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      Interaction between plasma fetuin‐A and free fatty acids predicts changes in insulin sensitivity in response to long‐term exercise

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          Abstract

          The hepatokine fetuin‐A can together with free fatty acids ( FFAs) enhance adipose tissue ( AT) inflammation and insulin resistance via toll‐like receptor 4 ( TLR4). Although some of the health benefits of exercise can be explained by altered release of myokines from the skeletal muscle, it is not well documented if some of the beneficial effects of exercise can be explained by altered secretion of hepatokines. The aim of this study was to examine the effect of interaction between fetuin‐A and FFAs on insulin sensitivity after physical exercise. In this study, 26 sedentary men who underwent 12 weeks of combined endurance and strength exercise were included. Insulin sensitivity was measured using euglycemic‐hyperinsulinemic clamp, and AT insulin resistance was indicated by the product of fasting plasma concentration of FFAs and insulin. Blood samples and biopsies from skeletal muscle and subcutaneous AT were collected. Several phenotypic markers were measured, and mRNA sequencing was performed on the biopsies. AT macrophages were analyzed based on mRNA markers. The intervention improved hepatic parameters, reduced plasma fetuin‐A concentration (~11%, P < 0.01), slightly changed FFAs concentration, and improved glucose infusion rate ( GIR) (~33%, P < 0.01) across all participants. The change in circulating fetuin‐A and FFAs interacted to predict some of the change in GIR ( β = −42.16, =  0.030), AT insulin resistance ( β = 0.579, =  0.003), gene expression related to TLR‐signaling in AT and AT macrophage mRNA ( β = 94.10, =  0.034) after exercise. We observed no interaction effects between FFAs concentrations and leptin and adiponectin on insulin sensitivity, or any interaction effects between Fetuin‐A and FFAs concentrations on skeletal muscle TLR‐signaling. The relationship between FFAs levels and insulin sensitivity seemed to be specific for fetuin‐A and the AT. Some of the beneficial effects of exercise on insulin sensitivity may be explained by changes in circulating fetuin‐A and FFAs, promoting less TLR4 signaling in AT perhaps by modulating AT macrophages.

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          Muscles, exercise and obesity: skeletal muscle as a secretory organ.

          Bente K. Pedersen, Mark A. Febbraio (2012)
          During the past decade, skeletal muscle has been identified as a secretory organ. Accordingly, we have suggested that cytokines and other peptides that are produced, expressed and released by muscle fibres and exert either autocrine, paracrine or endocrine effects should be classified as myokines. The finding that the muscle secretome consists of several hundred secreted peptides provides a conceptual basis and a whole new paradigm for understanding how muscles communicate with other organs, such as adipose tissue, liver, pancreas, bones and brain. However, some myokines exert their effects within the muscle itself. Thus, myostatin, LIF, IL-6 and IL-7 are involved in muscle hypertrophy and myogenesis, whereas BDNF and IL-6 are involved in AMPK-mediated fat oxidation. IL-6 also appears to have systemic effects on the liver, adipose tissue and the immune system, and mediates crosstalk between intestinal L cells and pancreatic islets. Other myokines include the osteogenic factors IGF-1 and FGF-2; FSTL-1, which improves the endothelial function of the vascular system; and the PGC-1α-dependent myokine irisin, which drives brown-fat-like development. Studies in the past few years suggest the existence of yet unidentified factors, secreted from muscle cells, which may influence cancer cell growth and pancreas function. Many proteins produced by skeletal muscle are dependent upon contraction; therefore, physical inactivity probably leads to an altered myokine response, which could provide a potential mechanism for the association between sedentary behaviour and many chronic diseases.
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            Quantitative insulin sensitivity check index: a simple, accurate method for assessing insulin sensitivity in humans.

            S Nambi, K Mather, A. Katz (2000)
            Insulin resistance plays an important role in the pathophysiology of diabetes and is associated with obesity and other cardiovascular risk factors. The "gold standard" glucose clamp and minimal model analysis are two established methods for determining insulin sensitivity in vivo, but neither is easily implemented in large studies. Thus, it is of interest to develop a simple, accurate method for assessing insulin sensitivity that is useful for clinical investigations. We performed both hyperinsulinemic isoglycemic glucose clamp and insulin-modified frequently sampled iv glucose tolerance tests on 28 nonobese, 13 obese, and 15 type 2 diabetic subjects. We obtained correlations between indexes of insulin sensitivity from glucose clamp studies (SI(Clamp)) and minimal model analysis (SI(MM)) that were comparable to previous reports (r = 0.57). We performed a sensitivity analysis on our data and discovered that physiological steady state values [i.e. fasting insulin (I(0)) and glucose (G(0))] contain critical information about insulin sensitivity. We defined a quantitative insulin sensitivity check index (QUICKI = 1/[log(I(0)) + log(G(0))]) that has substantially better correlation with SI(Clamp) (r = 0.78) than the correlation we observed between SI(MM) and SI(Clamp). Moreover, we observed a comparable overall correlation between QUICKI and SI(Clamp) in a totally independent group of 21 obese and 14 nonobese subjects from another institution. We conclude that QUICKI is an index of insulin sensitivity obtained from a fasting blood sample that may be useful for clinical research.
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              Glucose clamp technique: a method for quantifying insulin secretion and resistance.

              Christian R. Andres, Stephanie J. Tobin, R. DeFronzo (1979)
              Methods for the quantification of beta-cell sensitivity to glucose (hyperglycemic clamp technique) and of tissue sensitivity to insulin (euglycemic insulin clamp technique) are described. Hyperglycemic clamp technique. The plasma glucose concentration is acutely raised to 125 mg/dl above basal levels by a priming infusion of glucose. The desired hyperglycemic plateau is subsequently maintained by adjustment of a variable glucose infusion, based on the negative feedback principle. Because the plasma glucose concentration is held constant, the glucose infusion rate is an index of glucose metabolism. Under these conditions of constant hyperglycemia, the plasma insulin response is biphasic with an early burst of insulin release during the first 6 min followed by a gradually progressive increase in plasma insulin concentration. Euglycemic insulin clamp technique. The plasma insulin concentration is acutely raised and maintained at approximately 100 muU/ml by a prime-continuous infusion of insulin. The plasma glucose concentration is held constant at basal levels by a variable glucose infusion using the negative feedback principle. Under these steady-state conditions of euglycemia, the glucose infusion rate equals glucose uptake by all the tissues in the body and is therefore a measure of tissue sensitivity to exogenous insulin.
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                Author and article information

                Contributors
                Sindre Lee: sindre.lee@medisin.uio.no
                Journal
                Journal ID (nlm-ta): Physiol Rep
                Journal ID (iso-abbrev): Physiol Rep
                Journal ID (doi): 10.1002/(ISSN)2051-817X
                Journal ID (publisher-id): PHY2
                Journal ID (hwp): physreports
                Title: Physiological Reports
                Publisher: John Wiley and Sons Inc. (Hoboken )
                ISSN (Electronic): 2051-817X
                Publication date (Electronic): 07 March 2017
                Publication date Collection: March 2017
                Volume: 5
                Issue: 5 ( doiID: 10.1002/phy2.2017.5.issue-5 )
                Electronic Location Identifier: e13183
                Affiliations
                [ 1 ] Department of NutritionInstitute of Basic Medical Sciences Faculty of Medicine University of Oslo OsloNorway
                [ 2 ] Division of CardiologyDepartment of Medicine University of California at Los Angeles Los Angeles California
                [ 3 ] Institute of Clinical MedicineFaculty of Medicine University of Oslo OsloNorway
                [ 4 ] Department of Physical PerformanceNorwegian School of Sport Sciences OsloNorway
                [ 5 ] Department of Medical GeneticsOslo University Hospital and University of Oslo OsloNorway
                [ 6 ] Department of EndocrinologyMorbid Obesity and Preventive Medicine Oslo University Hospital OsloNorway
                Author notes
                [*] [* ] Correspondence

                Sindre Lee, Department of Nutrition, Institute of Basic Medical Sciences, Faculty of Medicine, University of Oslo, Oslo, Norway.

                Tel: +47696851

                E‐mail: sindre.lee@ 123456medisin.uio.no

                Article
                Publisher ID: PHY213183
                DOI: 10.14814/phy2.13183
                PMC ID: 5350184
                PubMed ID: 28270597
                SO-VID: b314f8e6-a988-485a-b66b-21726f947d9e
                Copyright © © 2017 The Authors. Physiological Reports published by Wiley Periodicals, Inc. on behalf of The Physiological Society and the American Physiological Society.
                License:

                This is an open access article under the terms of the Creative Commons Attribution License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.

                History
                Date received : 21 September 2016
                Date revision received : 30 January 2017
                Date accepted : 05 February 2017
                Page count
                Figures: 3, Tables: 6, Pages: 14, Words: 9049
                Funding
                Funded by: Institute of Basic Medical Sciences
                Funded by: UiO
                Funded by: Johan Throne‐Holst Foundation for Nutrition Research
                Funded by: Freia Medical Research Foundation
                Funded by: Research Council of Norway
                Funded by: Southeastern Regional Health Authorities
                Funded by: NutriTech
                Award ID: 289511
                Categories
                Subject: Immunology
                Subject: Signalling Pathways
                Subject: Endurance and Performance
                Subject: Adipose Tissue and Obesity
                Subject: Endocrine and Metabolic Conditons, Disorders and Treatments
                Subject: Original Research
                Subject: Original Research
                Custom metadata
                source-schema-version-number 2.0
                component-id phy213183
                cover-date March 2017
                details-of-publishers-convertor Converter:WILEY_ML3GV2_TO_NLMPMC version:5.0.8 mode:remove_FC converted:14.03.2017

                Keywords: adipose tissue,exercise,fetuin‐a,free fatty acids,hepatokine,human,insulin sensitivity
                Data availability:
                Keywords: adipose tissue, exercise, fetuin‐a, free fatty acids, hepatokine, human, insulin sensitivity

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