X-ROS Signaling Depends on Length-Dependent Calcium Buffering by Troponin

The stretching of a cardiomyocyte leads to the increased production of reactive oxygen species that increases ryanodine receptor open probability through a process termed X-ROS signaling. The stretching of the myocyte also increases the calcium affinity of myofilament Troponin C, which increases its...

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Main Authors: Sarita Limbu, Benjamin L. Prosser, William J. Lederer, Christopher W. Ward, Mohsin S. Jafri
Format: Article
Language:English
Published: MDPI AG 2021-05-01
Series:Cells
Subjects:
Online Access:https://www.mdpi.com/2073-4409/10/5/1189
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spelling doaj-f5d296ac36e6474ca7a634b3977f45902021-05-31T23:53:21ZengMDPI AGCells2073-44092021-05-01101189118910.3390/cells10051189X-ROS Signaling Depends on Length-Dependent Calcium Buffering by TroponinSarita Limbu0Benjamin L. Prosser1William J. Lederer2Christopher W. Ward3Mohsin S. Jafri4School of Systems Biology and The Krasnow Institute for Advanced Study, George Mason University, Fairfax, VA 22030, USADepartment of Physiology, Pennsylvania Muscle Institute, University of Pennsylvania Perelman School of Medicine, Philadelphia, PA 19104, USACenter for Biomedical Engineering and Technology, University of Maryland School of Medicine, Baltimore, MD 20201, USACenter for Biomedical Engineering and Technology and Department of Orthopaedics, University of Maryland School of Medicine, Baltimore, MD 20201, USASchool of Systems Biology and The Krasnow Institute for Advanced Study, George Mason University, Fairfax, VA 22030, USAThe stretching of a cardiomyocyte leads to the increased production of reactive oxygen species that increases ryanodine receptor open probability through a process termed X-ROS signaling. The stretching of the myocyte also increases the calcium affinity of myofilament Troponin C, which increases its calcium buffering capacity. Here, an integrative experimental and modeling study is pursued to explain the interplay of length-dependent changes in calcium buffering by troponin and stretch-activated X-ROS calcium signaling. Using this combination, we show that the troponin C-dependent increase in myoplasmic calcium buffering during myocyte stretching largely offsets the X-ROS-dependent increase in calcium release from the sarcoplasmic reticulum. The combination of modeling and experiment are further informed by the elimination of length-dependent changes to troponin C calcium binding in the presence of blebbistatin. Here, the model suggests that it is the X-ROS signaling-dependent Ca<sup>2+</sup> release increase that serves to maintain free myoplasmic calcium concentrations during a change in myocyte length. Together, our experimental and modeling approaches have further defined the relative contributions of X-ROS signaling and the length-dependent calcium buffering by troponin in shaping the myoplasmic calcium transient.https://www.mdpi.com/2073-4409/10/5/1189heartreactive oxygen speciescalciumblebbistatincomputational model
collection DOAJ
language English
format Article
sources DOAJ
author Sarita Limbu
Benjamin L. Prosser
William J. Lederer
Christopher W. Ward
Mohsin S. Jafri
spellingShingle Sarita Limbu
Benjamin L. Prosser
William J. Lederer
Christopher W. Ward
Mohsin S. Jafri
X-ROS Signaling Depends on Length-Dependent Calcium Buffering by Troponin
Cells
heart
reactive oxygen species
calcium
blebbistatin
computational model
author_facet Sarita Limbu
Benjamin L. Prosser
William J. Lederer
Christopher W. Ward
Mohsin S. Jafri
author_sort Sarita Limbu
title X-ROS Signaling Depends on Length-Dependent Calcium Buffering by Troponin
title_short X-ROS Signaling Depends on Length-Dependent Calcium Buffering by Troponin
title_full X-ROS Signaling Depends on Length-Dependent Calcium Buffering by Troponin
title_fullStr X-ROS Signaling Depends on Length-Dependent Calcium Buffering by Troponin
title_full_unstemmed X-ROS Signaling Depends on Length-Dependent Calcium Buffering by Troponin
title_sort x-ros signaling depends on length-dependent calcium buffering by troponin
publisher MDPI AG
series Cells
issn 2073-4409
publishDate 2021-05-01
description The stretching of a cardiomyocyte leads to the increased production of reactive oxygen species that increases ryanodine receptor open probability through a process termed X-ROS signaling. The stretching of the myocyte also increases the calcium affinity of myofilament Troponin C, which increases its calcium buffering capacity. Here, an integrative experimental and modeling study is pursued to explain the interplay of length-dependent changes in calcium buffering by troponin and stretch-activated X-ROS calcium signaling. Using this combination, we show that the troponin C-dependent increase in myoplasmic calcium buffering during myocyte stretching largely offsets the X-ROS-dependent increase in calcium release from the sarcoplasmic reticulum. The combination of modeling and experiment are further informed by the elimination of length-dependent changes to troponin C calcium binding in the presence of blebbistatin. Here, the model suggests that it is the X-ROS signaling-dependent Ca<sup>2+</sup> release increase that serves to maintain free myoplasmic calcium concentrations during a change in myocyte length. Together, our experimental and modeling approaches have further defined the relative contributions of X-ROS signaling and the length-dependent calcium buffering by troponin in shaping the myoplasmic calcium transient.
topic heart
reactive oxygen species
calcium
blebbistatin
computational model
url https://www.mdpi.com/2073-4409/10/5/1189
work_keys_str_mv AT saritalimbu xrossignalingdependsonlengthdependentcalciumbufferingbytroponin
AT benjaminlprosser xrossignalingdependsonlengthdependentcalciumbufferingbytroponin
AT williamjlederer xrossignalingdependsonlengthdependentcalciumbufferingbytroponin
AT christopherwward xrossignalingdependsonlengthdependentcalciumbufferingbytroponin
AT mohsinsjafri xrossignalingdependsonlengthdependentcalciumbufferingbytroponin
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