通过不同的交叉配型方法对已形成捐献者特异性抗体的患者进行活体肾移植前的风险分层。

IF 1.9 Q3 TRANSPLANTATION
Transplantation Direct Pub Date : 2024-08-08 eCollection Date: 2024-09-01 DOI:10.1097/TXD.0000000000001680
Malte Ziemann, Monika Lindemann, Michael Hallensleben, Wolfgang Altermann, Karina Althaus, Klemens Budde, Gunilla Einecke, Ute Eisenberger, Andrea Ender, Thorsten Feldkamp, Florian Grahammer, Martina Guthoff, Christopher Holzmann-Littig, Christian Hugo, Teresa Kauke, Stephan Kemmner, Martina Koch, Nils Lachmann, Matthias Marget, Christian Morath, Martin Nitschke, Lutz Renders, Sabine Scherer, Julian Stumpf, Vedat Schwenger, Florian Sommer, Bernd Spriewald, Caner Süsal, Daniel Zecher, Falko M Heinemann, Murielle Verboom
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引用次数: 0

摘要

背景:已形成的供体特异性 HLA 抗体(DSA)是肾移植中一个众所周知的风险因素。然而,关于预形成 DSA 患者的最佳风险分层仍存在很大争议。此外,有关不同交叉配型检测法对 DSA 阳性患者预后价值的数据也很少:方法:DSA 阳性的活体肾移植受者是从一项检查 4233 例连续肾移植的多中心研究中挑选出来的。另外还纳入了来自另外两个中心的 7 名患者。使用移植前血清和从新鲜样本中分离出的淋巴细胞,回顾性地进行了流式细胞术交叉配血(FXM)、基于 Luminex 的交叉配血以及基于 C1q 和 C3d 结合抗体的虚拟交叉配血(C1qXM 和 C3dXM)。这些样本来自 12 个中心的 44 对供体和受体。临床结果数据和无 DSA 的对照组数据由之前的研究汇编而来,并以 10 年死亡剪除移植物存活率(10yGS)数据作为补充:19%(C3dXM)到46%(FXM)的交叉配型呈阳性。交叉配型阳性患者在 6 个月内抗体介导的排斥反应(AMR)发生率很高(B 细胞 FXM+ 患者高达 60%)。交叉配型阴性患者的 AMR 发生率介于 5%(FXM-)和 13%(C1qXM-)之间。与无交叉配型阴性的患者和交叉配型阴性的患者相比,T细胞FXM阳性和总FXM阳性的患者10yGS明显受损:结论:FXM尤其适用于风险分层,因为DSA阳性、FXM阴性患者的预后与DSA阴性患者相似,而FXM阳性患者的AMR更多,10yGS下降。 由于灵敏度较低,基于Luminex的交叉配型、C1qXM和C3dXM在DSA较强的患者中的意义有待研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Risk Stratification Before Living Donor Kidney Transplantation in Patients With Preformed Donor-specific Antibodies by Different Crossmatch Methods.

Background: Preformed donor-specific HLA antibodies (DSA) are a well-known risk factor in kidney transplantation. There is still considerable debate, however, about the optimal risk stratification among patients with preformed DSA. Additionally, data on the prognostic value of different crossmatch assays in DSA-positive patients are scarce.

Methods: DSA-positive living kidney transplant recipients were selected from a multicenter study examining 4233 consecutive renal transplants. An additional 7 patients from 2 further centers were included. Flow cytometric crossmatches (FXM), Luminex-based crossmatches, and virtual crossmatches based on C1q- and C3d-binding antibodies (C1qXM and C3dXM) were performed retrospectively using pretransplant sera and lymphocytes isolated from fresh samples. These samples were obtained from 44 donor and recipient pairs from 12 centers. Clinical outcome data and the control group without DSA were compiled from the previous study and were supplemented by data on 10-y death-censored graft survival (10yGS).

Results: Between 19% (C3dXM) and 46% (FXM) of crossmatches were positive. Crossmatch-positive patients showed high incidences of antibody-mediated rejection (AMR) within 6 mo (up to 60% in B-cell FXM+ patients). The incidence of AMR in crossmatch-negative patients ranged between 5% (FXM-) and 13% (C1qXM-). 10yGS was significantly impaired in patients with positive T-cell FXM and total FXM compared with both patients without DSA and those with DSA with negative FXM.

Conclusions: Especially FXM are useful for risk stratification, as the outcome of DSA-positive, FXM-negative patients is similar to that of DSA-negative patients, whereas FXM-positive patients have both more AMR and decreased 10yGS. Because of their lower sensitivity, the significance of Luminex-based crossmatches, C1qXM, and C3dXM would have to be examined in patients with stronger DSA.

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来源期刊
Transplantation Direct
Transplantation Direct TRANSPLANTATION-
CiteScore
3.40
自引率
4.30%
发文量
193
审稿时长
8 weeks
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