HLA Ⅱ类错配负荷可提高活体供肾移植后 dnDSA 发展的预测能力。
HLA class II eplet mismatch load improves prediction of dnDSA development after living donor kidney transplantation.
机构信息
Blood and Transplantation Center of Porto, Portuguese Institute for Blood and Transplantation, Porto, Portugal.
Unit for Multidisciplinary Research in Biomedicine (UMIB), ICBAS, Porto, Portugal.
出版信息
Int J Immunogenet. 2021 Feb;48(1):1-7. doi: 10.1111/iji.12519. Epub 2020 Nov 3.
HLA donor-specific antibodies developed de novo after transplant remain a major cause of chronic allograft dysfunction. Our study main purpose was to determine whether HLA MM, assessed traditionally and by HLA total and AbVer eplet mismatch load (EptMM and EpvMM) assessed with HLAMatchMaker, had impact on dnDSA development after living donor kidney transplantation (LDKT). We retrospectively analysed a cohort of 96 LDKT between 2008 and 2017 performed in Hospital Santo António. Seven patients developed dnDSA-II and EpvMM and EptMM were greater in dnDSA-II group compared to the no dnDSA-II (18.0 ± 8.7 versus 9.9 ± 7.9, p = .041 and 41.3 ± 18.9 versus 23.1 ± 16.7, p = .018), which is not observed for AgMM (2.29 versus 1.56; p = .09). In a multivariate analysis, we found that preformed DSA (HR = 7.983; p = .023), living unrelated donors (HR = 8.052; p = .024) and retransplantation (HR = 14.393; p = .009) were predictors for dnDSA-II (AUC = 0.801; 0.622-0.981). HLA-II EpvMM (HR = 1.105; p = .028; AUC = 0.856) showed to be a superior predictor of dnDSA-II, when compared to AgMM (HR = 1.740; p = .113; AUC = 0.783), when adjusted for these clinical variables. Graft survival was significantly lower within dnDSA-II patient group (36% versus 88%, p < .001). HLA molecular mismatch analysis is extremely important to minimize risk for HLA-II dnDSA development improving outcome and increasing chance of retransplant lowering allosensitization.
HLA 供体特异性抗体在移植后新出现仍是慢性移植物功能障碍的主要原因。我们的研究主要目的是确定 HLA-MM 是否具有影响,HLA-MM 是通过传统方法和 HLA 总抗体和 AbVer 表位错配负荷(EptMM 和 EpvMM)评估,HLA 匹配器进行评估,在活体供肾移植(LDKT)后是否会影响 dnDSA 的发展。我们回顾性分析了 2008 年至 2017 年在圣安东尼医院进行的 96 例 LDKT 队列。7 例患者出现 dnDSA-II,dnDSA-II 组的 EpvMM 和 EptMM 均大于无 dnDSA-II 组(18.0±8.7 比 9.9±7.9,p=0.041 和 41.3±18.9 比 23.1±16.7,p=0.018),而 AgMM 则没有观察到(2.29 比 1.56;p=0.09)。在多变量分析中,我们发现预先存在的 DSA(HR=7.983;p=0.023)、活体无关供体(HR=8.052;p=0.024)和再次移植(HR=14.393;p=0.009)是 dnDSA-II 的预测因素(AUC=0.801;0.622-0.981)。与 AgMM(HR=1.740;p=0.113;AUC=0.783)相比,HLA-II EpvMM(HR=1.105;p=0.028;AUC=0.856)显示为 dnDSA-II 的更好预测因素,当调整这些临床变量时。dnDSA-II 患者组的移植物存活率明显较低(36%比 88%,p<0.001)。HLA 分子错配分析对于最小化 HLA-II dnDSA 发展风险非常重要,这可以改善结果并增加降低同种异体致敏的再次移植机会。
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