Is muscle glycogenolysis impaired in X-linked phosphorylase b kinase deficiency?

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Standard

Is muscle glycogenolysis impaired in X-linked phosphorylase b kinase deficiency? / Orngreen, M.C.; Schelhaas, H.J.; Jeppesen, T.D.; Akman, H.O.; Wevers, R.A.; Andersen, S.T.; Laak, H.J. ter; Diggelen, O.P. van; DiMauro, S.; Vissing, J.

I: Neurology, Bind 70, Nr. 20, 2008, s. 1876-1882.

Publikation: Bidrag til tidsskriftTidsskriftartikelForskningfagfællebedømt

Harvard

Orngreen, MC, Schelhaas, HJ, Jeppesen, TD, Akman, HO, Wevers, RA, Andersen, ST, Laak, HJT, Diggelen, OPV, DiMauro, S & Vissing, J 2008, 'Is muscle glycogenolysis impaired in X-linked phosphorylase b kinase deficiency?', Neurology, bind 70, nr. 20, s. 1876-1882.

APA

Orngreen, M. C., Schelhaas, H. J., Jeppesen, T. D., Akman, H. O., Wevers, R. A., Andersen, S. T., Laak, H. J. T., Diggelen, O. P. V., DiMauro, S., & Vissing, J. (2008). Is muscle glycogenolysis impaired in X-linked phosphorylase b kinase deficiency? Neurology, 70(20), 1876-1882.

Vancouver

Orngreen MC, Schelhaas HJ, Jeppesen TD, Akman HO, Wevers RA, Andersen ST o.a. Is muscle glycogenolysis impaired in X-linked phosphorylase b kinase deficiency? Neurology. 2008;70(20):1876-1882.

Author

Orngreen, M.C. ; Schelhaas, H.J. ; Jeppesen, T.D. ; Akman, H.O. ; Wevers, R.A. ; Andersen, S.T. ; Laak, H.J. ter ; Diggelen, O.P. van ; DiMauro, S. ; Vissing, J. / Is muscle glycogenolysis impaired in X-linked phosphorylase b kinase deficiency?. I: Neurology. 2008 ; Bind 70, Nr. 20. s. 1876-1882.

Bibtex

@article{847040d09c4111debc73000ea68e967b,
title = "Is muscle glycogenolysis impaired in X-linked phosphorylase b kinase deficiency?",
abstract = "OBJECTIVE: It is unclear to what extent muscle phosphorylase b kinase (PHK) deficiency is associated with exercise-related symptoms and impaired muscle metabolism, because 1) only four patients have been characterized at the molecular level, 2) reported symptoms have been nonspecific, and 3) lactate responses to ischemic handgrip exercise have been normal. METHODS: We studied a 50-year-old man with X-linked PHK deficiency using ischemic forearm and cycle ergometry exercise tests to define the derangement of muscle metabolism. We compared our findings with those in patients with McArdle disease and in healthy subjects. RESULTS: Sequencing of PHKA1 showed a novel pathogenic mutation (c.831G>A) in exon 7. There was a normal increase of plasma lactate during forearm ischemic exercise, but lactate did not change during dynamic, submaximal exercise in contrast to the fourfold increase in healthy subjects. Constant workload elicited a second wind in all patients with McArdle disease, but not in the patient with PHK deficiency. IV glucose administration appeared to improve exercise tolerance in the patient with PHK deficiency, but not to the same extent as in the patients with McArdle disease. Lipolysis was higher in the patient with PHK deficiency than in controls. CONCLUSION: These findings demonstrate that X-linked PHK deficiency causes a mild metabolic myopathy with blunted muscle glycogen breakdown and impaired lactate production during dynamic exercise, which impairs oxidative capacity only marginally. The different response of lactate to submaximal and maximal exercise is likely related to differential activation mechanisms for myophosphorylase Udgivelsesdato: 2008/5/13",
author = "M.C. Orngreen and H.J. Schelhaas and T.D. Jeppesen and H.O. Akman and R.A. Wevers and S.T. Andersen and Laak, {H.J. ter} and Diggelen, {O.P. van} and S. DiMauro and J. Vissing",
year = "2008",
language = "English",
volume = "70",
pages = "1876--1882",
journal = "Neurology",
issn = "0028-3878",
publisher = "Lippincott Williams & Wilkins",
number = "20",

}

RIS

TY - JOUR

T1 - Is muscle glycogenolysis impaired in X-linked phosphorylase b kinase deficiency?

AU - Orngreen, M.C.

AU - Schelhaas, H.J.

AU - Jeppesen, T.D.

AU - Akman, H.O.

AU - Wevers, R.A.

AU - Andersen, S.T.

AU - Laak, H.J. ter

AU - Diggelen, O.P. van

AU - DiMauro, S.

AU - Vissing, J.

PY - 2008

Y1 - 2008

N2 - OBJECTIVE: It is unclear to what extent muscle phosphorylase b kinase (PHK) deficiency is associated with exercise-related symptoms and impaired muscle metabolism, because 1) only four patients have been characterized at the molecular level, 2) reported symptoms have been nonspecific, and 3) lactate responses to ischemic handgrip exercise have been normal. METHODS: We studied a 50-year-old man with X-linked PHK deficiency using ischemic forearm and cycle ergometry exercise tests to define the derangement of muscle metabolism. We compared our findings with those in patients with McArdle disease and in healthy subjects. RESULTS: Sequencing of PHKA1 showed a novel pathogenic mutation (c.831G>A) in exon 7. There was a normal increase of plasma lactate during forearm ischemic exercise, but lactate did not change during dynamic, submaximal exercise in contrast to the fourfold increase in healthy subjects. Constant workload elicited a second wind in all patients with McArdle disease, but not in the patient with PHK deficiency. IV glucose administration appeared to improve exercise tolerance in the patient with PHK deficiency, but not to the same extent as in the patients with McArdle disease. Lipolysis was higher in the patient with PHK deficiency than in controls. CONCLUSION: These findings demonstrate that X-linked PHK deficiency causes a mild metabolic myopathy with blunted muscle glycogen breakdown and impaired lactate production during dynamic exercise, which impairs oxidative capacity only marginally. The different response of lactate to submaximal and maximal exercise is likely related to differential activation mechanisms for myophosphorylase Udgivelsesdato: 2008/5/13

AB - OBJECTIVE: It is unclear to what extent muscle phosphorylase b kinase (PHK) deficiency is associated with exercise-related symptoms and impaired muscle metabolism, because 1) only four patients have been characterized at the molecular level, 2) reported symptoms have been nonspecific, and 3) lactate responses to ischemic handgrip exercise have been normal. METHODS: We studied a 50-year-old man with X-linked PHK deficiency using ischemic forearm and cycle ergometry exercise tests to define the derangement of muscle metabolism. We compared our findings with those in patients with McArdle disease and in healthy subjects. RESULTS: Sequencing of PHKA1 showed a novel pathogenic mutation (c.831G>A) in exon 7. There was a normal increase of plasma lactate during forearm ischemic exercise, but lactate did not change during dynamic, submaximal exercise in contrast to the fourfold increase in healthy subjects. Constant workload elicited a second wind in all patients with McArdle disease, but not in the patient with PHK deficiency. IV glucose administration appeared to improve exercise tolerance in the patient with PHK deficiency, but not to the same extent as in the patients with McArdle disease. Lipolysis was higher in the patient with PHK deficiency than in controls. CONCLUSION: These findings demonstrate that X-linked PHK deficiency causes a mild metabolic myopathy with blunted muscle glycogen breakdown and impaired lactate production during dynamic exercise, which impairs oxidative capacity only marginally. The different response of lactate to submaximal and maximal exercise is likely related to differential activation mechanisms for myophosphorylase Udgivelsesdato: 2008/5/13

M3 - Journal article

VL - 70

SP - 1876

EP - 1882

JO - Neurology

JF - Neurology

SN - 0028-3878

IS - 20

ER -

ID: 14274762