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法国FRAILOMIC计划队列中血浆3-甲基组氨酸与衰弱状态的关联。

Associations of Plasma 3-Methylhistidine with Frailty Status in French Cohorts of the FRAILOMIC Initiative.

作者信息

Kochlik Bastian, Stuetz Wolfgang, Pérès Karine, Féart Catherine, Tegner Jesper, Rodriguez-Mañas Leocadio, Grune Tilman, Weber Daniela

机构信息

Department of Molecular Toxicology, German Institute of Human Nutrition Potsdam-Rehbruecke (DIfE), 14558 Nuthetal, Germany.

NutriAct-Competence Cluster Nutrition Research Berlin-Potsdam, 14558 Nuthetal, Germany.

出版信息

J Clin Med. 2019 Jul 10;8(7):1010. doi: 10.3390/jcm8071010.

Abstract

Frailty and sarcopenia are characterized by a loss of muscle mass and functionality and are diagnosed mainly by functional tests and imaging parameters. However, more muscle specific biomarkers are needed to improve frailty diagnosis. Plasma 3-methylhistidine (3-MH), as well as the 3-MH-to-creatinine (3-MH/Crea) and 3-MH-to-estimated glomerular filtration rate (3-MH/eGFR) ratios might support the diagnosis of frailty. Therefore, we investigated the cross-sectional associations between plasma 3-MH, 3-MH/Crea and 3-MH/eGFR with the frailty status of community-dwelling individuals (>65 years). 360 participants from two French cohorts of the FRAILOMIC initiative were classified into robust, pre-frail and frail according to Fried's frailty criteria. General linear models as well as bivariate and multiple linear and logistic regression models, which were adjusted for several confounders, were applied to determine associations between biomarkers and frailty status. The present study consisted of 37.8% robust, 43.1% pre-frail and 19.2% frail participants. Frail participants had significantly higher plasma 3-MH, 3-MH/Crea and 3-MH/eGFR ratios than robust individuals, and these biomarkers were positively associated with frailty status. Additionally, the likelihood to be frail was significantly higher for every increase in 3-MH (1.31-fold) and 3-MH/GFR (1.35-fold) quintile after adjusting for confounders. We conclude that 3-MH, 3-MH/Crea and 3-MH/eGFR in plasma might be potential biomarkers to identify frail individuals or those at higher risk to be frail, and we assume that there might be biomarker thresholds to identify these individuals. However, further, especially longitudinal studies are needed.

摘要

衰弱和肌肉减少症的特征是肌肉质量和功能丧失,主要通过功能测试和成像参数进行诊断。然而,需要更多肌肉特异性生物标志物来改善衰弱诊断。血浆3-甲基组氨酸(3-MH)以及3-甲基组氨酸与肌酐的比值(3-MH/Crea)和3-甲基组氨酸与估计肾小球滤过率的比值(3-MH/eGFR)可能有助于衰弱的诊断。因此,我们研究了血浆3-MH、3-MH/Crea和3-MH/eGFR与社区居住个体(>65岁)衰弱状态之间的横断面关联。来自法国FRAILOMIC倡议的两个队列的360名参与者根据弗里德衰弱标准被分为强壮、衰弱前期和衰弱。应用一般线性模型以及经多种混杂因素调整的双变量和多变量线性及逻辑回归模型来确定生物标志物与衰弱状态之间的关联。本研究包括37.8%的强壮参与者、43.1%的衰弱前期参与者和19.2%的衰弱参与者。衰弱参与者的血浆3-MH、3-MH/Crea和3-MH/eGFR比值显著高于强壮个体,这些生物标志物与衰弱状态呈正相关。此外,在调整混杂因素后,3-MH(1.31倍)和3-MH/GFR(1.35倍)每增加一个五分位数,衰弱的可能性就显著更高。我们得出结论,血浆中的3-MH、3-MH/Crea和3-MH/eGFR可能是识别衰弱个体或衰弱风险较高个体的潜在生物标志物,并且我们假设可能存在识别这些个体的生物标志物阈值。然而,还需要进一步的研究,尤其是纵向研究。

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