重复人类白细胞抗原外显子,伴侣分型的重要性。

IF 1.6 4区 医学 Q4 IMMUNOLOGY
Carolina dos Reis Ferreira , Vítor Martinho da Silva Fernandes , Sandra Cristina Ribeiro Tafulo , Ana Cerqueira , Ana Cristina Braga Rocha , Ana Teresa Pires Morais Nunes , Inês Passos Castro Neto Ferreira , Maria Joana Cunha Santos , Ana Teresa Marques Teixeira Pinho , Isabel Cristina Tavares , Maria Manuela Brito Bustorff Guerra , Susana Maria Moreira Sampaio Norton
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引用次数: 0

摘要

导言:抗体介导的排斥反应(AMR)是肾移植后免疫介导的同种异体移植失败的最常见原因,并影响同种异体移植的存活率。先前的致敏是产生供体特异性抗体(DSA)的主要风险因素。AMR可以有多种临床特征,如肾功能受损、蛋白尿/高血压,也可以是亚临床症状。HLA 分子有特定的抗原区域与抗体结合,称为表位,表位被认为是负责免疫识别的重要组成部分。我们为您介绍一位移植后 1 周出现亚临床 AMR 的患者:一名 48 岁的白种女性,患有继发于常染色体显性多囊肾(ADPKD)的终末期肾病(ESKD),正在进行腹膜透析。她是一名高敏患者,之前曾三次怀孕,计算得出的全组反应性抗体为 93.48%。她是通过肾脏配对交换捐赠进行移植的,移植前没有发现 DSA。手术和术后情况均无异常,移植肾功能良好且立竿见影。按照方案,第 5 天的 DSA 水平为 DR1 3300 MFI,到第 13 天,MFI 增加到 7820 MFI,新的 B41 为 1979MFI。移植肾活检结果确诊为 AMR,她接受了免疫球蛋白和血浆置换治疗。由于在移植后观察到了早发性 AMR,因此假定之前接触过 allo-HLA 会产生过敏反应。我们决定对她的丈夫,也就是她儿子的父亲进行分型,因为他出现了 DSA。错配外显子分析表明,供体和丈夫共有 41 T 和 67LQ 外显子,分别导致了反应性和新的 HLA I 类 B41 和 HLA II 类 DR1 DSA:讨论:患者丈夫和供体之间共享的外显子是导致同种免疫反应和早期 DSAs 发生的原因。本病例强调了移植后高度致敏患者早期监测DSA水平的重要性,以便及时处理并降低炎症损伤。错配外显子分析可对免疫兼容性进行全面、精确的评估,为免疫风险分层、供体选择和移植后免疫抑制治疗及监测提供了有用的技术。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Repeated human leukocyte antigens eplets, importance of typing the partner

Introduction

Antibody-mediated rejection (AMR) is the most common cause of immune-mediated allograft failure after kidney transplant and impacts allograft survival. Previous sensitization is a major risk factor for development of donor specific antibodies (DSA). AMR can have a wide range of clinical features such as impaired kidney function, proteinuria/hypertension or can be subclinical. HLA molecules have specific regions of antigens binding antibodies called epitopes and eplets are considered essential components responsible for immune recognition. We present a patient with subclinical AMR 1 week post transplantation.

Case report

A 48-year-old, caucasian woman with end-stage kidney disease (ESKD) secondary to autosomal dominant polycystic kidney disease (ADPKD) on peritoneal dialysis was registered in deceased donor waitlist. She was a hypersensitized patient from 3 prior pregnancies with a calculated panel reactive antibody of 93,48%. She was transplanted through kidney paired exchange donation with no evidence of DSA pre transplantation. Surgery and post-op were unremarkable with excellent and immediate graft function. Per protocol DSA levels on the 5th day was DR1 of 3300 MFI, with an increase in MFI by day 13 with 7820 MFI and a new B41 1979MFI. Allograft kidney biopsy findings were diagnostic of AMR and she was treated with immunoglobulin and plasmapheresis. As early onset AMR post transplantation was observed an anamnestic response was hypothesized from a previous exposure to allo-HLA. We decided to type her husband, her son's father, which was presented with DSA. Mismatch eplet analysis revealed a shared 41 T and 67LQ eplets between the donor and husband, responsible for the reactivity and new HLA class I B41 and HLA class II DR1 DSA, respectively.

Discussion

Shared eplets between the patient husband and donor was responsible for the alloimmune response and early development of DSAs. This case highlights the importance of early monitoring DSA levels in highly sensitized patients after transplant in order to promptly address and lower inflammatory damage. Mismatch eplet analysis can provide a thorough and precise evaluation of immune compatibility providing a useful technique to immune risk stratification, donor selection and post-transplant immunosuppressive therapy and monitoring.

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来源期刊
Transplant immunology
Transplant immunology 医学-免疫学
CiteScore
2.10
自引率
13.30%
发文量
198
审稿时长
48 days
期刊介绍: Transplant Immunology will publish up-to-date information on all aspects of the broad field it encompasses. The journal will be directed at (basic) scientists, tissue typers, transplant physicians and surgeons, and research and data on all immunological aspects of organ-, tissue- and (haematopoietic) stem cell transplantation are of potential interest to the readers of Transplant Immunology. Original papers, Review articles and Hypotheses will be considered for publication and submitted manuscripts will be rapidly peer-reviewed and published. They will be judged on the basis of scientific merit, originality, timeliness and quality.
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