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Alkaline phosphatase at diagnosis of primary sclerosing cholangitis and 1 year later: evaluation of prognostic value

机译:碱性磷酸酶在原发性硬化性胆管炎和一年后的诊断:预后价值评估

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Background: Primary sclerosing cholangitis (PSC) is a slowly progressive liver disease. Reliable biomarkers to predict outcome are urgently needed to serve as surrogate endpoints and/or stratifiers in clinical trials. Reduction in serum alkaline phosphatase (ALP) has been proposed as prognostic surrogate marker in PSC. The aim of this study was to asses if ALP at diagnosis (T0), 1 year later (T1), and percentage change between both time points hold prognostic value, and to determine the optimal threshold. Methods: We retrospectively collected ALP levels at T0 and T1 for patients included in a large PSC cohort. The association of ALP at T0, T1, and percentage change with the combined endpoint (PSC-related death, liver transplantation) was analysed. Predictive value was determined using C-statistics. Results: A total of 366 patients were included, of whom 66 (18%) reached an endpoint: 26 (7%) PSC-related death, 40 (11%) liver transplantation. At T0 and T1, 84% used ursodeoxycholic acid. A positive association was observed between level of ALP at T0 and T1 and the hazard of reaching an endpoint, up to values around 2.5 times upper limit of normal (xULN). A larger decrease in ALP between T0 and T1 decreased the event rate. A range of thresholds (0.5-3xULN) with about similar C-statistics was found. In this cohort, the optimal threshold was 1.3xULN at T1. Conclusion: ALP can be used to discriminate between PSC patients with a good and a poor prognosis. These findings indicate that ALP can serve as stratifier, and potentially as surrogate endpoint for clinical trials in PSC.
机译:背景:原发性硬化性胆管炎(PSC)是一种缓慢进行性肝病。迫切需要可靠的生物标志物来预测结果,以作为临床试验中的替代终点和/或分层剂。有人提出降低血清碱性磷酸酶(ALP)作为PSC中的预后替代指标。这项研究的目的是评估ALP诊断(T0),一年后(T1)以及两个时间点之间的百分比变化是否具有预后价值,并确定最佳阈值。方法:我们回顾性地收集了大型PSC队列中患者的T0和T1时的ALP水平。分析了T0,T1处的ALP和百分比变化与合并终点(PSC相关的死亡,肝移植)的相关性。使用C统计量确定预测值。结果:共纳入366例患者,其中66例(18%)达到终点:PSC相关死亡26例(7%),肝移植40例(11%)。在T0和T1,有84%使用熊去氧胆酸。在T0和T1处的ALP水平与达到终点的危险之间存在正相关,直至达到正常上限(xULN)的2.5倍。 T0和T1之间的ALP大幅降低会降低事件发生率。发现了一系列阈值(0.5-3xULN),具有近似的C统计量。在该队列中,T1的最佳阈值为1.3xULN。结论:ALP可用于区分预后良好和不良的PSC患者。这些发现表明,ALP可以作为分层剂,并有可能作为PSC临床试验的替代终点。

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