Donor specific antibodies before and after kidney transplant: the University of Colorado Experience.

Clinical transplants Pub Date : 2013-01-01

James E Cooper, Jane Gralla, Oluwafisayo Adebiyi, Alexander C Wiseman, Laurence Chan

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Abstract

We summarize in this manuscript our donor specific antibody (DSA) screening experience in the past six years as it applies to pre-existing DSA, de novo DSA, and post-transplant DSA treatment. Of 547 patients receiving a kidney or kidney/pancreas with negative pre-transplant flow cytometry crossmatch (FCXM), 196 had DSA (mean fluorescence intensity, MFI >or= 500) detected prior to transplant by single antigen bead analysis. Acute rejection rates at one year were similar in DSA+ versus DSA- (15% versus 12%, respectively, p=0.22), although acute rejection occurred earlier in the DSA+ group. De novo DSA was detected in 65 of 261 patients (27%). All DSA was detected within the first posttransplant year. While acute rejection was more likely in patients with de novo DSA (29% versus 9.5% in those with no DSA), prospective DSA screening failed to predict this outcome as DSA was detected at the time of or after a rejection episode in 16 of 19 patients with both DSA and acute rejection. Two-year estimated graft survival was significantly worse in patients with versus without DSA, but was identical when removing patients with a prior acute rejection episode from the analysis. We have used a protocol of high dose (5 gm/kg) intravenous immunoglobulin infused over the course of 6 months in patients with DSA and either chronic graft dysfunction or following a recent acute antibody mediated rejection (AMR) episode. DSA MFI was reduced by 18% from the time of initiation to last follow up. This effect was largely due to reductions in class I DSA (-37%) and DSA in patients with a recent acute AMR (-51.5%), with a minimal effect on class II DSA and DSA in patients with chronic graft dysfunction. Despite treatment directed at antibody-producing plasma cells, antibody levels either persisted or worsened with no improvement in graft function. Overall, DSA is more amendable to treatment when associated with a recent acute rejection event.

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肾移植前后供体特异性抗体:科罗拉多大学的经验。

我们在这篇文章中总结了过去六年我们的供体特异性抗体(DSA)筛选经验，因为它适用于预先存在的DSA，新生DSA和移植后的DSA治疗。547例移植前流式细胞术交叉匹配(FCXM)阴性的肾脏或肾/胰腺患者中，196例在移植前通过单抗原珠分析检测到DSA(平均荧光强度，MFI >或= 500)。尽管急性排斥反应在DSA+组发生得更早，但一年内急性排斥反应在DSA+组和DSA-组相似(分别为15%和12%，p=0.22)。261例患者中有65例(27%)检测到新生DSA。所有DSA均在移植后一年内检测到。虽然新发DSA患者更有可能出现急性排斥反应(29%对9.5%)，但前瞻性DSA筛查未能预测这一结果，因为在19例同时患有DSA和急性排斥反应的患者中，有16例在排斥事件发生时或之后检测到DSA。接受DSA的患者与不接受DSA的患者相比，两年的移植存活率明显更差，但当从分析中剔除有急性排斥事件的患者时，两者的存活率是相同的。我们使用了高剂量(5 gm/kg)静脉注射免疫球蛋白6个月的方案，用于慢性移植物功能障碍或近期急性抗体介导的排斥反应(AMR)发作的DSA患者。从开始到最后一次随访，DSA MFI减少了18%。这种影响主要是由于近期急性AMR患者的I类DSA(-37%)和DSA(-51.5%)降低，对慢性移植物功能障碍患者的II类DSA和DSA的影响很小。尽管针对产生抗体的浆细胞进行治疗，但抗体水平要么持续存在，要么恶化，移植物功能没有改善。总的来说，当与近期急性排斥事件相关时，DSA更适合治疗。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Clinical transplants

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