Col1a2-Deleted Mice Have Defective Type I Collagen and Secondary Reactive Cardiac Fibrosis with Altered Hypertrophic Dynamics

Rationale: The adult cardiac extracellular matrix (ECM) is largely comprised of type I collagen. In addition to serving as the primary structural support component of the cardiac ECM, type I collagen also provides an organizational platform for other ECM proteins, matricellular proteins, and signali...

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Autores principales: Bowers, Stephanie L. K., Meng, Qinghang, Kuwabara, Yasuhide, Huo, Jiuzhou, Minerath, Rachel, York, Allen J., Sargent, Michelle A., Prasad, Vikram, Saviola, Anthony J., Galindo, David Ceja, Hansen, Kirk C., Vagnozzi, Ronald J., Yutzey, Katherine E., Molkentin, Jeffery D.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10486458/
https://www.ncbi.nlm.nih.gov/pubmed/37681905
http://dx.doi.org/10.3390/cells12172174
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author Bowers, Stephanie L. K.
Meng, Qinghang
Kuwabara, Yasuhide
Huo, Jiuzhou
Minerath, Rachel
York, Allen J.
Sargent, Michelle A.
Prasad, Vikram
Saviola, Anthony J.
Galindo, David Ceja
Hansen, Kirk C.
Vagnozzi, Ronald J.
Yutzey, Katherine E.
Molkentin, Jeffery D.
author_facet Bowers, Stephanie L. K.
Meng, Qinghang
Kuwabara, Yasuhide
Huo, Jiuzhou
Minerath, Rachel
York, Allen J.
Sargent, Michelle A.
Prasad, Vikram
Saviola, Anthony J.
Galindo, David Ceja
Hansen, Kirk C.
Vagnozzi, Ronald J.
Yutzey, Katherine E.
Molkentin, Jeffery D.
author_sort Bowers, Stephanie L. K.
collection PubMed
description Rationale: The adult cardiac extracellular matrix (ECM) is largely comprised of type I collagen. In addition to serving as the primary structural support component of the cardiac ECM, type I collagen also provides an organizational platform for other ECM proteins, matricellular proteins, and signaling components that impact cellular stress sensing in vivo. Objective: Here we investigated how the content and integrity of type I collagen affect cardiac structure function and response to injury. Methods and Results: We generated and characterized Col1a2(−/−) mice using standard gene targeting. Col1a2(−/−) mice were viable, although by young adulthood their hearts showed alterations in ECM mechanical properties, as well as an unanticipated activation of cardiac fibroblasts and induction of a progressive fibrotic response. This included augmented TGFβ activity, increases in fibroblast number, and progressive cardiac hypertrophy, with reduced functional performance by 9 months of age. Col1a2-loxP-targeted mice were also generated and crossed with the tamoxifen-inducible Postn-MerCreMer mice to delete the Col1a2 gene in myofibroblasts with pressure overload injury. Interestingly, while germline Col1a2(−/−) mice showed gradual pathologic hypertrophy and fibrosis with aging, the acute deletion of Col1a2 from activated adult myofibroblasts showed a loss of total collagen deposition with acute cardiac injury and an acute reduction in pressure overload-induce cardiac hypertrophy. However, this reduction in hypertrophy due to myofibroblast-specific Col1a2 deletion was lost after 2 and 6 weeks of pressure overload, as fibrotic deposition accumulated. Conclusions: Defective type I collagen in the heart alters the structural integrity of the ECM and leads to cardiomyopathy in adulthood, with fibroblast expansion, activation, and alternate fibrotic ECM deposition. However, acute inhibition of type I collagen production can have an anti-fibrotic and anti-hypertrophic effect.
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spelling pubmed-104864582023-09-09 Col1a2-Deleted Mice Have Defective Type I Collagen and Secondary Reactive Cardiac Fibrosis with Altered Hypertrophic Dynamics Bowers, Stephanie L. K. Meng, Qinghang Kuwabara, Yasuhide Huo, Jiuzhou Minerath, Rachel York, Allen J. Sargent, Michelle A. Prasad, Vikram Saviola, Anthony J. Galindo, David Ceja Hansen, Kirk C. Vagnozzi, Ronald J. Yutzey, Katherine E. Molkentin, Jeffery D. Cells Article Rationale: The adult cardiac extracellular matrix (ECM) is largely comprised of type I collagen. In addition to serving as the primary structural support component of the cardiac ECM, type I collagen also provides an organizational platform for other ECM proteins, matricellular proteins, and signaling components that impact cellular stress sensing in vivo. Objective: Here we investigated how the content and integrity of type I collagen affect cardiac structure function and response to injury. Methods and Results: We generated and characterized Col1a2(−/−) mice using standard gene targeting. Col1a2(−/−) mice were viable, although by young adulthood their hearts showed alterations in ECM mechanical properties, as well as an unanticipated activation of cardiac fibroblasts and induction of a progressive fibrotic response. This included augmented TGFβ activity, increases in fibroblast number, and progressive cardiac hypertrophy, with reduced functional performance by 9 months of age. Col1a2-loxP-targeted mice were also generated and crossed with the tamoxifen-inducible Postn-MerCreMer mice to delete the Col1a2 gene in myofibroblasts with pressure overload injury. Interestingly, while germline Col1a2(−/−) mice showed gradual pathologic hypertrophy and fibrosis with aging, the acute deletion of Col1a2 from activated adult myofibroblasts showed a loss of total collagen deposition with acute cardiac injury and an acute reduction in pressure overload-induce cardiac hypertrophy. However, this reduction in hypertrophy due to myofibroblast-specific Col1a2 deletion was lost after 2 and 6 weeks of pressure overload, as fibrotic deposition accumulated. Conclusions: Defective type I collagen in the heart alters the structural integrity of the ECM and leads to cardiomyopathy in adulthood, with fibroblast expansion, activation, and alternate fibrotic ECM deposition. However, acute inhibition of type I collagen production can have an anti-fibrotic and anti-hypertrophic effect. MDPI 2023-08-30 /pmc/articles/PMC10486458/ /pubmed/37681905 http://dx.doi.org/10.3390/cells12172174 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Bowers, Stephanie L. K.
Meng, Qinghang
Kuwabara, Yasuhide
Huo, Jiuzhou
Minerath, Rachel
York, Allen J.
Sargent, Michelle A.
Prasad, Vikram
Saviola, Anthony J.
Galindo, David Ceja
Hansen, Kirk C.
Vagnozzi, Ronald J.
Yutzey, Katherine E.
Molkentin, Jeffery D.
Col1a2-Deleted Mice Have Defective Type I Collagen and Secondary Reactive Cardiac Fibrosis with Altered Hypertrophic Dynamics
title Col1a2-Deleted Mice Have Defective Type I Collagen and Secondary Reactive Cardiac Fibrosis with Altered Hypertrophic Dynamics
title_full Col1a2-Deleted Mice Have Defective Type I Collagen and Secondary Reactive Cardiac Fibrosis with Altered Hypertrophic Dynamics
title_fullStr Col1a2-Deleted Mice Have Defective Type I Collagen and Secondary Reactive Cardiac Fibrosis with Altered Hypertrophic Dynamics
title_full_unstemmed Col1a2-Deleted Mice Have Defective Type I Collagen and Secondary Reactive Cardiac Fibrosis with Altered Hypertrophic Dynamics
title_short Col1a2-Deleted Mice Have Defective Type I Collagen and Secondary Reactive Cardiac Fibrosis with Altered Hypertrophic Dynamics
title_sort col1a2-deleted mice have defective type i collagen and secondary reactive cardiac fibrosis with altered hypertrophic dynamics
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10486458/
https://www.ncbi.nlm.nih.gov/pubmed/37681905
http://dx.doi.org/10.3390/cells12172174
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