临床稳定期威尔逊氏病患者的非血浆铜和尿铜:与推荐目标一致

IF 9.5 1区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY
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引用次数: 0

摘要

背景& 目的威尔逊病(WD)主要是由于铜在肝脏和大脑中蓄积所致。在使用D-青霉胺维持治疗WD期间,现行指南建议治疗期间的尿铜排泄量(UCE)范围为200-500 μg/24小时,血清非结合铜(NCC)范围为50-150 μg/L。我们比较了接受D-青霉胺治疗的临床稳定型WD患者的NCC(通过两种新型测定法测定)和UCE与这些建议的差异。方法这是对螯合试验(NCT03539952)数据的二次分析,该试验招募了医生选定的接受D-青霉胺维持治疗(剂量不变至少4个月)的临床稳定型WD患者。我们分析了干预前首次筛查的实验室样本。NCC通过阴离子交换高效液相色谱蛋白质标样法(NCC-Sp)进行测定,然后通过电感耦合等离子体质谱法进行铜测定,或者通过可交换铜(NCC-Ex)进行测定。结果在平均治疗年数为 21.3±14.3 年的 76 位 WD 患者中,分别有 61% 和 54% 的患者的 NCC-Sp(平均值±SD:56.6±26.2 μg/L)和 NCC-Ex(平均值±SD:57.9±24.7 μg/L)在 50-150 μg/L 的目标值范围内。此外,分别有 36% 和 31% 的患者甚至低于正常范围(NCC-Sp:46-213 μg/L,NCC-Ex:41-71 μg/L)。NCC-Ex 与 NCC-Sp 呈正相关(r2 = 0.66,p <0.001),但存在系统性偏差。58% 的 UCE 超出了 200-500 μg/24 h 的目标范围。只有 14/69 人(20%)同时达到了 NCC-Sp 和 UCE 的目标。结论接受D-青霉胺维持治疗的临床病情稳定的WD患者的NCC-Sp或UCE经常低于目前的建议值或高于建议值,但没有过度治疗的迹象。影响和意义:目前,对威尔逊病患者(WD)的螯合剂治疗是通过测量非甘油脂结合铜(NCC)和24小时尿铜排泄量(UCE)来指导的,但其有效性有限。在76名有≈21年WD治疗史且接受D-青霉胺治疗后病情临床稳定的成年人中,无论是通过蛋白质分型(NCC-Sp)还是可交换铜(NCC-Ex)测量,NCC普遍低于正常值和推荐的目标范围,而49%的人的UCE值高于推荐的目标范围。按照常理,这些病例应接受过度治疗,但临床或生化指标均未发现铜缺乏症。对肝酶的探索性分析表明,低于对照组水平的 NCC 可能是有益的,而与 UCE 的关系则不太明确。这些数据要求对治疗 WD 的目标范围进行重要的重新评估,特别是针对药物和实验室方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Non-ceruloplasmin copper and urinary copper in clinically stable Wilson disease: Alignment with recommended targets

Non-ceruloplasmin copper and urinary copper in clinically stable Wilson disease: Alignment with recommended targets

Background & Aims

Wilson disease (WD) is caused by accumulation of copper primarily in the liver and brain. During maintenance therapy of WD with D-penicillamine, current guidelines recommend on-treatment ranges of urinary copper excretion (UCE) of 200-500 μg/24 h and serum non-ceruloplasmin-bound copper (NCC) of 50-150 μg/L. We compared NCC (measured by two novel assays) and UCE from patients with clinically stable WD on D-penicillamine therapy with these recommendations.

Methods

This is a secondary analysis of data from the Chelate trial (NCT03539952) that enrolled physician-selected patients with clinically stable WD on D-penicillamine maintenance therapy (at an unaltered dose for at least 4 months). We analyzed laboratory samples from the first screening visit, prior to interventions. NCC was measured by either protein speciation (NCC-Sp) using anion exchange high-performance liquid chromatography protein speciation followed by copper determination with inductively coupled plasma mass spectroscopy or as exchangeable copper (NCC-Ex). NCC-Sp was also analyzed in healthy controls (n = 75).

Results

In 76 patients with WD with 21.3±14.3 average treatment-years, NCC-Sp (mean±SD: 56.6±26.2 μg/L) and NCC-Ex (mean±SD: 57.9±24.7 μg/L) were within the 50-150 μg/L target in 61% and 54% of patients, respectively. In addition, 36% and 31%, respectively, were even below the normal ranges (NCC-Sp: 46-213 μg/L, NCC-Ex: 41-71 μg/L). NCC-Ex positively correlated with NCC-Sp (r2 = 0.66, p <0.001) but with systematic deviation. UCE was outside the 200-500 μg/24 h target range in 58%. Only 14/69 (20%) fulfilled both the NCC-Sp and UCE targets. Clinical or biochemical signs of copper deficiency were not detected.

Conclusion

Clinically stable patients with WD on maintenance D-penicillamine therapy frequently have lower NCC-Sp or higher UCE than current recommendations without signs of overtreatment. Further studies are warranted to identify appropriate target ranges of NCC-Sp, NCC-Ex and UCE in treated WD.

Impact and implications:

Chelator treatment of patients with Wilson disease (WD) is currently guided by measurements of non-ceruloplasmin-bound copper (NCC) and 24 h urinary copper excretion (UCE) but validation is limited. In 76 adults with ≈21 years history of treated WD and clinically stable disease on D-penicillamine therapy, NCC was commonly found to be below normal values and recommended target ranges whether measured by protein speciation (NCC-Sp) or as exchangeable copper (NCC-Ex), while UCE values were above the recommended target range in 49%. Common wisdom would suggest overtreatment in these cases, but no clinical or biochemical signs of copper deficiency were observed. Exploratory analysis of liver enzymes suggested that NCC below levels seen in controls may be beneficial, while the relation to UCE was less clear. The data calls for critical re-evaluation of target ranges for treatment of WD, specific for drug and laboratory methodology.

Clinical trial number

(NCT03539952)

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来源期刊
JHEP Reports
JHEP Reports GASTROENTEROLOGY & HEPATOLOGY-
CiteScore
12.40
自引率
2.40%
发文量
161
审稿时长
36 days
期刊介绍: JHEP Reports is an open access journal that is affiliated with the European Association for the Study of the Liver (EASL). It serves as a companion journal to the highly respected Journal of Hepatology. The primary objective of JHEP Reports is to publish original papers and reviews that contribute to the advancement of knowledge in the field of liver diseases. The journal covers a wide range of topics, including basic, translational, and clinical research. It also focuses on global issues in hepatology, with particular emphasis on areas such as clinical trials, novel diagnostics, precision medicine and therapeutics, cancer research, cellular and molecular studies, artificial intelligence, microbiome research, epidemiology, and cutting-edge technologies. In summary, JHEP Reports is dedicated to promoting scientific discoveries and innovations in liver diseases through the publication of high-quality research papers and reviews covering various aspects of hepatology.
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