Please use this identifier to cite or link to this item: http://hdl.handle.net/1893/31599
Appears in Collections:Faculty of Health Sciences and Sport Journal Articles
Peer Review Status: Refereed
Title: Human skeletal muscle metabolic responses to 6 days of high-fat overfeeding are associated with dietary n-3PUFA content and muscle oxidative capacity
Author(s): Wardle, Sophie L
Macnaughton, Lindsay S
McGlory, Chris
Witard, Oliver C
Dick, James R
Whitfield, Philip D
Ferrando, Arny A
Wolfe, Robert R
Kim, Il‐Young
Hamilton, D Lee
Moran, Colin N
Tipton, Kevin D
Galloway, S D
Contact Email: s.d.r.galloway@stir.ac.uk
Keywords: exercise
fish oil
insulin resistance
omega‐3
overfeeding
type 2 diabetes
Issue Date: Aug-2020
Date Deposited: 26-Aug-2020
Citation: Wardle SL, Macnaughton LS, McGlory C, Witard OC, Dick JR, Whitfield PD, Ferrando AA, Wolfe RR, Kim I, Hamilton DL, Moran CN, Tipton KD & Galloway SD (2020) Human skeletal muscle metabolic responses to 6 days of high-fat overfeeding are associated with dietary n-3PUFA content and muscle oxidative capacity. Physiological Reports, 8 (16), Art. No.: e14529. https://doi.org/10.14814/phy2.14529
Abstract: Understanding human physiological responses to high-fat energy excess (HFEE) may help combat the development of metabolic disease. We aimed to investigate the impact of manipulating the n-3PUFA content of HFEE diets on whole-body and skeletal muscle markers of insulin sensitivity. Twenty healthy males were overfed (150% energy, 60% fat, 25% carbohydrate, 15% protein) for 6 d. One group (n=10) received 10% of fat intake as n-3PUFA rich fish oil (HF-FO), and the other group consumed a mix of fats (HF-C). Oral glucose tolerance tests with stable isotope tracer infusions were conducted before, and following, HFEE, with muscle biopsies obtained in basal and insulin-stimulated states for measurement of membrane phospholipids, ceramides, mitochondrial enzyme activities, and PKB and AMPKα2 activity. Insulin sensitivity and glucose disposal did not change following HFEE, irrespective of group. Skeletal muscle ceramide content increased following HFEE (8.5±1.2 to 12.1±1.7 nmol·mg-1, P=0.03), irrespective of group. No change in mitochondrial enzyme activity was observed following HFEE, but citrate synthase activity was inversely associated with increases in ceramide content (r=-0.52, P=0.048). A time by group interaction was observed for PKB activity (P=0.003), with increased activity following HFEE in HF-C (4.5±13.0 mU·mg-1) and decreased activity in HF-FO (-10.1±20.7mU·mg-1) following HFEE. Basal AMPKα2 activity increased in HF-FO (4.1±0.6 to 5.3±0.7 mU·mg-1, P=0.049), but did not change in HF-C (4.6±0.7 to 3.8±0.9 mU·mg-1) following HFEE. We conclude that early skeletal muscle signalling responses to HFEE appear to be modified by dietary n-3PUFA content, but the potential impact on future development of metabolic disease needs exploring.
DOI Link: 10.14814/phy2.14529
Rights: © 2020 The Authors. Physiological Reports published by Wiley Periodicals, Inc. on behalf of The Physiological Society and the American Physiological Society This is an open access article under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/), which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
Licence URL(s): http://creativecommons.org/licenses/by/4.0/

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