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血浆gelsolin 与 80 岁以上社区居住男性虚弱表型和死亡率的关系:一项队列研究。

Association of plasma gelsolin with frailty phenotype and mortality among octogenarian community-dwelling men: a cohort study.

机构信息

Helsinki University Hospital, HUS, University of Helsinki, PO Box 340, FI-00029, Helsinki, Finland.

Center for Life Course Health Research, University of Oulu, Oulu, Finland.

出版信息

Aging Clin Exp Res. 2022 May;34(5):1095-1101. doi: 10.1007/s40520-022-02083-2. Epub 2022 Feb 15.

Abstract

BACKGROUND

Biomarkers are needed for frailty, a common phenotype often associated with muscle loss in older people. Plasma gelsolin (pGSN) is a protein largely synthesized and secreted by skeletal muscle.

AIMS

To investigate whether pGSN could be a biomarker of the frailty phenotype and predict mortality.

METHODS

A homogenous cohort of males (born 1919-1934, baseline n = 3490) has been followed since the 1960s. In 2010/11, frailty phenotypes by modified Fried criteria were assessed. pGSN was measured in a convenience subset (n = 469, mean age 83) and re-measured in survivors (n = 127) in 2017. Mortality through December 31, 2018 was retrieved from national registers. Regression models were used for analyses.

RESULTS

Of 469 males, 152 (32.4%) were robust, 284 (60.6%) prefrail, and 33 (7.0%) frail in 2010/11. There was a graded (p = 0.018) association between pGSN (mean 58.1 ug/mL, SD 9.3) and frailty. After multivariable adjustment, higher pGSN levels were associated with lower odds of having contemporaneous phenotypic prefrailty (OR per 1 SD 0.73, 95% CI 0.58-0.92) and frailty (OR per 1 SD 0.70, 95% CI 0.44-1.11). By 2018, 179 males (38.2%) had died, and higher baseline pGSN predicted a lower 7-year mortality rate (HR per 1 SD 0.85, 95% CI 0.72-1.00). pGSN concentrations in 2010/11 and 2017 were correlated (n = 127, r = 0.34, p < 0.001).

DISCUSSION

Higher baseline pGSN concentrations were associated with a persistently robust phenotype and lower mortality rate over 7 years in a cohort of octogenarian males with high socioeconomic status and may be a promising laboratory biomarker for the development of a frailty phenotype.

摘要

背景

生物标志物是虚弱的需要,虚弱是一种常见的表型,通常与老年人的肌肉丧失有关。血浆凝溶胶蛋白(pGSN)是一种主要由骨骼肌合成和分泌的蛋白质。

目的

研究 pGSN 是否可以作为虚弱表型的生物标志物并预测死亡率。

方法

自 20 世纪 60 年代以来,一直对一组同质的男性(出生于 1919-1934 年,基线 n=3490)进行随访。在 2010/11 年,根据改良的 Fried 标准评估了虚弱表型。在便利样本(n=469,平均年龄 83 岁)中测量了 pGSN,并在幸存者(n=127)中于 2017 年重新测量了 pGSN。通过国家登记册检索 2018 年 12 月 31 日之前的死亡率。使用回归模型进行分析。

结果

在 469 名男性中,有 152 名(32.4%)身体健壮,284 名(60.6%)为虚弱前期,33 名(7.0%)为虚弱(2010/11 年)。pGSN(平均 58.1 ug/mL,SD 9.3)与虚弱呈梯度(p=0.018)相关。经过多变量调整后,较高的 pGSN 水平与同时具有虚弱前期表型的可能性较低相关(每 SD 1 个标准差的比值为 0.73,95%CI 为 0.58-0.92)和虚弱(每 SD 1 个标准差的比值为 0.70,95%CI 为 0.44-1.11)。到 2018 年,有 179 名男性(38.2%)死亡,较高的基线 pGSN 预测 7 年死亡率较低(每 SD 1 个标准差的 HR 为 0.85,95%CI 为 0.72-1.00)。2010/11 年和 2017 年的 pGSN 浓度相关(n=127,r=0.34,p<0.001)。

讨论

在具有高社会经济地位的 80 岁以上男性队列中,较高的基线 pGSN 浓度与持续强健的表型相关,并且在 7 年内死亡率较低,这可能是虚弱表型发展的有前途的实验室生物标志物。

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