Dynamic changes in the mouse skeletal muscle proteome during denervation-induced atrophy

Dynamic changes in the mouse skeletal muscle proteome during denervation-induced atrophy

Loss of neuronal stimulation enhances protein breakdown and reduces protein synthesis, causing rapid loss of muscle mass. To elucidate the pathophysiological adaptations that occur in atrophying muscles, we used stable isotope labelling and mass spectrometry to quantify protein expression changes ac...

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Main Authors: Franziska Lang, Sriram Aravamudhan, Hendrik Nolte, Clara Türk, Soraya Hölper, Stefan Müller, Stefan Günther, Bert Blaauw, Thomas Braun, Marcus Krüger
Format: Article
Language:English
Published: The Company of Biologists 2017-07-01
Series:Disease Models & Mechanisms
Subjects:
Muscle atrophy
Denervation
Pulsed SILAC
Ubiquitination
Random forest
Online Access:http://dmm.biologists.org/content/10/7/881
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spelling doaj-d21884356e0f497c8ab97e2ecf126f942020-11-24T21:50:22ZengThe Company of BiologistsDisease Models & Mechanisms1754-84031754-84112017-07-0110788189610.1242/dmm.028910028910Dynamic changes in the mouse skeletal muscle proteome during denervation-induced atrophyFranziska Lang0Sriram Aravamudhan1Hendrik Nolte2Clara Türk3Soraya Hölper4Stefan Müller5Stefan Günther6Bert Blaauw7Thomas Braun8Marcus Krüger9 Institute for Genetics, Cologne Excellence Cluster on Cellular Stress Responses in Aging-Associated Diseases (CECAD), 50931 Cologne, Germany Max Planck Institute for Heart and Lung Research, 61231 Bad Nauheim, Germany Institute for Genetics, Cologne Excellence Cluster on Cellular Stress Responses in Aging-Associated Diseases (CECAD), 50931 Cologne, Germany Institute for Genetics, Cologne Excellence Cluster on Cellular Stress Responses in Aging-Associated Diseases (CECAD), 50931 Cologne, Germany Institute of Biochemistry II, Goethe University Medical School, 60590 Frankfurt, Germany Center for Molecular Medicine (CMMC), University of Cologne, 50931 Cologne, Germany Max Planck Institute for Heart and Lung Research, 61231 Bad Nauheim, Germany Venetian Institute of Molecular Medicine (VIMM), Department of Biomedical Sciences Padova, University of Padova, 35137 Padova, Italy Max Planck Institute for Heart and Lung Research, 61231 Bad Nauheim, Germany Institute for Genetics, Cologne Excellence Cluster on Cellular Stress Responses in Aging-Associated Diseases (CECAD), 50931 Cologne, Germany Loss of neuronal stimulation enhances protein breakdown and reduces protein synthesis, causing rapid loss of muscle mass. To elucidate the pathophysiological adaptations that occur in atrophying muscles, we used stable isotope labelling and mass spectrometry to quantify protein expression changes accurately during denervation-induced atrophy after sciatic nerve section in the mouse gastrocnemius muscle. Additionally, mice were fed a stable isotope labelling of amino acids in cell culture (SILAC) diet containing 13C6-lysine for 4, 7 or 11 days to calculate relative levels of protein synthesis in denervated and control muscles. Ubiquitin remnant peptides (K-ε-GG) were profiled by immunoaffinity enrichment to identify potential substrates of the ubiquitin-proteasomal pathway. Of the 4279 skeletal muscle proteins quantified, 850 were differentially expressed significantly within 2 weeks after denervation compared with control muscles. Moreover, pulse labelling identified Lys6 incorporation in 4786 proteins, of which 43 had differential Lys6 incorporation between control and denervated muscle. Enrichment of diglycine remnants identified 2100 endogenous ubiquitination sites and revealed a metabolic and myofibrillar protein diglycine signature, including myosin heavy chains, myomesins and titin, during denervation. Comparative analysis of these proteomic data sets with known atrogenes using a random forest approach identified 92 proteins subject to atrogene-like regulation that have not previously been associated directly with denervation-induced atrophy. Comparison of protein synthesis and proteomic data indicated that upregulation of specific proteins in response to denervation is mainly achieved by protein stabilization. This study provides the first integrated analysis of protein expression, synthesis and ubiquitin signatures during muscular atrophy in a living animal.http://dmm.biologists.org/content/10/7/881Muscle atrophyDenervationPulsed SILACUbiquitinationRandom forest
collection DOAJ
language English
format Article
sources DOAJ
author Franziska Lang
Sriram Aravamudhan
Hendrik Nolte
Clara Türk
Soraya Hölper
Stefan Müller
Stefan Günther
Bert Blaauw
Thomas Braun
Marcus Krüger
spellingShingle Franziska Lang
Sriram Aravamudhan
Hendrik Nolte
Clara Türk
Soraya Hölper
Stefan Müller
Stefan Günther
Bert Blaauw
Thomas Braun
Marcus Krüger
Dynamic changes in the mouse skeletal muscle proteome during denervation-induced atrophy
Disease Models & Mechanisms
Muscle atrophy
Denervation
Pulsed SILAC
Ubiquitination
Random forest
author_facet Franziska Lang
Sriram Aravamudhan
Hendrik Nolte
Clara Türk
Soraya Hölper
Stefan Müller
Stefan Günther
Bert Blaauw
Thomas Braun
Marcus Krüger
author_sort Franziska Lang
title Dynamic changes in the mouse skeletal muscle proteome during denervation-induced atrophy
title_short Dynamic changes in the mouse skeletal muscle proteome during denervation-induced atrophy
title_full Dynamic changes in the mouse skeletal muscle proteome during denervation-induced atrophy
title_fullStr Dynamic changes in the mouse skeletal muscle proteome during denervation-induced atrophy
title_full_unstemmed Dynamic changes in the mouse skeletal muscle proteome during denervation-induced atrophy
title_sort dynamic changes in the mouse skeletal muscle proteome during denervation-induced atrophy
publisher The Company of Biologists
series Disease Models & Mechanisms
issn 1754-8403
1754-8411
publishDate 2017-07-01
description Loss of neuronal stimulation enhances protein breakdown and reduces protein synthesis, causing rapid loss of muscle mass. To elucidate the pathophysiological adaptations that occur in atrophying muscles, we used stable isotope labelling and mass spectrometry to quantify protein expression changes accurately during denervation-induced atrophy after sciatic nerve section in the mouse gastrocnemius muscle. Additionally, mice were fed a stable isotope labelling of amino acids in cell culture (SILAC) diet containing 13C6-lysine for 4, 7 or 11 days to calculate relative levels of protein synthesis in denervated and control muscles. Ubiquitin remnant peptides (K-ε-GG) were profiled by immunoaffinity enrichment to identify potential substrates of the ubiquitin-proteasomal pathway. Of the 4279 skeletal muscle proteins quantified, 850 were differentially expressed significantly within 2 weeks after denervation compared with control muscles. Moreover, pulse labelling identified Lys6 incorporation in 4786 proteins, of which 43 had differential Lys6 incorporation between control and denervated muscle. Enrichment of diglycine remnants identified 2100 endogenous ubiquitination sites and revealed a metabolic and myofibrillar protein diglycine signature, including myosin heavy chains, myomesins and titin, during denervation. Comparative analysis of these proteomic data sets with known atrogenes using a random forest approach identified 92 proteins subject to atrogene-like regulation that have not previously been associated directly with denervation-induced atrophy. Comparison of protein synthesis and proteomic data indicated that upregulation of specific proteins in response to denervation is mainly achieved by protein stabilization. This study provides the first integrated analysis of protein expression, synthesis and ubiquitin signatures during muscular atrophy in a living animal.
topic Muscle atrophy
Denervation
Pulsed SILAC
Ubiquitination
Random forest
url http://dmm.biologists.org/content/10/7/881
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