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Sexually Distinct Multi-Omic Responses to Progressive Endurance Exercise Training in the Rat Lung – Findings from MoTrPAC

作者
Gina M. Many,Tyler J. Sagendorf,Hugh Mitchell,James Sanford,Samuel M. Cohen,Ravi Misra,Igor L. Estevao,Ivo Díaz Ludovico,David A. Gaul,Maléne E. Lindholm,Mereena George Ushakumary,James C. Pino,Nicholas Musi,Jia Nie,Facundo M. Fernández,Eric A. Ortlund,Karyn A. Esser,Sue C. Bodine,Simon Schenk,Gérémy Clair
出处
期刊:American Journal of Respiratory Cell and Molecular Biology [American Thoracic Society]
标识
DOI:10.1165/rcmb.2025-0249oc
摘要

Endurance exercise is broadly beneficial to cardiopulmonary function, with these benefits thought to be driven by extrapulmonary factors rather than direct structural changes in the lungs. Thus, to address how endurance exercise training and sex impact molecular responses in the lungs, we used a multi-omics approach to study 6-month-old Fischer 344 rats that undertook a progressive endurance treadmill training protocol for 1 to 8 weeks. Specifically, we reannotated publicly accessible transcriptomics, metabolomics, proteomics and phosphoproteomics data from the Molecular Transducers of Physical Activity Consortium (MoTrPAC) and integrated newly analyzed acetylproteomics data to assess multi-omic sex differences in sedentary and treadmill trained rats. Female rats displayed enrichment in immune-related features and pathways at the transcriptome and proteome level that were largely maintained with training. However, both sexes exhibited decreases in immune pathway activity following 8 weeks of training, although the effect was more pronounced in males. Shared responses to training included increased enrichment in transcriptomic pathways related to type I alveoli, proteomic pathways related to cilia, and decreased acetylation of pathways linked to mitochondrial function. Furthermore, features known to be enriched in lung diseases were attenuated with training in both sexes. Together, our findings provide novel insight into responses to endurance exercise training in the healthy rat lung and may offer translational insight into sex-specific differences in lung disease pathogenesis and treatment.

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