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      Skeletal muscle metabolism during prolonged exercise in Pompe disease

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          Abstract

          Objective

          Pompe disease (glycogenosis type II) is caused by lysosomal alpha-glucosidase deficiency, which leads to a block in intra-lysosomal glycogen breakdown. In spite of enzyme replacement therapy, Pompe disease continues to be a progressive metabolic myopathy. Considering the health benefits of exercise, it is important in Pompe disease to acquire more information about muscle substrate use during exercise.

          Methods

          Seven adults with Pompe disease were matched to a healthy control group (1:1). We determined (1) peak oxidative capacity (VO 2peak) and (2) carbohydrate and fatty acid metabolism during submaximal exercise (33 W) for 1 h, using cycle-ergometer exercise, indirect calorimetry and stable isotopes.

          Results

          In the patients, VO 2peak was less than half of average control values; mean difference −1659 mL/min (CI: −2450 to −867, P = 0.001). However, the respiratory exchange ratio increased to >1.0 and lactate levels rose 5-fold in the patients, indicating significant glycolytic flux. In line with this, during submaximal exercise, the rates of oxidation (ROX) of carbohydrates and palmitate were similar between patients and controls (mean difference 0.226 g/min (CI: 0.611 to −0.078, P = 0.318) and mean difference 0.016 µmol/kg/min (CI: 1.287 to −1.255, P = 0.710), respectively).

          Conclusion

          Reflecting muscle weakness and wasting, Pompe disease is associated with markedly reduced maximal exercise capacity. However, glycogenolysis is not impaired in exercise. Unlike in other metabolic myopathies, skeletal muscle substrate use during exercise is normal in Pompe disease rendering exercise less complicated for e.g. medical or recreational purposes.

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          Most cited references35

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          Perceived exertion as an indicator of somatic stress.

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            Table of nonprotein respiratory quotient: an update.

            The purpose of this paper is to point out some limits and inconsistencies in the table of nonprotein respiratory quotient that is universally used. This table, developed by Lusk in 1924, was derived from biochemical and physical data that are now outdated. A new table of nonprotein respiratory quotient, consistent with modern chemical and physical data, is proposed. The revised table is based on (a) the average composition of human triacylglycerol stores, (b) energy potential of fatty acids and glucose, and (c) the volumes occupied by one mole of oxygen or carbon dioxide (which are not ideal gases) under STPD conditions.
              • Record: found
              • Abstract: found
              • Article: not found

              Power and sample size calculations. A review and computer program.

              Methods of sample size and power calculations are reviewed for the most common study designs. The sample size and power equations for these designs are shown to be special cases of two generic formulae for sample size and power calculations. A computer program is available that can be used for studies with dichotomous, continuous, or survival response measures. The alternative hypotheses of interest may be specified either in terms of differing response rates, means, or survival times, or in terms of relative risks or odds ratios. Studies with dichotomous or continuous outcomes may involve either a matched or independent study design. The program can determine the sample size needed to detect a specified alternative hypothesis with the required power, the power with which a specific alternative hypothesis can be detected with a given sample size, or the specific alternative hypotheses that can be detected with a given power and sample size. The program can generate help messages on request that facilitate the use of this software. It writes a log file of all calculated estimates and can produce an output file for plotting power curves. It is written in FORTRAN-77 and is in the public domain.

                Author and article information

                Journal
                Endocr Connect
                Endocr Connect
                EC
                Endocrine Connections
                Bioscientifica Ltd (Bristol )
                2049-3614
                August 2017
                10 May 2017
                : 6
                : 6
                : 384-394
                Affiliations
                [1 ]Copenhagen Neuromuscular Center , Department of Neurology, Rigshospitalet, University of Copenhagen, Copenhagen, Denmark
                [2 ]Centre de Référence de Pathologie Neuromusculaire Paris-Est , Institut de Myologie, GH Pitié-Salpêtrière, Assistance Publique-Hôpitaux de Paris, Paris, France
                [3 ]Department of Inflammation Research , Rigshospitalet, Copenhagen, Denmark
                [4 ]Department of Neurology , Sahlgrenska University Hospital, Gothenburg, Sweden
                Author notes
                Correspondence should be addressed to N Preisler; Email: npreisler@ 123456hotmail.com
                Article
                EC-17-0042
                10.1530/EC-17-0042
                8450668
                28490439
                8b735dee-7cdf-4b10-b660-f7baedb4ef63
                © 2017 The authors

                This work is licensed under a Creative Commons Attribution-NonCommercial 4.0 International License.

                History
                : 8 May 2017
                : 10 May 2017
                Categories
                Research

                skeletal muscle metabolism,glycogen,exercise,pompe disease,glycogenosis

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