groups among standard renal allograft recipients. Independent validation in other patient populations and different ethnicities is required.

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来源期刊
HLA
HLA Immunology and Microbiology-Immunology
CiteScore
3.00
自引率
28.80%
发文量
368
期刊介绍: HLA, the journal, publishes articles on various aspects of immunogenetics. These include the immunogenetics of cell surface antigens, the ontogeny and phylogeny of the immune system, the immunogenetics of cell interactions, the functional aspects of cell surface molecules and their natural ligands, and the role of tissue antigens in immune reactions. Additionally, the journal covers experimental and clinical transplantation, the relationships between normal tissue antigens and tumor-associated antigens, the genetic control of immune response and disease susceptibility, and the biochemistry and molecular biology of alloantigens and leukocyte differentiation. Manuscripts on molecules expressed on lymphoid cells, myeloid cells, platelets, and non-lineage-restricted antigens are welcomed. Lastly, the journal focuses on the immunogenetics of histocompatibility antigens in both humans and experimental animals, including their tissue distribution, regulation, and expression in normal and malignant cells, as well as the use of antigens as markers for disease.
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