Power training and postmenopausal hormone therapy affect transcriptional control of specific co-regulated gene clusters in skeletal muscle

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RESEARCH PRODUCT

Power training and postmenopausal hormone therapy affect transcriptional control of specific co-regulated gene clusters in skeletal muscle

Paula H. A. Ronkainen Satu O A Koskinen Dennis R. Taaffe Urho M. Kujala Timo Törmäkangas Eija Pöllänen Sulin Cheng Vuokko Kovanen Timo Takala Harri Suominen Vidal Fey Jukka Puolakka Sarianna Sipilä

subject

Aging Candidate gene Transcription Genetic vaihdevuodet menopaussi Bioinformatics Estrogen deprivation 0302 clinical medicine Gene expression estrogen Transcriptional regulation 0303 health sciences Estrogen Replacement Therapy General Medicine Middle Aged estrogeeni Postmenopause medicine.anatomical_structure Female voimaharjoittelu Menopause medicine.symptom Transcriptome-wide study medicine.medical_specialty Plyometric training medicine.drug_class Biology Article transkriptomin laajuuinen tutkimus 03 medical and health sciences plyometrinen harjoittelu Internal medicine medicine Humans Skeletal muscle characteristics KEGG Muscle Skeletal Exercise Gene 030304 developmental biology hormonikorvaushoito Skeletal muscle Muscle weakness deprivaatio Power training Ageing Endocrinology luurankolihakset Hormone replacement therapy Estrogen Geriatrics and Gerontology 030217 neurology & neurosurgery

description

At the moment, there is no clear molecular explanation for the steeper decline in muscle performance after menopause or the mechanisms of counteractive treatments. The goal of this genome-wide study was to identify the genes and gene clusters through which power training (PT) comprising jumping activities or estrogen containing hormone replacement therapy (HRT) may affect skeletal muscle properties after menopause. We used musculus vastus lateralis samples from early stage postmenopausal (50–57 years old) women participating in a yearlong randomized double-blind placebo-controlled trial with PT and HRT interventions. Using microarray platform with over 24,000 probes, we identified 665 differentially expressed genes. The hierarchical clustering method was used to assort the genes. Additionally, enrichment analysis of gene ontology (GO) terms and Kyoto Encyclopedia of Genes and Genomes (KEGG) pathways was carried out to clarify whether assorted gene clusters are enriched with particular functional categories. The analysis revealed transcriptional regulation of 49 GO/KEGG categories. PT upregulated transcription in “response to contraction”—category revealing novel candidate genes for contraction-related regulation of muscle function while HRT upregulated gene expression related to functionality of mitochondria. Moreover, several functional categories tightly related to muscle energy metabolism, development, and function were affected regardless of the treatment. Our results emphasize that during the early stages of the postmenopause, muscle properties are under transcriptional modulation, which both PT and HRT partially counteract leading to preservation of muscle power and potentially reducing the risk for aging-related muscle weakness. More specifically, PT and HRT may function through improving energy metabolism, response to contraction as well as by preserving functionality of the mitochondria. Electronic supplementary material The online version of this article (doi:10.1007/s11357-010-9140-1) contains supplementary material, which is available to authorized users.

year	journal	country	edition	language
2010-01-01	AGE

10.1007/s11357-010-9140-1 http://dx.doi.org/10.1007/s11357-010-9140-1