Co-expression analysis identifies networks of miRNAs implicated in biological ageing and modulated by short-term interval training
Adult
Male
Aging
0303 health sciences
WGCNA
Gene Expression Profiling
Telomere Homeostasis
High-Intensity Interval Training
Regulatory Sequences, Ribonucleic Acid
796
Healthy Aging
MicroRNAs
03 medical and health sciences
Physical Fitness
telomere length
Leukocytes
Humans
Female
gene
exercise training
Exercise
small non-coding RNA
Signal Transduction
DOI:
10.1016/j.mad.2021.111552
Publication Date:
2021-08-05T10:01:26Z
AUTHORS (6)
ABSTRACT
Exercise training seems to promote healthy biological ageing partly by inducing telomere maintenance, yet the molecular mechanisms are not fully understood. Recent studies have emphasised the importance of microRNAs (miRNAs) in ageing and their ability to mirror pathophysiological alterations associated with age-related diseases. We examined the association between aerobic fitness and leukocyte telomere length before determining the influence of vigorous exercise training on the regulation of leukocyte miRNA networks. Telomere length was positively correlated to aerobic fitness (r = 0.32, p = 0.02). 104 miRNAs were differentially expressed after six weeks of thrice-weekly sprint interval training (SIT) in healthy men (q < 0.05). Gene co-expression analysis (WGCNA) detected biologically meaningful miRNA networks, five of which were significantly correlated with pre-SIT and post-SIT expression profiles (p < 0.001) and telomere length. Enrichment analysis revealed that the immune response, T cell differentiation and lipid metabolism associated miRNAs clusters were significantly down-regulated after SIT. Using data acquired from the Gene Expression Omnibus (GEO), we also identified two co-expressed miRNAs families that were modulated by exercise training in previous investigations. Collectively, our findings highlight the miRNA networks implicated in exercise adaptations and telomere regulation, and suggest that SIT may attenuate biological ageing through the control of the let-7 and miR-320 miRNA families.
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CITATIONS (6)
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