血清 copeptin 是常染色体显性多囊肾病的可调节生物标志物吗?

Moomal Tasneem, Carly Mannix, Annette Wong, Jennifer Zhang, Gopala Rangan
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摘要

随着用于治疗常染色体显性多囊肾病(ADPKD)的改变病情药物的出现,人们对准确预测该病肾脏预后和/或治疗反应的需求日益迫切。精氨酸加压素(AVP)是决定 ADPKD 患者出生后肾囊肿生长的关键因素。Copeptin(前体 AVP 肽的 C 端糖蛋白)是 AVP 释放的精确替代标记物,它既稳定又易于用免疫测定法测量。队列研究显示,血清 copeptin 与 ADPKD 的疾病严重程度相关,并可预测未来的肾脏事件[肾功能下降和肾脏总容量 (TKV) 增加]。然而,血清 copeptin 与肌酐密切相关,其作为预后生物标志物的额外价值还不确定是否超过估计肾小球滤过率和 TKV。也有人认为,肝素肽可以作为一种预测性生物标志物,用于选择最有可能从改变 AVP 的疗法中获益的 ADPKD 患者,但需要前瞻性数据来验证这一假设。在这方面,评估规定的水摄入量对肾囊肿生长的影响的长期随机临床试验可能有助于解决这一假设。总之,尽管血清 copeptin 与 ADPKD 的基本发病机制一致,但仍需要进一步的严格研究来确定它是否有助于为 ADPKD 患者提供个性化治疗。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Is serum copeptin a modifiable biomarker in autosomal dominant polycystic kidney disease?

The availability of disease-modifying drugs for the management of autosomal dominant polycystic kidney disease (ADPKD) has accelerated the need to accurately predict renal prognosis and/or treatment response in this condition. Arginine vasopressin (AVP) is a critical determinant of postnatal kidney cyst growth in ADPKD. Copeptin (the C-terminal glycoprotein of the precursor AVP peptide) is an accurate surrogate marker of AVP release that is stable and easily measured by immunoassay. Cohort studies show that serum copeptin is correlated with disease severity in ADPKD, and predicts future renal events [decline in renal function and increase in total kidney volume (TKV)]. However, serum copeptin is strongly correlated with creatinine, and its additional value as a prognostic biomarker over estimated glomerular filtration rate and TKV is not certain. It has also been suggested that copeptin could be a predictive biomarker to select ADPKD patients who are most likely to benefit from AVP-modifying therapies, but prospective data to validate this assumption are required. In this regard, long-term randomised clinical trials evaluating the effect of prescribed water intake on renal cyst growth may contribute to addressing this hypothesis. In conclusion, although serum copeptin is aligned with the basic pathogenesis of ADPKD, further rigorous studies are needed to define if it will contribute to enabling the delivery of personalised care in ADPKD.

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