常染色体显性遗传多囊肾病的影像学识别:托伐普坦的简单入选标准。
Imaging Identification of Rapidly Progressing Autosomal Dominant Polycystic Kidney Disease: Simple Eligibility Criterion for Tolvaptan.
机构信息
Department of Hereditary Kidney Disease Research, Kyorin University School of Medicine, Tokyo, Japan,
Department of Urology, Kyorin University School of Medicine, Tokyo, Japan,
出版信息
Am J Nephrol. 2020;51(11):881-890. doi: 10.1159/000511797. Epub 2020 Nov 23.
BACKGROUND
Tolvaptan was approved for the treatment of autosomal dominant polycystic kidney disease (ADPKD). However, the official indication of "rapidly progressive disease" is described differently in the clinical guidelines. We aim to define "rapidly progressive disease" by risk of ESRD, which is evaluated using estimated height-adjusted total kidney volume (HtTKV) growth rate.
METHODS
The risk of ESRD was retrospectively analyzed in 617 initially non-ESRD adults with ADPKD and observed with standard of care between 2007 and 2018. The estimated annual growth rate of the HtTKV, termed as eHTKV-α (%/year), is derived from the following equation: [HtTKV at age t] = K(1 + eHTKV-α/100)t, where K = 150 mL/m is used in Mayo Imaging Classification and K = 130 mL/m is proposed for individually stable eHTKV-α value from baseline. The accuracy of eHTKV-α to predict ESRD for censored ages was analyzed using time-dependent receiver-operating characteristic curves (ROC). The cutoff point of initially measured eHTKV-α to predict ESRD was assessed using Kaplan-Meier and Cox's proportional hazards models. Performance characteristics of the cutoff point for censored ages were calculated using time-dependent ROC and validated by the bootstrap method.
RESULTS
The area under the time-dependent ROC of eHTKV-α to predict ESRD at age 65 was 0.89 ± 0.04 (K = 130). The mean renal survival was less than 70 years at eHTKV-α ≥4.0%/year (K = 130). Mean renal survival was approximately 12 years shorter, and hazard ratio of ESRD was more than 5-time higher at this cutoff point than at lower point. Time-dependent sensitivity for age 65 and cutoff point of 4.0%/year (K = 130) was 93.4 ± 0.3%. Between cutoff points ≥4.0%/year (K = 130) and ≥3.5%/year (K = 150), there was no significant difference in performance characteristics and accuracy to predict ESRD.
CONCLUSION
eHTKV-α well predicts ESRD. Initially, measured eHTKV-α ≥4.0%/year (K = 130) defines high-risk ESRD. Without additional conditions, a single eHTKV-α cutoff point identifies subjects that are most likely to benefit from tolvaptan.
背景
托伐普坦获批用于治疗常染色体显性多囊肾病(ADPKD)。然而,临床指南中对“快速进展性疾病”的官方描述有所不同。我们旨在通过估算的身高校正总肾体积(HtTKV)增长率来评估终末期肾病(ESRD)风险,从而定义“快速进展性疾病”。
方法
回顾性分析了 2007 年至 2018 年期间 617 名初诊非 ESRD 的 ADPKD 成年患者的 ESRD 风险,这些患者接受了标准治疗。从以下公式中得出估算的 HtTKV 年增长率,即 eHTKV-α(%/年):[年龄 t 时的 HtTKV] = K(1 + eHTKV-α/100)t,其中 K = 150 mL/m 用于 Mayo 影像学分类,K = 130 mL/m 用于从基线开始稳定的个体 eHTKV-α 值。使用时间依赖性接收者操作特征曲线(ROC)分析 eHTKV-α 预测 ESRD 年龄的准确性。使用 Kaplan-Meier 和 Cox 比例风险模型评估初始测量的 eHTKV-α 预测 ESRD 的截止值。使用时间依赖性 ROC 和 bootstrap 方法验证评估截点在censored 年龄的性能特征。
结果
eHTKV-α 预测 ESRD 年龄 65 岁的时间依赖性 ROC 曲线下面积为 0.89 ± 0.04(K = 130)。eHTKV-α≥4.0%/年(K = 130)时,平均肾脏生存时间不到 70 年。在该截点处,肾脏生存率比在较低截点处短约 12 年,ESRD 的风险比超过 5 倍。年龄 65 岁和 4.0%/年(K = 130)的时间依赖性灵敏度为 93.4 ± 0.3%。在截点≥4.0%/年(K = 130)和≥3.5%/年(K = 150)之间,预测 ESRD 的性能特征和准确性没有显著差异。
结论
eHTKV-α 可很好地预测 ESRD。初测 eHTKV-α≥4.0%/年(K = 130)定义为 ESRD 高危。没有其他条件,单一的 eHTKV-α 截止点可以确定最有可能从托伐普坦获益的患者。
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