High-throughput proteomics fiber typing (ProFiT) for comprehensive characterization of single skeletal muscle fibers

High-throughput proteomics fiber typing (ProFiT) for comprehensive characterization of single skeletal muscle fibers

Abstract Background Skeletal muscles are composed of a heterogeneous collection of fiber types with different physiological adaption in response to a stimulus and disease-related conditions. Each fiber has a specific molecular expression of myosin heavy chain molecules (MyHC). So far, MyHCs are curr...

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Main Authors: Sebastian Kallabis, Lena Abraham, Stefan Müller, Verena Dzialas, Clara Türk, Janica Lea Wiederstein, Theresa Bock, Hendrik Nolte, Leonardo Nogara, Bert Blaauw, Thomas Braun, Marcus Krüger
Format: Article
Language:English
Published: BMC 2020-03-01
Series:Skeletal Muscle
Subjects:
Muscle fiber proteomics
MyHC profiling
Protein turnover
Phosphoproteomics
Online Access:http://link.springer.com/article/10.1186/s13395-020-00226-5
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spelling doaj-277cd04e3dab44c684355adea4b6995b2020-11-25T02:19:41ZengBMCSkeletal Muscle2044-50402020-03-0110111810.1186/s13395-020-00226-5High-throughput proteomics fiber typing (ProFiT) for comprehensive characterization of single skeletal muscle fibersSebastian Kallabis0Lena Abraham1Stefan Müller2Verena Dzialas3Clara Türk4Janica Lea Wiederstein5Theresa Bock6Hendrik Nolte7Leonardo Nogara8Bert Blaauw9Thomas Braun10Marcus Krüger11CECAD Research Center, Institute for Genetics, University of CologneCECAD Research Center, Institute for Genetics, University of CologneCECAD Research Center, Institute for Genetics, University of CologneCECAD Research Center, Institute for Genetics, University of CologneCECAD Research Center, Institute for Genetics, University of CologneCECAD Research Center, Institute for Genetics, University of CologneCECAD Research Center, Institute for Genetics, University of CologneMax Planck Institute for the Biology of AgingVenetian Institute of Molecular Medicine (VIMM)Venetian Institute of Molecular Medicine (VIMM)Max Planck Institute for Heart and Lung ResearchCECAD Research Center, Institute for Genetics, University of CologneAbstract Background Skeletal muscles are composed of a heterogeneous collection of fiber types with different physiological adaption in response to a stimulus and disease-related conditions. Each fiber has a specific molecular expression of myosin heavy chain molecules (MyHC). So far, MyHCs are currently the best marker proteins for characterization of individual fiber types, and several proteome profiling studies have helped to dissect the molecular signature of whole muscles and individual fibers. Methods Herein, we describe a mass spectrometric workflow to measure skeletal muscle fiber type-specific proteomes. To bypass the limited quantities of protein in single fibers, we developed a Proteomics high-throughput fiber typing (ProFiT) approach enabling profiling of MyHC in single fibers. Aliquots of protein extracts from separated muscle fibers were subjected to capillary LC-MS gradients to profile MyHC isoforms in a 96-well format. Muscle fibers with the same MyHC protein expression were pooled and subjected to proteomic, pulsed-SILAC, and phosphoproteomic analysis. Results Our fiber type-specific quantitative proteome analysis confirmed the distribution of fiber types in the soleus muscle, substantiates metabolic adaptions in oxidative and glycolytic fibers, and highlighted significant differences between the proteomes of type IIb fibers from different muscle groups, including a differential expression of desmin and actinin-3. A detailed map of the Lys-6 incorporation rates in muscle fibers showed an increased turnover of slow fibers compared to fast fibers. In addition, labeling of mitochondrial respiratory chain complexes revealed a broad range of Lys-6 incorporation rates, depending on the localization of the subunits within distinct complexes. Conclusion Overall, the ProFiT approach provides a versatile tool to rapidly characterize muscle fibers and obtain fiber-specific proteomes for different muscle groups.http://link.springer.com/article/10.1186/s13395-020-00226-5Muscle fiber proteomicsMyHC profilingProtein turnoverPhosphoproteomics
collection DOAJ
language English
format Article
sources DOAJ
author Sebastian Kallabis
Lena Abraham
Stefan Müller
Verena Dzialas
Clara Türk
Janica Lea Wiederstein
Theresa Bock
Hendrik Nolte
Leonardo Nogara
Bert Blaauw
Thomas Braun
Marcus Krüger
spellingShingle Sebastian Kallabis
Lena Abraham
Stefan Müller
Verena Dzialas
Clara Türk
Janica Lea Wiederstein
Theresa Bock
Hendrik Nolte
Leonardo Nogara
Bert Blaauw
Thomas Braun
Marcus Krüger
High-throughput proteomics fiber typing (ProFiT) for comprehensive characterization of single skeletal muscle fibers
Skeletal Muscle
Muscle fiber proteomics
MyHC profiling
Protein turnover
Phosphoproteomics
author_facet Sebastian Kallabis
Lena Abraham
Stefan Müller
Verena Dzialas
Clara Türk
Janica Lea Wiederstein
Theresa Bock
Hendrik Nolte
Leonardo Nogara
Bert Blaauw
Thomas Braun
Marcus Krüger
author_sort Sebastian Kallabis
title High-throughput proteomics fiber typing (ProFiT) for comprehensive characterization of single skeletal muscle fibers
title_short High-throughput proteomics fiber typing (ProFiT) for comprehensive characterization of single skeletal muscle fibers
title_full High-throughput proteomics fiber typing (ProFiT) for comprehensive characterization of single skeletal muscle fibers
title_fullStr High-throughput proteomics fiber typing (ProFiT) for comprehensive characterization of single skeletal muscle fibers
title_full_unstemmed High-throughput proteomics fiber typing (ProFiT) for comprehensive characterization of single skeletal muscle fibers
title_sort high-throughput proteomics fiber typing (profit) for comprehensive characterization of single skeletal muscle fibers
publisher BMC
series Skeletal Muscle
issn 2044-5040
publishDate 2020-03-01
description Abstract Background Skeletal muscles are composed of a heterogeneous collection of fiber types with different physiological adaption in response to a stimulus and disease-related conditions. Each fiber has a specific molecular expression of myosin heavy chain molecules (MyHC). So far, MyHCs are currently the best marker proteins for characterization of individual fiber types, and several proteome profiling studies have helped to dissect the molecular signature of whole muscles and individual fibers. Methods Herein, we describe a mass spectrometric workflow to measure skeletal muscle fiber type-specific proteomes. To bypass the limited quantities of protein in single fibers, we developed a Proteomics high-throughput fiber typing (ProFiT) approach enabling profiling of MyHC in single fibers. Aliquots of protein extracts from separated muscle fibers were subjected to capillary LC-MS gradients to profile MyHC isoforms in a 96-well format. Muscle fibers with the same MyHC protein expression were pooled and subjected to proteomic, pulsed-SILAC, and phosphoproteomic analysis. Results Our fiber type-specific quantitative proteome analysis confirmed the distribution of fiber types in the soleus muscle, substantiates metabolic adaptions in oxidative and glycolytic fibers, and highlighted significant differences between the proteomes of type IIb fibers from different muscle groups, including a differential expression of desmin and actinin-3. A detailed map of the Lys-6 incorporation rates in muscle fibers showed an increased turnover of slow fibers compared to fast fibers. In addition, labeling of mitochondrial respiratory chain complexes revealed a broad range of Lys-6 incorporation rates, depending on the localization of the subunits within distinct complexes. Conclusion Overall, the ProFiT approach provides a versatile tool to rapidly characterize muscle fibers and obtain fiber-specific proteomes for different muscle groups.
topic Muscle fiber proteomics
MyHC profiling
Protein turnover
Phosphoproteomics
url http://link.springer.com/article/10.1186/s13395-020-00226-5
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