Increased resistance to fatigue in creatine kinase deficient muscle is not due to improved contractile economy

被引:0
作者
Frank ter Veld
Klaas Nicolay
Jeroen A.L. Jeneson
机构
[1] University Medical Center Utrecht,Department of Experimental In Vivo NMR, Image Sciences Institute
[2] Eindhoven University of Technology,Biomedical NMR, Department of Biomedical Engineering
[3] Utrecht University,Department of Pathobiology, Division of Anatomy and Physiology, School of Veterinary Medicine
[4] German Diabetes Center,undefined
来源
Pflügers Archiv | 2006年 / 452卷
关键词
Contractile economy; Transgenic mice; Skeletal muscle; Muscle fatigue; Creatine kinase;
D O I
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中图分类号
学科分类号
摘要
There has been speculation on the origin of the increased endurance of skeletal muscles in creatine kinase (CK)-deficient mice. Important factors that have been raised include the documented increased mitochondrial capacity and alterations in myosin heavy chain (MyHC) isoform composition in CK-deficient muscle. More recently, the absence of inorganic phosphate release from phosphocreatine hydrolysis in exercising CK-deficient muscle has been postulated to contribute to the lower fatigueability in skeletal muscle. In this study, we tested the hypothesis that the reported shift in MyHC composition to slower isoforms in CK-deficient muscle leads to a decrease in oxygen cost of twitch performance. To that aim, extensor digitorum longus (EDL) and soleus (SOL) muscles were isolated from wild-type (WT) and knock-out mice deficient in the cytoplasmic muscle-type and sarcomeric mitochondrial isoenzymes of CK, and oxygen consumption per twitch time–tension-integral (TTI) was measured. The results show that the adaptive response to loss of CK function does not involve any major change to contractile economy of skeletal muscle.
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页码:342 / 348
页数:6
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