Multi-omic integrated networks connect DNA methylation and miRNA with skeletal muscle plasticity to chronic exercise in Type 2 diabetic obesity-Reference-Cited by-同舟云学术

Multi-omic integrated networks connect DNA methylation and miRNA with skeletal muscle plasticity to chronic exercise in Type 2 diabetic obesity

Published:2014-10-15 Issue:20 Volume:46 Page:747-765
ISSN:1094-8341
Container-title:Physiological Genomics
language:en
Short-container-title:Physiological Genomics

Author:

Rowlands David S.¹,Page Rachel A.²,Sukala William R.²,Giri Mamta³,Ghimbovschi Svetlana D.³,Hayat Irum²,Cheema Birinder S.⁴,Lys Isabelle⁵,Leikis Murray⁶,Sheard Phillip W.⁷,Wakefield St. John⁸,Breier Bernhard²,Hathout Yetrib³,Brown Kristy³,Marathi Ramya³,Orkunoglu-Suer Funda E.³,Devaney Joseph M.³,Leiken Benjamin³,Many Gina³,Krebs Jeremy⁹,Hopkins Will G.¹⁰,Hoffman Eric P.³

Affiliation:

1. School of Sport and Exercise, Massey University, Wellington, New Zealand;

2. Institute of Food, Nutrition & Human Health, Massey University, New Zealand;

3. Children's National Medical Center, Center for Genetic Medicine Research (CGMR), Washington, District of Columbia;

4. School of Science and Health, University of Western Sydney, Campbelltown, Australia;

5. Faculty of Engineering, Health, Science and the Environment, Charles Darwin University, Australia;

6. Wellington Hospital, Capital and Coast District Health Board, Wellington, New Zealand;

7. Department of Physiology, University of Otago, Dunedin, New Zealand;

8. Department of Pathology, University of Otago, Wellington, New Zealand; and

9. Endocrine and Diabetes Unit, Capital and Coast District Health Board, Wellington, New Zealand;

10. Health Science/Sport and Recreation, Auckland University of Technology, Auckland, New Zealand

Abstract

Epigenomic regulation of the transcriptome by DNA methylation and posttranscriptional gene silencing by miRNAs are potential environmental modulators of skeletal muscle plasticity to chronic exercise in healthy and diseased populations. We utilized transcriptome networks to connect exercise-induced differential methylation and miRNA with functional skeletal muscle plasticity. Biopsies of the vastus lateralis were collected from middle-aged Polynesian men and women with morbid obesity (44 kg/m2 ± 10) and Type 2 diabetes before and following 16 wk of resistance ( n = 9) or endurance training ( n = 8). Longitudinal transcriptome, methylome, and microRNA (miRNA) responses were obtained via microarray, filtered by novel effect-size based false discovery rate probe selection preceding bioinformatic interrogation. Metabolic and microvascular transcriptome topology dominated the network landscape following endurance exercise. Lipid and glucose metabolism modules were connected to: microRNA (miR)-29a; promoter region hypomethylation of nuclear receptor factor ( NRF1) and fatty acid transporter ( SLC27A4), and hypermethylation of fatty acid synthase, and to exon hypomethylation of 6-phosphofructo-2-kinase and Ser/Thr protein kinase. Directional change in the endurance networks was validated by lower intramyocellular lipid, increased capillarity, GLUT4, hexokinase, and mitochondrial enzyme activity and proteome. Resistance training also lowered lipid and increased enzyme activity and caused GLUT4 promoter hypomethylation; however, training was inconsequential to GLUT4, capillarity, and metabolic transcriptome. miR-195 connected to negative regulation of vascular development. To conclude, integrated molecular network modelling revealed differential DNA methylation and miRNA expression changes occur in skeletal muscle in response to chronic exercise training that are most pronounced with endurance training and topographically associated with functional metabolic and microvascular plasticity relevant to diabetes rehabilitation.

Publisher

American Physiological Society

Subject

Genetics,Physiology

Link

https://www.physiology.org/doi/pdf/10.1152/physiolgenomics.00024.2014

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