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一种新型综合衰老过程的检测表明存在复杂的生理整合。

Detection of a novel, integrative aging process suggests complex physiological integration.

作者信息

Cohen Alan A, Milot Emmanuel, Li Qing, Bergeron Patrick, Poirier Roxane, Dusseault-Bélanger Francis, Fülöp Tamàs, Leroux Maxime, Legault Véronique, Metter E Jeffrey, Fried Linda P, Ferrucci Luigi

机构信息

Groupe de recherche PRIMUS, Department of Family Medicine, University of Sherbrooke, 3001 12e Ave N, Sherbrooke, QC, J1H 5N4, Canada.

Department of Chemistry, Biochemistry and Physics, Université du Québec à Trois-Rivières, 3351, boul. des Forges, C.P. 500, Trois-Rivières, QC, G9A 5H7, Canada.

出版信息

PLoS One. 2015 Mar 11;10(3):e0116489. doi: 10.1371/journal.pone.0116489. eCollection 2015.

Abstract

Many studies of aging examine biomarkers one at a time, but complex systems theory and network theory suggest that interpretations of individual markers may be context-dependent. Here, we attempted to detect underlying processes governing the levels of many biomarkers simultaneously by applying principal components analysis to 43 common clinical biomarkers measured longitudinally in 3694 humans from three longitudinal cohort studies on two continents (Women's Health and Aging I & II, InCHIANTI, and the Baltimore Longitudinal Study on Aging). The first axis was associated with anemia, inflammation, and low levels of calcium and albumin. The axis structure was precisely reproduced in all three populations and in all demographic sub-populations (by sex, race, etc.); we call the process represented by the axis "integrated albunemia." Integrated albunemia increases and accelerates with age in all populations, and predicts mortality and frailty--but not chronic disease--even after controlling for age. This suggests a role in the aging process, though causality is not yet clear. Integrated albunemia behaves more stably across populations than its component biomarkers, and thus appears to represent a higher-order physiological process emerging from the structure of underlying regulatory networks. If this is correct, detection of this process has substantial implications for physiological organization more generally.

摘要

许多关于衰老的研究一次只检测一种生物标志物,但复杂系统理论和网络理论表明,对单个标志物的解读可能取决于背景。在此,我们试图通过对来自两大洲三项纵向队列研究(女性健康与衰老研究I和II、InCHIANTI以及巴尔的摩纵向衰老研究)的3694名人类纵向测量的43种常见临床生物标志物应用主成分分析,来同时检测控制多种生物标志物水平的潜在过程。第一轴与贫血、炎症以及钙和白蛋白水平低有关。轴结构在所有三个人群以及所有人口统计学亚群(按性别、种族等)中都得到了精确再现;我们将该轴所代表的过程称为“综合白蛋白血症”。在所有人群中,综合白蛋白血症都随年龄增长且加速,并且即使在控制年龄后,也能预测死亡率和虚弱程度——但不能预测慢性病。这表明其在衰老过程中发挥作用,尽管因果关系尚不清楚。综合白蛋白血症在不同人群中的表现比其组成生物标志物更稳定,因此似乎代表了一种从潜在调节网络结构中浮现的高阶生理过程。如果这是正确的,那么检测到这个过程对更普遍的生理组织具有重大意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/194a/4356614/425689b49086/pone.0116489.g001.jpg

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