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网络动力学稳定性分析揭示了关键的“失衡”自然变量,这些变量侵蚀了体内平衡并导致与年龄相关的健康衰退。

Network dynamical stability analysis reveals key "mallostatic" natural variables that erode homeostasis and drive age-related decline of health.

机构信息

Department of Physics and Atmospheric Science, Dalhousie University, Halifax, NS, B3H 4R2, Canada.

出版信息

Sci Rep. 2023 Dec 13;13(1):22140. doi: 10.1038/s41598-023-49129-7.

Abstract

Using longitudinal study data, we dynamically model how aging affects homeostasis in both mice and humans. We operationalize homeostasis as a multivariate mean-reverting stochastic process. We hypothesize that biomarkers have stable equilibrium values, but that deviations from equilibrium of each biomarker affects other biomarkers through an interaction network-this precludes univariate analysis. We therefore looked for age-related changes to homeostasis using dynamic network stability analysis, which transforms observed biomarker data into independent "natural" variables and determines their associated recovery rates. Most natural variables remained near equilibrium and were essentially constant in time. A small number of natural variables were unable to equilibrate due to a gradual drift with age in their homeostatic equilibrium, i.e. allostasis. This drift caused them to accumulate over the lifespan course and makes them natural aging variables. Their rate of accumulation was correlated with risk of adverse outcomes: death or dementia onset. We call this tendency for aging organisms to drift towards an equilibrium position of ever-worsening health "mallostasis". We demonstrate that the effects of mallostasis on observed biomarkers are spread out through the interaction network. This could provide a redundancy mechanism to preserve functioning until multi-system dysfunction emerges at advanced ages.

摘要

利用纵向研究数据,我们动态地模拟了衰老如何影响小鼠和人类的体内平衡。我们将体内平衡操作化为一个多变量均值回复随机过程。我们假设生物标志物具有稳定的平衡值,但每个生物标志物的平衡偏差会通过相互作用网络影响其他生物标志物——这排除了单变量分析。因此,我们使用动态网络稳定性分析来寻找与体内平衡相关的年龄变化,该分析将观察到的生物标志物数据转换为独立的“自然”变量,并确定它们的相关恢复率。大多数自然变量接近平衡,并且在时间上基本保持不变。由于其体内平衡的动态平衡随着年龄的增长而逐渐漂移,即适应,一小部分自然变量无法达到平衡。这种漂移导致它们在整个生命周期中积累,并使它们成为自然老化变量。它们的积累速度与不良后果的风险(死亡或痴呆发作)相关。我们称生物体向健康状况不断恶化的平衡位置漂移的这种趋势为“mallostasis”。我们证明,mallostasis 对观察到的生物标志物的影响通过相互作用网络传播。这可能提供了一种冗余机制,以在多系统功能障碍出现在高龄之前保持功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b327/10719307/d26afe41ae96/41598_2023_49129_Fig1_HTML.jpg

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