Deletion of Fstl1 (Follistatin-Like 1) From the Endocardial/Endothelial Lineage Causes Mitral Valve Disease

Stuti Prakash; Luis J. J. Borreguero; Marc Sylva; Lorena Flores Ruiz; Fereshte Rezai; Quinn D. Gunst; José-Luis de la Pompa; Jan M. Ruijter; Maurice J. B. van den Hoff

doi:https://doi.org/10.1161/ATVBAHA.117.309089

Deletion of Fstl1 (Follistatin-Like 1) From the Endocardial/Endothelial Lineage Causes Mitral Valve Disease

Stuti Prakash, Luis J. J. Borreguero, Marc Sylva, Lorena Flores Ruiz, Fereshte Rezai, Quinn D. Gunst, José-Luis de la Pompa, Jan M. Ruijter, Maurice J. B. van den Hoff

Research output: Contribution to journal › Article › Academic › peer-review

23 Citations (Scopus)

Abstract

Objective-Fstl1 (Follistatin-like 1) is a secreted protein that is expressed in the atrioventricular valves throughout embryonic development, postnatal maturation, and adulthood. In this study, we investigated the loss of Fstl1 in the endocardium/endothelium and their derived cells. Approach and Results-We conditionally ablated Fstl1 from the endocardial lineage using a transgenic Tie2-Cre mouse model. These mice showed a sustained Bmp and Tgf beta signaling after birth. This resulted in ongoing proliferation and endocardial-to-mesenchymal transition and ultimately in deformed nonfunctional mitral valves and a hypertrophic dilated heart. Echocardiographic and electrocardiographic analyses revealed that loss of Fstl1 leads to mitral regurgitation and left ventricular diastolic dysfunction. Cardiac function gradually deteriorated resulting in heart failure with preserved ejection fraction and death of the mice between 2 and 4 weeks after birth. Conclusions-We report on a mouse model in which deletion of Fstl1 from the endocardial/endothelial lineage results in deformed mitral valves, which cause regurgitation, heart failure, and early cardiac death. The findings provide a potential molecular target for the clinical research into myxomatous mitral valve disease. Visual Overview-An online visual overview is available for this article

Original language	English
Pages (from-to)	E116-E130
Journal	Arteriosclerosis, Thrombosis, and Vascular Biology
Volume	37
Issue number	9
Early online date	2017
DOIs	https://doi.org/10.1161/ATVBAHA.117.309089
Publication status	Published - 2017

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https://doi.org/10.1161/ATVBAHA.117.309089

Cite this

Prakash, S., Borreguero, L. J. J., Sylva, M., Flores Ruiz, L., Rezai, F., Gunst, Q. D., de la Pompa, J.-L., Ruijter, J. M., & van den Hoff, M. J. B. (2017). Deletion of Fstl1 (Follistatin-Like 1) From the Endocardial/Endothelial Lineage Causes Mitral Valve Disease. Arteriosclerosis, Thrombosis, and Vascular Biology, 37(9), E116-E130. https://doi.org/10.1161/ATVBAHA.117.309089

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title = "Deletion of Fstl1 (Follistatin-Like 1) From the Endocardial/Endothelial Lineage Causes Mitral Valve Disease",

abstract = "Objective-Fstl1 (Follistatin-like 1) is a secreted protein that is expressed in the atrioventricular valves throughout embryonic development, postnatal maturation, and adulthood. In this study, we investigated the loss of Fstl1 in the endocardium/endothelium and their derived cells. Approach and Results-We conditionally ablated Fstl1 from the endocardial lineage using a transgenic Tie2-Cre mouse model. These mice showed a sustained Bmp and Tgf beta signaling after birth. This resulted in ongoing proliferation and endocardial-to-mesenchymal transition and ultimately in deformed nonfunctional mitral valves and a hypertrophic dilated heart. Echocardiographic and electrocardiographic analyses revealed that loss of Fstl1 leads to mitral regurgitation and left ventricular diastolic dysfunction. Cardiac function gradually deteriorated resulting in heart failure with preserved ejection fraction and death of the mice between 2 and 4 weeks after birth. Conclusions-We report on a mouse model in which deletion of Fstl1 from the endocardial/endothelial lineage results in deformed mitral valves, which cause regurgitation, heart failure, and early cardiac death. The findings provide a potential molecular target for the clinical research into myxomatous mitral valve disease. Visual Overview-An online visual overview is available for this article",

author = "Stuti Prakash and Borreguero, {Luis J. J.} and Marc Sylva and {Flores Ruiz}, Lorena and Fereshte Rezai and Gunst, {Quinn D.} and {de la Pompa}, Jos{\'e}-Luis and Ruijter, {Jan M.} and {van den Hoff}, {Maurice J. B.}",

year = "2017",

doi = "https://doi.org/10.1161/ATVBAHA.117.309089",

language = "English",

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pages = "E116--E130",

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T1 - Deletion of Fstl1 (Follistatin-Like 1) From the Endocardial/Endothelial Lineage Causes Mitral Valve Disease

AU - Prakash, Stuti

AU - Borreguero, Luis J. J.

AU - Sylva, Marc

AU - Flores Ruiz, Lorena

AU - Rezai, Fereshte

AU - Gunst, Quinn D.

AU - de la Pompa, José-Luis

AU - Ruijter, Jan M.

AU - van den Hoff, Maurice J. B.

PY - 2017

Y1 - 2017

N2 - Objective-Fstl1 (Follistatin-like 1) is a secreted protein that is expressed in the atrioventricular valves throughout embryonic development, postnatal maturation, and adulthood. In this study, we investigated the loss of Fstl1 in the endocardium/endothelium and their derived cells. Approach and Results-We conditionally ablated Fstl1 from the endocardial lineage using a transgenic Tie2-Cre mouse model. These mice showed a sustained Bmp and Tgf beta signaling after birth. This resulted in ongoing proliferation and endocardial-to-mesenchymal transition and ultimately in deformed nonfunctional mitral valves and a hypertrophic dilated heart. Echocardiographic and electrocardiographic analyses revealed that loss of Fstl1 leads to mitral regurgitation and left ventricular diastolic dysfunction. Cardiac function gradually deteriorated resulting in heart failure with preserved ejection fraction and death of the mice between 2 and 4 weeks after birth. Conclusions-We report on a mouse model in which deletion of Fstl1 from the endocardial/endothelial lineage results in deformed mitral valves, which cause regurgitation, heart failure, and early cardiac death. The findings provide a potential molecular target for the clinical research into myxomatous mitral valve disease. Visual Overview-An online visual overview is available for this article

AB - Objective-Fstl1 (Follistatin-like 1) is a secreted protein that is expressed in the atrioventricular valves throughout embryonic development, postnatal maturation, and adulthood. In this study, we investigated the loss of Fstl1 in the endocardium/endothelium and their derived cells. Approach and Results-We conditionally ablated Fstl1 from the endocardial lineage using a transgenic Tie2-Cre mouse model. These mice showed a sustained Bmp and Tgf beta signaling after birth. This resulted in ongoing proliferation and endocardial-to-mesenchymal transition and ultimately in deformed nonfunctional mitral valves and a hypertrophic dilated heart. Echocardiographic and electrocardiographic analyses revealed that loss of Fstl1 leads to mitral regurgitation and left ventricular diastolic dysfunction. Cardiac function gradually deteriorated resulting in heart failure with preserved ejection fraction and death of the mice between 2 and 4 weeks after birth. Conclusions-We report on a mouse model in which deletion of Fstl1 from the endocardial/endothelial lineage results in deformed mitral valves, which cause regurgitation, heart failure, and early cardiac death. The findings provide a potential molecular target for the clinical research into myxomatous mitral valve disease. Visual Overview-An online visual overview is available for this article

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DO - https://doi.org/10.1161/ATVBAHA.117.309089

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