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A method to reduce variability in scoring antibody-mediated rejection in renal allografts: implications for clinical trials - a retrospective study

机译:一种减少肾同种异体移植术中评分抗体介导的变异性的方法:对临床试验的影响 - 回顾性研究

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Poor reproducibility in scoring antibody-mediated rejection (ABMR) using the Banff criteria might limit the use of histology in clinical trials. We evaluated the reproducibility of Banff scoring of 67 biopsies by six renal pathologists at three institutions. Agreement by any two pathologists was poor: 44.8-65.7% for glomerulitis, 44.8-67.2% for peritubular capillaritis, and 53.7-80.6% for chronic glomerulopathy (cg). All pathologists agreed on cg0 (n = 20) and cg3 (n = 9) cases, however, many disagreed on scores of cg1 or cg2. The range for the incidence of composite diagnoses by individual pathologists was: 16.4-22.4% for no ABMR; 17.9-47.8% for active ABMR; and 35.8-59.7% for chronic, active antibody-mediated rejection (cABMR). A "majority rules" approach was then tested in which the scores of three pathologists were used to reach an agreement. This increased consensus both for individual scores (ex. 67.2-77.6% for cg) and for composite diagnoses (ex. 74.6-86.6% cABMR). Modeling using these results showed that differences in individual scoring could affect the outcome assessment in a mock study of cABMR. We conclude that the Banff schema has high variability and a majority rules approach could be used to adjudicate differences between pathologists and reduce variability in scoring in clinical trials.
机译:使用班夫标准评分抗体介导的抑制(ABMR)的再现性差可能限制在临床试验中的组织学中的使用。我们在三个机构中评估了67个肾病学家67个活检的班夫评分的再现性。任何两位病理学家的协议很差:肾小球炎的44.8-65.7%,慢性肾小球疗法的44.8-67.2%,53.7-80.6%(CG)。然而,所有病理学医生都同意CG0(n = 20)和CG3(n = 9)案例,许多人在CG1或CG2的得分中不同意。单个病理学家的综合诊断发病率的范围是:16.4-22.4%的禁止的abmr;有效ABMR的17.9-47.8%;慢性活性抗体介导的排斥(CABMR)的35.8-59.7%。然后测试了“多数规则”方法,其中三名病理学家的得分用于达成协议。这种增加的个人评分(ex.67.2-77.6%,综合诊断(例如74.6-86.6%CABMR)增加了共识。使用这些结果建模表明,个体评分的差异可能会影响CABMR的模拟研究中的结果评估。我们得出结论,班夫架构具有高度变化,多数规则方法可用于裁定病理学家之间的差异,并降低临床试验中得分的变化。

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