Skeletal muscle myosin cross‐bridge cycling is necessary for myofibrillogenesis

Abstract A major stimulus affecting myofibrillogenesis in both embryonic and mature striated muscle is contractile activity. There are two major signals associated with contractile activity: a physiological signal, the transient increase in intracellular calcium, and a physical signal, the transient...

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Published in:Cell Motility
Main Authors: Ramachandran, Indu, Terry, Monica, Ferrari, Michael B.
Format: Article in Journal/Newspaper
Language:English
Published: Wiley 2003
Subjects:
Avian Studies
Online Access:http://dx.doi.org/10.1002/cm.10113
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spelling crwiley:10.1002/cm.10113 2024-06-02T08:03:47+00:00 Skeletal muscle myosin cross‐bridge cycling is necessary for myofibrillogenesis Ramachandran, Indu Terry, Monica Ferrari, Michael B. 2003 http://dx.doi.org/10.1002/cm.10113 https://api.wiley.com/onlinelibrary/tdm/v1/articles/10.1002%2Fcm.10113 https://onlinelibrary.wiley.com/doi/pdf/10.1002/cm.10113 en eng Wiley http://onlinelibrary.wiley.com/termsAndConditions#vor Cell Motility volume 55, issue 1, page 61-72 ISSN 0886-1544 journal-article 2003 crwiley https://doi.org/10.1002/cm.10113 2024-05-03T11:43:25Z Abstract A major stimulus affecting myofibrillogenesis in both embryonic and mature striated muscle is contractile activity. There are two major signals associated with contractile activity: a physiological signal, the transient increase in intracellular calcium, and a physical signal, the transient increase in tension production. However, dissociating these two signals to examine their relative contributions to myofibrillogenesis has proven difficult. In this study, we have used two different myosin inhibitors to determine the importance of myosin cross‐bridge cycling in sarcomere assembly. We find that the small‐molecule inhibitor 2,3‐butanedione monoxime (BDM), which inhibits myosin ATPase, disrupts myofibrillogenesis in amphibian myocytes, consistent with results from avian studies. However, BDM is a weak myosin inhibitor and it is non‐specific; concentrations that inhibit contraction and disrupt myofibrillogenesis also disrupt calcium signaling. Therefore, we also used the recently identified skeletal muscle myosin II inhibitor, N ‐benzyl‐ p ‐toluenesulphonamide (BTS), which has high affinity and specificity for skeletal muscle fast myosin. BTS inhibits contraction and results in myofibrillar disruption that phenocopies our results with BDM. However, BTS does not affect either spontaneous or induced calcium transients. Furthermore, BTS is reversible and does not significantly affect the expression levels of myosin or actin. Thus, our convergent results with BDM and BTS suggest that sarcomere assembly depends on active regulation of tension in the forming myofibril. Cell Motil. Cytoskeleton 55:61–72, 2003. © 2003 Wiley‐Liss, Inc. Article in Journal/Newspaper Avian Studies Wiley Online Library Cell Motility 55 1 61 72
institution Open Polar
collection Wiley Online Library
op_collection_id crwiley
language English
description Abstract A major stimulus affecting myofibrillogenesis in both embryonic and mature striated muscle is contractile activity. There are two major signals associated with contractile activity: a physiological signal, the transient increase in intracellular calcium, and a physical signal, the transient increase in tension production. However, dissociating these two signals to examine their relative contributions to myofibrillogenesis has proven difficult. In this study, we have used two different myosin inhibitors to determine the importance of myosin cross‐bridge cycling in sarcomere assembly. We find that the small‐molecule inhibitor 2,3‐butanedione monoxime (BDM), which inhibits myosin ATPase, disrupts myofibrillogenesis in amphibian myocytes, consistent with results from avian studies. However, BDM is a weak myosin inhibitor and it is non‐specific; concentrations that inhibit contraction and disrupt myofibrillogenesis also disrupt calcium signaling. Therefore, we also used the recently identified skeletal muscle myosin II inhibitor, N ‐benzyl‐ p ‐toluenesulphonamide (BTS), which has high affinity and specificity for skeletal muscle fast myosin. BTS inhibits contraction and results in myofibrillar disruption that phenocopies our results with BDM. However, BTS does not affect either spontaneous or induced calcium transients. Furthermore, BTS is reversible and does not significantly affect the expression levels of myosin or actin. Thus, our convergent results with BDM and BTS suggest that sarcomere assembly depends on active regulation of tension in the forming myofibril. Cell Motil. Cytoskeleton 55:61–72, 2003. © 2003 Wiley‐Liss, Inc.
format Article in Journal/Newspaper
author Ramachandran, Indu
Terry, Monica
Ferrari, Michael B.
spellingShingle Ramachandran, Indu
Terry, Monica
Ferrari, Michael B.
Skeletal muscle myosin cross‐bridge cycling is necessary for myofibrillogenesis
author_facet Ramachandran, Indu
Terry, Monica
Ferrari, Michael B.
author_sort Ramachandran, Indu
title Skeletal muscle myosin cross‐bridge cycling is necessary for myofibrillogenesis
title_short Skeletal muscle myosin cross‐bridge cycling is necessary for myofibrillogenesis
title_full Skeletal muscle myosin cross‐bridge cycling is necessary for myofibrillogenesis
title_fullStr Skeletal muscle myosin cross‐bridge cycling is necessary for myofibrillogenesis
title_full_unstemmed Skeletal muscle myosin cross‐bridge cycling is necessary for myofibrillogenesis
title_sort skeletal muscle myosin cross‐bridge cycling is necessary for myofibrillogenesis
publisher Wiley
publishDate 2003
url http://dx.doi.org/10.1002/cm.10113
https://api.wiley.com/onlinelibrary/tdm/v1/articles/10.1002%2Fcm.10113
https://onlinelibrary.wiley.com/doi/pdf/10.1002/cm.10113
genre Avian Studies
genre_facet Avian Studies
op_source Cell Motility
volume 55, issue 1, page 61-72
ISSN 0886-1544
op_rights http://onlinelibrary.wiley.com/termsAndConditions#vor
op_doi https://doi.org/10.1002/cm.10113
container_title Cell Motility
container_volume 55
container_issue 1
container_start_page 61
op_container_end_page 72
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