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高血压患者表现出代谢改变。尿液中的特定代谢物特征能够预测蛋白尿的进展。

Hypertensive patients exhibit an altered metabolism. A specific metabolite signature in urine is able to predict albuminuria progression.

作者信息

Gonzalez-Calero Laura, Martin-Lorenzo Marta, Martínez Paula J, Baldan-Martin Montserrat, Ruiz-Hurtado Gema, Segura Julian, de la Cuesta Fernando, Barderas Maria G, Ruilope Luis M, Vivanco Fernando, Alvarez-Llamas Gloria

机构信息

Departamento de Inmunologia, IIS-Fundacion Jimenez Diaz, UAM, Madrid, Spain.

Laboratorio de Fisiopatologia Vascular, Hospital Nacional de Paraplejicos SESCAM, Toledo, Spain.

出版信息

Transl Res. 2016 Dec;178:25-37.e7. doi: 10.1016/j.trsl.2016.07.003. Epub 2016 Jul 15.

Abstract

Hypertension (HTN) is increasing in prevalence, and albuminuria is a strong indicator of cardiovascular risk and renal damage progression. Despite blood pressure control with chronic treatment, a relevant subgroup of patients develop albuminuria. However, the biological factors responsible for albuminuria development and progression are underexplored. We aimed to identify key metabolic targets and biological pathways involved in the negative progression of cardiovascular and renal damage in hypertensives undergoing chronic treatment. A series of 1533 patients were followed for 5 years to investigate the evolution of albuminuria. Patients were classified as: (1) patients with persistent normoalbuminuria; (2) patients developing de novo albuminuria; and (3) patients with maintained albuminuria. At the end of follow-up, urine from 30 nonhypertensive subjects (control group) and a representative cohort of 118 patients was collected for metabolomic analysis. Metabolic patterns of interest were identified in a first discovery phase by nuclear magnetic resonance and further confirmed by liquid chromatography-mass spectrometry. Metabolites corresponding to HTN or albuminuria were measured in a prospective study carried out in 35 individuals still in normoalbuminuria, to evaluate their potential as predictors of albuminuria development. Nine metabolites were significantly altered, linking β-alanine metabolism, arginine and proline metabolism, and tricarboxylic acid cycle. The prospective study revealed a panel composed of guanidinoacetate, glutamate, and pantothenate, which was able to predict development of albuminuria. These metabolic signatures open new possibilities in hypertensive therapy and cardiovascular risk control, providing prompt and more efficient intervention, particularly in patients with worse cardiovascular prognosis.

摘要

高血压(HTN)的患病率正在上升,蛋白尿是心血管风险和肾脏损害进展的有力指标。尽管通过长期治疗控制了血压,但仍有相当一部分患者出现蛋白尿。然而,导致蛋白尿发生和进展的生物学因素尚未得到充分研究。我们旨在确定接受长期治疗的高血压患者心血管和肾脏损害负面进展中涉及的关键代谢靶点和生物学途径。对1533例患者进行了为期5年的随访,以研究蛋白尿的演变。患者被分为:(1)持续性正常蛋白尿患者;(2)新发蛋白尿患者;(3)持续性蛋白尿患者。随访结束时,收集了30名非高血压受试者(对照组)和118名患者的代表性队列的尿液进行代谢组学分析。在第一个发现阶段通过核磁共振鉴定出感兴趣的代谢模式,并通过液相色谱-质谱进一步确认。在一项对35名仍处于正常蛋白尿状态的个体进行的前瞻性研究中,测量了与高血压或蛋白尿相关的代谢物,以评估它们作为蛋白尿发生预测指标的潜力。9种代谢物发生了显著变化,涉及β-丙氨酸代谢、精氨酸和脯氨酸代谢以及三羧酸循环。前瞻性研究揭示了一个由胍基乙酸盐、谷氨酸和泛酸盐组成的组合,它能够预测蛋白尿的发生。这些代谢特征为高血压治疗和心血管风险控制开辟了新的可能性,提供了及时且更有效的干预措施,特别是对于心血管预后较差的患者。

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