Transcriptomic analyses of peripheral blood mononuclear cells reveal age-specific basal and acute exercise responsiveness differences in humans.

IF 3.1 2区医学 Q1 ENDOCRINOLOGY & METABOLISM

American journal of physiology. Endocrinology and metabolism Pub Date : 2025-08-01 Epub Date: 2025-07-22 DOI:10.1152/ajpendo.00169.2025

Bradley A Ruple, Nicholas A Carlini, Jason S Kofoed, Helya Rostamkhani, Brady E Hanson, Isaac Wilcox, Jesse C Craig, Shelby C Osburn, Micah J Drummond, Ryan M Broxterman, Joel D Trinity

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引用次数: 0

Abstract

Aging is associated with alterations in immune cell function, contributing to age-related diseases and frailty. As peripheral blood mononuclear cells (PBMCs) are key drivers of the immune response, we investigated their transcriptome using RNA-sequencing before and immediately after a single bout of high-intensity knee-extension exercise in young (young; n = 7, 23 ± 4 yr) and older individuals (old; n = 8, 65 ± 7 yr). We used bioinformatics analyses to identify the biological processes and pathways that may be altered with age and in response to acute exercise. At baseline, 665 genes differed between young and old, with notable differences in pathways involved in DNA damage/telomere stress-induced senescence, NAD signaling pathway, and oxidative stress-induced senescence. After the exercise bout, 53 genes were differentially expressed in young, whereas 1,026 genes changed in old. In young, the enriched processes and predicted pathways were linked to natural killer cells, whereas in old, these pathways were associated with cell signaling immune responses. Finally, 26 genes exhibited similar responses to exercise between groups, enriching the biological process of natural killer cell-mediated immunity regulation. Our findings indicate that PBMC gene expression and the response to acute exercise are altered with aging, where exercise induces more pronounced PBMC transcriptomic adaptations in the old. In addition, although aging is associated with increased expression of genes linked to cellular dysfunction and suppressed immune function, acute exercise attenuated these age-related differences by downregulating the genes related to those pathways. Finally, acute exercise activated similar immune-related pathways in both age groups.NEW & NOTEWORTHY This study demonstrates that aging alters the transcriptional landscape of PBMCs at rest and in response to acute high-intensity exercise. Older adults exhibited greater transcriptomic responsiveness to exercise, particularly in pathways related to immune signaling and cellular stress. Notably, exercise elicited shared activation of NK cell-mediated processes across age groups, suggesting a conserved immunomodulatory effect. These findings provide molecular insight into how aging and exercise interact to shape immune cell function.

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外周血单个核细胞的转录组学分析揭示了人类年龄特异性基础和急性运动反应性差异。

衰老与免疫细胞功能的改变有关，从而导致与年龄有关的疾病和虚弱。由于外周血单核细胞（PBMCs）是免疫反应的关键驱动因素，我们使用rna测序研究了他们的转录组，在单次高强度膝关节伸展运动之前和之后。n=7, 23±4岁)和老年个体(Old；N =8, 65±7年)。我们使用生物信息学分析来确定可能随着年龄和急性运动而改变的生物过程和途径。在基线时，665个基因在年轻人和老年人之间存在差异，其中DNA损伤/端粒应激诱导衰老的途径、NAD信号通路和氧化应激诱导衰老的途径存在显著差异。运动后，53个基因在Young中表达不同，而1026个基因在Old中表达不同。在Young中，富集的过程和预测的途径与自然杀伤细胞有关，而在Old中，这些途径与细胞信号免疫反应有关。最后，26个基因对运动表现出相似的反应，丰富了自然杀伤细胞介导的免疫调节的生物学过程。我们的研究结果表明，PBMC基因表达和对急性运动的反应随着年龄的增长而改变，其中运动诱导老年人更明显的PBMC转录组适应。此外，虽然衰老与细胞功能障碍和免疫功能抑制相关基因的表达增加有关，但急性运动通过下调与这些途径相关的基因来减弱这些与年龄相关的差异。最后，急性运动在两个年龄组中激活了相似的免疫相关途径。

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来源期刊

American journal of physiology. Endocrinology and metabolism 医学-内分泌学与代谢

CiteScore

9.80

自引率

0.00%

发文量

审稿时长

1 months

期刊介绍： The American Journal of Physiology-Endocrinology and Metabolism publishes original, mechanistic studies on the physiology of endocrine and metabolic systems. Physiological, cellular, and molecular studies in whole animals or humans will be considered. Specific themes include, but are not limited to, mechanisms of hormone and growth factor action; hormonal and nutritional regulation of metabolism, inflammation, microbiome and energy balance; integrative organ cross talk; paracrine and autocrine control of endocrine cells; function and activation of hormone receptors; endocrine or metabolic control of channels, transporters, and membrane function; temporal analysis of hormone secretion and metabolism; and mathematical/kinetic modeling of metabolism. Novel molecular, immunological, or biophysical studies of hormone action are also welcome.