首页> 美国卫生研究院文献>Journal of Clinical Medicine >Urinary Biomarkers α-GST and π-GST for Evaluation and Monitoring in Living and Deceased Donor Kidney Grafts
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Urinary Biomarkers α-GST and π-GST for Evaluation and Monitoring in Living and Deceased Donor Kidney Grafts

机译:尿生物标志物α-GST和π-GST用于评估和监测活体和死者的肾脏移植肾

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摘要

The aim of this study was to analyze the value of urine α- and π-GST in monitoring and predicting kidney graft function following transplantation. In addition, urine samples from corresponding organ donors was analyzed and compared with graft function after organ donation from brain-dead and living donors. Urine samples from brain-dead ( = 30) and living related ( = 50) donors and their corresponding recipients were analyzed before and after kidney transplantation. Urine α- and π-GST values were measured. Kidney recipients were grouped into patients with acute graft rejection (AGR), calcineurin inhibitor toxicity (CNI), and delayed graft function (DGF), and compared to those with unimpaired graft function. Urinary π-GST revealed significant differences in deceased kidney donor recipients with episodes of AGR or DGF at day one after transplantation ( = 0.0023 and = 0.036, respectively). High π-GST values at postoperative day 1 (cutoff: >21.4 ng/mg urine creatinine (uCrea) or >18.3 ng/mg uCrea for AGR or DGF, respectively) distinguished between rejection and no rejection (sensitivity, 100%; specificity, 66.6%) as well as between DGF and normal-functioning grafts (sensitivity, 100%; specificity, 62.6%). In living donor recipients, urine levels of α- and π-GST were about 10 times lower than in deceased donor recipients. In deceased donors with impaired graft function in corresponding recipients, urinary α- and π-GST were elevated. α-GST values >33.97 ng/mg uCrea were indicative of AGR with a sensitivity and specificity of 77.7% and 100%, respectively. In deceased donor kidney transplantation, evaluation of urinary α- and π-GST seems to predict different events that deteriorate graft function. To elucidate the potential advantages of such biomarkers, further analysis is warranted.
机译:这项研究的目的是分析尿α-和谷胱甘肽S-转移酶在监测和预测移植后肾移植功能方面的价值。此外,分析了来自相应器官供体的尿液样本,并将其与脑死亡和活体供体器官捐献后的移植物功能进行了比较。在肾脏移植之前和之后分析了来自脑死亡(= 30)和与生命相关(= 50)的供体及其对应受体的尿液样本。测量尿中的α-和GST值。将肾脏接受者分为急性移植排斥反应(AGR),钙调神经磷酸酶抑制剂毒性(CNI)和延迟移植功能(DGF)的患者,并与移植功能未受损的患者进行比较。尿中的π-GST显示,在移植后第一天,已死亡的AGR或DGF肾捐赠者的接受者有显着差异(分别为0.0023和0.036)。术后第1天的高π-GST值(AGR或DGF分别为> 21.4 ng / mg尿肌酐(uCrea)或> 18.3 ng / mg uCrea分别)在排斥和无排斥之间进行区分(敏感性为100%;特异性为66.6%)以及DGF和正常运作的移植物之间(敏感性为100%;特异性为62.6%)。在活体捐献者中,α-和GST的尿液含量比死者捐献者低约10倍。在相应受体中移植功能受损的已故献血者中,尿中α-和GST含量升高。 α-GST值> 33.97 ng / mg uCrea表示AGR,敏感性和特异性分别为77.7%和100%。在已故的供体肾脏移植中,尿α-和GST的评估似乎可以预测使移植物功能恶化的不同事件。为阐明此类生物标志物的潜在优势,有必要进行进一步分析。

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