Skeletal Muscle Expression of the Adhesion-GPCR CD97: CD97 Deletion Induces an Abnormal Structure of the Sarcoplasmatic Reticulum but Does Not Impair Skeletal Muscle Function

CD97 is a widely expressed adhesion class G-protein-coupled receptor (aGPCR). Here, we investigated the presence of CD97 in normal and malignant human skeletal muscle as well as the ultrastructural and functional consequences of CD97 deficiency in mice. In normal human skeletal muscle, CD97 was expr...

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Autores principales: Zyryanova, Tatiana, Schneider, Rick, Adams, Volker, Sittig, Doreen, Kerner, Christiane, Gebhardt, Claudia, Ruffert, Henrik, Glasmacher, Stefan, Hepp, Pierre, Punkt, Karla, Neuhaus, Jochen, Hamann, Jörg, Aust, Gabriela
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4065095/
https://www.ncbi.nlm.nih.gov/pubmed/24949957
http://dx.doi.org/10.1371/journal.pone.0100513
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author Zyryanova, Tatiana
Schneider, Rick
Adams, Volker
Sittig, Doreen
Kerner, Christiane
Gebhardt, Claudia
Ruffert, Henrik
Glasmacher, Stefan
Hepp, Pierre
Punkt, Karla
Neuhaus, Jochen
Hamann, Jörg
Aust, Gabriela
author_facet Zyryanova, Tatiana
Schneider, Rick
Adams, Volker
Sittig, Doreen
Kerner, Christiane
Gebhardt, Claudia
Ruffert, Henrik
Glasmacher, Stefan
Hepp, Pierre
Punkt, Karla
Neuhaus, Jochen
Hamann, Jörg
Aust, Gabriela
author_sort Zyryanova, Tatiana
collection PubMed
description CD97 is a widely expressed adhesion class G-protein-coupled receptor (aGPCR). Here, we investigated the presence of CD97 in normal and malignant human skeletal muscle as well as the ultrastructural and functional consequences of CD97 deficiency in mice. In normal human skeletal muscle, CD97 was expressed at the peripheral sarcolemma of all myofibers, as revealed by immunostaining of tissue sections and surface labeling of single myocytes using flow cytometry. In muscle cross-sections, an intracellular polygonal, honeycomb-like CD97-staining pattern, typical for molecules located in the T-tubule or sarcoplasmatic reticulum (SR), was additionally found. CD97 co-localized with SR Ca(2+)-ATPase (SERCA), a constituent of the longitudinal SR, but not with the receptors for dihydropyridine (DHPR) or ryanodine (RYR), located in the T-tubule and terminal SR, respectively. Intracellular expression of CD97 was higher in slow-twitch compared to most fast-twitch myofibers. In rhabdomyosarcomas, CD97 was strongly upregulated and in part more N-glycosylated compared to normal skeletal muscle. All tumors were strongly CD97-positive, independent of the underlying histological subtype, suggesting high sensitivity of CD97 for this tumor. Ultrastructural analysis of murine skeletal myofibers confirmed the location of CD97 in the SR. CD97 knock-out mice had a dilated SR, resulting in a partial increase in triad diameter yet not affecting the T-tubule, sarcomeric, and mitochondrial structure. Despite these obvious ultrastructural changes, intracellular Ca(2+) release from single myofibers, force generation and fatigability of isolated soleus muscles, and wheel-running capacity of mice were not affected by the lack of CD97. We conclude that CD97 is located in the SR and at the peripheral sarcolemma of human and murine skeletal muscle, where its absence affects the structure of the SR without impairing skeletal muscle function.
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spelling pubmed-40650952014-06-25 Skeletal Muscle Expression of the Adhesion-GPCR CD97: CD97 Deletion Induces an Abnormal Structure of the Sarcoplasmatic Reticulum but Does Not Impair Skeletal Muscle Function Zyryanova, Tatiana Schneider, Rick Adams, Volker Sittig, Doreen Kerner, Christiane Gebhardt, Claudia Ruffert, Henrik Glasmacher, Stefan Hepp, Pierre Punkt, Karla Neuhaus, Jochen Hamann, Jörg Aust, Gabriela PLoS One Research Article CD97 is a widely expressed adhesion class G-protein-coupled receptor (aGPCR). Here, we investigated the presence of CD97 in normal and malignant human skeletal muscle as well as the ultrastructural and functional consequences of CD97 deficiency in mice. In normal human skeletal muscle, CD97 was expressed at the peripheral sarcolemma of all myofibers, as revealed by immunostaining of tissue sections and surface labeling of single myocytes using flow cytometry. In muscle cross-sections, an intracellular polygonal, honeycomb-like CD97-staining pattern, typical for molecules located in the T-tubule or sarcoplasmatic reticulum (SR), was additionally found. CD97 co-localized with SR Ca(2+)-ATPase (SERCA), a constituent of the longitudinal SR, but not with the receptors for dihydropyridine (DHPR) or ryanodine (RYR), located in the T-tubule and terminal SR, respectively. Intracellular expression of CD97 was higher in slow-twitch compared to most fast-twitch myofibers. In rhabdomyosarcomas, CD97 was strongly upregulated and in part more N-glycosylated compared to normal skeletal muscle. All tumors were strongly CD97-positive, independent of the underlying histological subtype, suggesting high sensitivity of CD97 for this tumor. Ultrastructural analysis of murine skeletal myofibers confirmed the location of CD97 in the SR. CD97 knock-out mice had a dilated SR, resulting in a partial increase in triad diameter yet not affecting the T-tubule, sarcomeric, and mitochondrial structure. Despite these obvious ultrastructural changes, intracellular Ca(2+) release from single myofibers, force generation and fatigability of isolated soleus muscles, and wheel-running capacity of mice were not affected by the lack of CD97. We conclude that CD97 is located in the SR and at the peripheral sarcolemma of human and murine skeletal muscle, where its absence affects the structure of the SR without impairing skeletal muscle function. Public Library of Science 2014-06-20 /pmc/articles/PMC4065095/ /pubmed/24949957 http://dx.doi.org/10.1371/journal.pone.0100513 Text en © 2014 Zyryanova et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Zyryanova, Tatiana
Schneider, Rick
Adams, Volker
Sittig, Doreen
Kerner, Christiane
Gebhardt, Claudia
Ruffert, Henrik
Glasmacher, Stefan
Hepp, Pierre
Punkt, Karla
Neuhaus, Jochen
Hamann, Jörg
Aust, Gabriela
Skeletal Muscle Expression of the Adhesion-GPCR CD97: CD97 Deletion Induces an Abnormal Structure of the Sarcoplasmatic Reticulum but Does Not Impair Skeletal Muscle Function
title Skeletal Muscle Expression of the Adhesion-GPCR CD97: CD97 Deletion Induces an Abnormal Structure of the Sarcoplasmatic Reticulum but Does Not Impair Skeletal Muscle Function
title_full Skeletal Muscle Expression of the Adhesion-GPCR CD97: CD97 Deletion Induces an Abnormal Structure of the Sarcoplasmatic Reticulum but Does Not Impair Skeletal Muscle Function
title_fullStr Skeletal Muscle Expression of the Adhesion-GPCR CD97: CD97 Deletion Induces an Abnormal Structure of the Sarcoplasmatic Reticulum but Does Not Impair Skeletal Muscle Function
title_full_unstemmed Skeletal Muscle Expression of the Adhesion-GPCR CD97: CD97 Deletion Induces an Abnormal Structure of the Sarcoplasmatic Reticulum but Does Not Impair Skeletal Muscle Function
title_short Skeletal Muscle Expression of the Adhesion-GPCR CD97: CD97 Deletion Induces an Abnormal Structure of the Sarcoplasmatic Reticulum but Does Not Impair Skeletal Muscle Function
title_sort skeletal muscle expression of the adhesion-gpcr cd97: cd97 deletion induces an abnormal structure of the sarcoplasmatic reticulum but does not impair skeletal muscle function
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4065095/
https://www.ncbi.nlm.nih.gov/pubmed/24949957
http://dx.doi.org/10.1371/journal.pone.0100513
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