Deleting Titin’s C-Terminal PEVK Exons Increases Passive Stiffness, Alters Splicing, and Induces Cross-Sectional and Longitudinal Hypertrophy in Skeletal Muscle

The Proline, Glutamate, Valine and Lysine-rich (PEVK) region of titin constitutes an entropic spring that provides passive tension to striated muscle. To study the functional and structural repercussions of a small reduction in the size of the PEVK region, we investigated skeletal muscles of a mouse...

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Autores principales: van der Pijl, Robbert J., Hudson, Brian, Granzier-Nakajima, Tomotaroh, Li, Frank, Knottnerus, Anne M., Smith, John, Chung, Charles S., Gotthardt, Michael, Granzier, Henk L., Ottenheijm, Coen A. C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Physiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7274174/
https://www.ncbi.nlm.nih.gov/pubmed/32547410
http://dx.doi.org/10.3389/fphys.2020.00494
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author van der Pijl, Robbert J.
Hudson, Brian
Granzier-Nakajima, Tomotaroh
Li, Frank
Knottnerus, Anne M.
Smith, John
Chung, Charles S.
Gotthardt, Michael
Granzier, Henk L.
Ottenheijm, Coen A. C.
author_facet van der Pijl, Robbert J.
Hudson, Brian
Granzier-Nakajima, Tomotaroh
Li, Frank
Knottnerus, Anne M.
Smith, John
Chung, Charles S.
Gotthardt, Michael
Granzier, Henk L.
Ottenheijm, Coen A. C.
author_sort van der Pijl, Robbert J.
collection PubMed
description The Proline, Glutamate, Valine and Lysine-rich (PEVK) region of titin constitutes an entropic spring that provides passive tension to striated muscle. To study the functional and structural repercussions of a small reduction in the size of the PEVK region, we investigated skeletal muscles of a mouse with the constitutively expressed C-terminal PEVK exons 219–225 deleted, the Ttn(Δ219–225) model (MGI: Ttn(TM 2.1Mgot)). Based on this deletion, passive tension in skeletal muscle was predicted to be increased by ∼17% (sarcomere length 3.0 μm). In contrast, measured passive tension (sarcomere length 3.0 μm) in both soleus and EDL muscles was increased 53 ± 11% and 62 ± 4%, respectively. This unexpected increase was due to changes in titin, not to alterations in the extracellular matrix, and is likely caused by co-expression of two titin isoforms in Ttn(Δ219–225) muscles: a larger isoform that represents the Ttn(Δ219–225) N2A titin and a smaller isoform, referred to as N2A2. N2A2 represents a splicing adaption with reduced expression of spring element exons, as determined by titin exon microarray analysis. Maximal tetanic tension was increased in Ttn(Δ219–225) soleus muscle (WT 240 ± 9; Ttn(Δ219–225) 276 ± 17 mN/mm(2)), but was reduced in EDL muscle (WT 315 ± 9; Ttn(Δ219–225) 280 ± 14 mN/mm(2)). The changes in active tension coincided with a switch toward slow fiber types and, unexpectedly, faster kinetics of tension generation and relaxation. Functional overload (FO; ablation) and hindlimb suspension (HS; unloading) experiments were also conducted. Ttn(Δ219–225) mice showed increases in both longitudinal hypertrophy (increased number of sarcomeres in series) and cross-sectional hypertrophy (increased number of sarcomeres in parallel) in response to FO and attenuated cross-sectional atrophy in response to HS. In summary, slow- and fast-twitch muscles in a mouse model devoid of titin’s PEVK exons 219–225 have high passive tension, due in part to alterations elsewhere in splicing of titin’s spring region, increased kinetics of tension generation and relaxation, and altered trophic responses to both functional overload and unloading. This implicates titin’s C-terminal PEVK region in regulating passive and active muscle mechanics and muscle plasticity.
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spelling pubmed-72741742020-06-15 Deleting Titin’s C-Terminal PEVK Exons Increases Passive Stiffness, Alters Splicing, and Induces Cross-Sectional and Longitudinal Hypertrophy in Skeletal Muscle van der Pijl, Robbert J. Hudson, Brian Granzier-Nakajima, Tomotaroh Li, Frank Knottnerus, Anne M. Smith, John Chung, Charles S. Gotthardt, Michael Granzier, Henk L. Ottenheijm, Coen A. C. Front Physiol Physiology The Proline, Glutamate, Valine and Lysine-rich (PEVK) region of titin constitutes an entropic spring that provides passive tension to striated muscle. To study the functional and structural repercussions of a small reduction in the size of the PEVK region, we investigated skeletal muscles of a mouse with the constitutively expressed C-terminal PEVK exons 219–225 deleted, the Ttn(Δ219–225) model (MGI: Ttn(TM 2.1Mgot)). Based on this deletion, passive tension in skeletal muscle was predicted to be increased by ∼17% (sarcomere length 3.0 μm). In contrast, measured passive tension (sarcomere length 3.0 μm) in both soleus and EDL muscles was increased 53 ± 11% and 62 ± 4%, respectively. This unexpected increase was due to changes in titin, not to alterations in the extracellular matrix, and is likely caused by co-expression of two titin isoforms in Ttn(Δ219–225) muscles: a larger isoform that represents the Ttn(Δ219–225) N2A titin and a smaller isoform, referred to as N2A2. N2A2 represents a splicing adaption with reduced expression of spring element exons, as determined by titin exon microarray analysis. Maximal tetanic tension was increased in Ttn(Δ219–225) soleus muscle (WT 240 ± 9; Ttn(Δ219–225) 276 ± 17 mN/mm(2)), but was reduced in EDL muscle (WT 315 ± 9; Ttn(Δ219–225) 280 ± 14 mN/mm(2)). The changes in active tension coincided with a switch toward slow fiber types and, unexpectedly, faster kinetics of tension generation and relaxation. Functional overload (FO; ablation) and hindlimb suspension (HS; unloading) experiments were also conducted. Ttn(Δ219–225) mice showed increases in both longitudinal hypertrophy (increased number of sarcomeres in series) and cross-sectional hypertrophy (increased number of sarcomeres in parallel) in response to FO and attenuated cross-sectional atrophy in response to HS. In summary, slow- and fast-twitch muscles in a mouse model devoid of titin’s PEVK exons 219–225 have high passive tension, due in part to alterations elsewhere in splicing of titin’s spring region, increased kinetics of tension generation and relaxation, and altered trophic responses to both functional overload and unloading. This implicates titin’s C-terminal PEVK region in regulating passive and active muscle mechanics and muscle plasticity. Frontiers Media S.A. 2020-05-29 /pmc/articles/PMC7274174/ /pubmed/32547410 http://dx.doi.org/10.3389/fphys.2020.00494 Text en Copyright © 2020 van der Pijl, Hudson, Granzier-Nakajima, Li, Knottnerus, Smith, Chung, Gotthardt, Granzier and Ottenheijm. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Physiology
van der Pijl, Robbert J.
Hudson, Brian
Granzier-Nakajima, Tomotaroh
Li, Frank
Knottnerus, Anne M.
Smith, John
Chung, Charles S.
Gotthardt, Michael
Granzier, Henk L.
Ottenheijm, Coen A. C.
Deleting Titin’s C-Terminal PEVK Exons Increases Passive Stiffness, Alters Splicing, and Induces Cross-Sectional and Longitudinal Hypertrophy in Skeletal Muscle
title Deleting Titin’s C-Terminal PEVK Exons Increases Passive Stiffness, Alters Splicing, and Induces Cross-Sectional and Longitudinal Hypertrophy in Skeletal Muscle
title_full Deleting Titin’s C-Terminal PEVK Exons Increases Passive Stiffness, Alters Splicing, and Induces Cross-Sectional and Longitudinal Hypertrophy in Skeletal Muscle
title_fullStr Deleting Titin’s C-Terminal PEVK Exons Increases Passive Stiffness, Alters Splicing, and Induces Cross-Sectional and Longitudinal Hypertrophy in Skeletal Muscle
title_full_unstemmed Deleting Titin’s C-Terminal PEVK Exons Increases Passive Stiffness, Alters Splicing, and Induces Cross-Sectional and Longitudinal Hypertrophy in Skeletal Muscle
title_short Deleting Titin’s C-Terminal PEVK Exons Increases Passive Stiffness, Alters Splicing, and Induces Cross-Sectional and Longitudinal Hypertrophy in Skeletal Muscle
title_sort deleting titin’s c-terminal pevk exons increases passive stiffness, alters splicing, and induces cross-sectional and longitudinal hypertrophy in skeletal muscle
topic Physiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7274174/
https://www.ncbi.nlm.nih.gov/pubmed/32547410
http://dx.doi.org/10.3389/fphys.2020.00494
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