Defects in sarcolemma repair and skeletal muscle function after injury in a mouse model of Niemann-Pick type A/B disease

Defects in sarcolemma repair and skeletal muscle function after injury in a mouse model of Niemann-Pick type A/B disease

Abstract Background Niemann-Pick disease type A (NPDA), a disease caused by mutations in acid sphingomyelinase (ASM), involves severe neurodegeneration and early death. Intracellular lipid accumulation and plasma membrane alterations are implicated in the pathology. ASM is also linked to the mechani...

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Main Authors: V. Michailowsky, H. Li, B. Mittra, S. R. Iyer, D. A. G. Mazála, M. Corrotte, Y. Wang, E. R. Chin, R. M. Lovering, N. W. Andrews
Format: Article
Language:English
Published: BMC 2019-01-01
Series:Skeletal Muscle
Subjects:
Acid sphingomyelinase
Skeletal muscle
Lysosome
Calcium
Plasma membrane repair
Online Access:http://link.springer.com/article/10.1186/s13395-018-0187-5
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spelling doaj-5eae96934ef04e10951d66152b5cd1662020-11-24T21:21:05ZengBMCSkeletal Muscle2044-50402019-01-019111510.1186/s13395-018-0187-5Defects in sarcolemma repair and skeletal muscle function after injury in a mouse model of Niemann-Pick type A/B diseaseV. Michailowsky0H. Li1B. Mittra2S. R. Iyer3D. A. G. Mazála4M. Corrotte5Y. Wang6E. R. Chin7R. M. Lovering8N. W. Andrews9Department of Cell Biology and Molecular Genetics, University of MarylandDepartment of Kinesiology, University of Maryland School of Public HealthDepartment of Cell Biology and Molecular Genetics, University of MarylandDepartment of Orthopaedics, University of Maryland School of MedicineCenter for Genetic Medicine Research, Children’s National Health SystemDepartment of Cell Biology and Molecular Genetics, University of MarylandProteomics Core Facility, College of Computer, Mathematical and Natural Sciences, University of MarylandDepartment of Kinesiology, University of Maryland School of Public HealthDepartment of Orthopaedics, University of Maryland School of MedicineDepartment of Cell Biology and Molecular Genetics, University of MarylandAbstract Background Niemann-Pick disease type A (NPDA), a disease caused by mutations in acid sphingomyelinase (ASM), involves severe neurodegeneration and early death. Intracellular lipid accumulation and plasma membrane alterations are implicated in the pathology. ASM is also linked to the mechanism of plasma membrane repair, so we investigated the impact of ASM deficiency in skeletal muscle, a tissue that undergoes frequent cycles of injury and repair in vivo. Methods Utilizing the NPDA/B mouse model ASM−/− and wild type (WT) littermates, we performed excitation-contraction coupling/Ca2+ mobilization and sarcolemma injury/repair assays with isolated flexor digitorum brevis fibers, proteomic analyses with quadriceps femoris, flexor digitorum brevis, and tibialis posterior muscle and in vivo tests of the contractile force (maximal isometric torque) of the quadriceps femoris muscle before and after eccentric contraction-induced muscle injury. Results ASM−/− flexor digitorum brevis fibers showed impaired excitation-contraction coupling compared to WT, a defect expressed as reduced tetanic [Ca2+]i in response to electrical stimulation and early failure in sustaining [Ca2+]i during repeated tetanic contractions. When injured mechanically by needle passage, ASM−/− flexor digitorum brevis fibers showed susceptibility to injury similar to WT, but a reduced ability to reseal the sarcolemma. Proteomic analyses revealed changes in a small group of skeletal muscle proteins as a consequence of ASM deficiency, with downregulation of calsequestrin occurring in the three different muscles analyzed. In vivo, the loss in maximal isometric torque of WT quadriceps femoris was similar immediately after and 2 min after injury. The loss in ASM−/− mice immediately after injury was similar to WT, but was markedly larger at 2 min after injury. Conclusions Skeletal muscle fibers from ASM−/− mice have an impairment in intracellular Ca2+ handling that results in reduced Ca2+ mobilization and a more rapid decline in peak Ca2+ transients during repeated contraction-relaxation cycles. Isolated fibers show reduced ability to repair damage to the sarcolemma, and this is associated with an exaggerated deficit in force during recovery from an in vivo eccentric contraction-induced muscle injury. Our findings uncover the possibility that skeletal muscle functional defects may play a role in the pathology of NPDA/B disease.http://link.springer.com/article/10.1186/s13395-018-0187-5Acid sphingomyelinaseSkeletal muscleLysosomeCalciumPlasma membrane repair
collection DOAJ
language English
format Article
sources DOAJ
author V. Michailowsky
H. Li
B. Mittra
S. R. Iyer
D. A. G. Mazála
M. Corrotte
Y. Wang
E. R. Chin
R. M. Lovering
N. W. Andrews
spellingShingle V. Michailowsky
H. Li
B. Mittra
S. R. Iyer
D. A. G. Mazála
M. Corrotte
Y. Wang
E. R. Chin
R. M. Lovering
N. W. Andrews
Defects in sarcolemma repair and skeletal muscle function after injury in a mouse model of Niemann-Pick type A/B disease
Skeletal Muscle
Acid sphingomyelinase
Skeletal muscle
Lysosome
Calcium
Plasma membrane repair
author_facet V. Michailowsky
H. Li
B. Mittra
S. R. Iyer
D. A. G. Mazála
M. Corrotte
Y. Wang
E. R. Chin
R. M. Lovering
N. W. Andrews
author_sort V. Michailowsky
title Defects in sarcolemma repair and skeletal muscle function after injury in a mouse model of Niemann-Pick type A/B disease
title_short Defects in sarcolemma repair and skeletal muscle function after injury in a mouse model of Niemann-Pick type A/B disease
title_full Defects in sarcolemma repair and skeletal muscle function after injury in a mouse model of Niemann-Pick type A/B disease
title_fullStr Defects in sarcolemma repair and skeletal muscle function after injury in a mouse model of Niemann-Pick type A/B disease
title_full_unstemmed Defects in sarcolemma repair and skeletal muscle function after injury in a mouse model of Niemann-Pick type A/B disease
title_sort defects in sarcolemma repair and skeletal muscle function after injury in a mouse model of niemann-pick type a/b disease
publisher BMC
series Skeletal Muscle
issn 2044-5040
publishDate 2019-01-01
description Abstract Background Niemann-Pick disease type A (NPDA), a disease caused by mutations in acid sphingomyelinase (ASM), involves severe neurodegeneration and early death. Intracellular lipid accumulation and plasma membrane alterations are implicated in the pathology. ASM is also linked to the mechanism of plasma membrane repair, so we investigated the impact of ASM deficiency in skeletal muscle, a tissue that undergoes frequent cycles of injury and repair in vivo. Methods Utilizing the NPDA/B mouse model ASM−/− and wild type (WT) littermates, we performed excitation-contraction coupling/Ca2+ mobilization and sarcolemma injury/repair assays with isolated flexor digitorum brevis fibers, proteomic analyses with quadriceps femoris, flexor digitorum brevis, and tibialis posterior muscle and in vivo tests of the contractile force (maximal isometric torque) of the quadriceps femoris muscle before and after eccentric contraction-induced muscle injury. Results ASM−/− flexor digitorum brevis fibers showed impaired excitation-contraction coupling compared to WT, a defect expressed as reduced tetanic [Ca2+]i in response to electrical stimulation and early failure in sustaining [Ca2+]i during repeated tetanic contractions. When injured mechanically by needle passage, ASM−/− flexor digitorum brevis fibers showed susceptibility to injury similar to WT, but a reduced ability to reseal the sarcolemma. Proteomic analyses revealed changes in a small group of skeletal muscle proteins as a consequence of ASM deficiency, with downregulation of calsequestrin occurring in the three different muscles analyzed. In vivo, the loss in maximal isometric torque of WT quadriceps femoris was similar immediately after and 2 min after injury. The loss in ASM−/− mice immediately after injury was similar to WT, but was markedly larger at 2 min after injury. Conclusions Skeletal muscle fibers from ASM−/− mice have an impairment in intracellular Ca2+ handling that results in reduced Ca2+ mobilization and a more rapid decline in peak Ca2+ transients during repeated contraction-relaxation cycles. Isolated fibers show reduced ability to repair damage to the sarcolemma, and this is associated with an exaggerated deficit in force during recovery from an in vivo eccentric contraction-induced muscle injury. Our findings uncover the possibility that skeletal muscle functional defects may play a role in the pathology of NPDA/B disease.
topic Acid sphingomyelinase
Skeletal muscle
Lysosome
Calcium
Plasma membrane repair
url http://link.springer.com/article/10.1186/s13395-018-0187-5
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