Inhibition of plasminogen activators or matrix metalloproteinases prevents cardiac rupture but impairs therapeutic angiogenesis and causes cardiac failure

S. Heymans; A. Luttun; D. Nuyens; G. Theilmeier; E. Creemers; L. Moons; G. D. Dyspersin; J. P.M. Cleutjens; M. Shipley; A. Angellilo; M. Levi; O. Nübe; A. Baker; E. Keshet; F. Lupu; J. M. Herbert; J. F.M. Smits; S. D. Shapiro; M. Baes; M. Borgers; D. Collen; M. J.A.P. Daemen; P. Carmeliet

doi:10.1038/13459

Inhibition of plasminogen activators or matrix metalloproteinases prevents cardiac rupture but impairs therapeutic angiogenesis and causes cardiac failure

S. Heymans^*, A. Luttun, D. Nuyens, G. Theilmeier, E. Creemers, L. Moons, G. D. Dyspersin, J. P.M. Cleutjens, M. Shipley, A. Angellilo, M. Levi, O. Nübe, A. Baker, E. Keshet, F. Lupu, J. M. Herbert, J. F.M. Smits, S. D. Shapiro, M. Baes, M. BorgersD. Collen, M. J.A.P. Daemen, P. Carmeliet

^*Corresponding author for this work

Institute for Medical Research Israel-Canada (IMRIC)

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Abstract

Cardiac rupture is a fatal complication of acute myocardial infarction lacking treatment. Here, acute myocardial infarction resulted in rupture in wild-type mice and in mice lacking tissue-type plasminogen activator, urokinase receptor, matrix metalloproteinase stromelysin-1 or metalloelastase. Instead, deficiency of urokinase-type plasminogen activator u-PA(-/-) completely protected against rupture, whereas lack of gelatinase-B partially protected against rupture. However, u-PA(-/-) mice showed impaired scar formation and infarct revascularization, even after treatment with vascular endothelial growth factor, and died of cardiac failure due to depressed contractility, arrhythmias and ischemia. Temporary administration of PA inhibitor-1 or the matrix metalloproteinase-inhibitor TIMP-1 completely protected wild-type mice against rupture but did not abort infarct healing, thus constituting a new approach to prevent cardiac rupture after acute myocardial infarction.

Original language	English
Pages (from-to)	1135-1142
Number of pages	8
Journal	Nature Medicine
Volume	5
Issue number	10
DOIs	https://doi.org/10.1038/13459
State	Published - Oct 1999

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Heymans, S., Luttun, A., Nuyens, D., Theilmeier, G., Creemers, E., Moons, L., Dyspersin, G. D., Cleutjens, J. P. M., Shipley, M., Angellilo, A., Levi, M., Nübe, O., Baker, A., Keshet, E., Lupu, F., Herbert, J. M., Smits, J. F. M., Shapiro, S. D., Baes, M., ... Carmeliet, P. (1999). Inhibition of plasminogen activators or matrix metalloproteinases prevents cardiac rupture but impairs therapeutic angiogenesis and causes cardiac failure. Nature Medicine, 5(10), 1135-1142. https://doi.org/10.1038/13459

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title = "Inhibition of plasminogen activators or matrix metalloproteinases prevents cardiac rupture but impairs therapeutic angiogenesis and causes cardiac failure",

abstract = "Cardiac rupture is a fatal complication of acute myocardial infarction lacking treatment. Here, acute myocardial infarction resulted in rupture in wild-type mice and in mice lacking tissue-type plasminogen activator, urokinase receptor, matrix metalloproteinase stromelysin-1 or metalloelastase. Instead, deficiency of urokinase-type plasminogen activator u-PA(-/-) completely protected against rupture, whereas lack of gelatinase-B partially protected against rupture. However, u-PA(-/-) mice showed impaired scar formation and infarct revascularization, even after treatment with vascular endothelial growth factor, and died of cardiac failure due to depressed contractility, arrhythmias and ischemia. Temporary administration of PA inhibitor-1 or the matrix metalloproteinase-inhibitor TIMP-1 completely protected wild-type mice against rupture but did not abort infarct healing, thus constituting a new approach to prevent cardiac rupture after acute myocardial infarction.",

author = "S. Heymans and A. Luttun and D. Nuyens and G. Theilmeier and E. Creemers and L. Moons and Dyspersin, {G. D.} and Cleutjens, {J. P.M.} and M. Shipley and A. Angellilo and M. Levi and O. N{\"u}be and A. Baker and E. Keshet and F. Lupu and Herbert, {J. M.} and Smits, {J. F.M.} and Shapiro, {S. D.} and M. Baes and M. Borgers and D. Collen and Daemen, {M. J.A.P.} and P. Carmeliet",

year = "1999",

month = oct,

doi = "10.1038/13459",

language = "אנגלית",

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Heymans, S, Luttun, A, Nuyens, D, Theilmeier, G, Creemers, E, Moons, L, Dyspersin, GD, Cleutjens, JPM, Shipley, M, Angellilo, A, Levi, M, Nübe, O, Baker, A, Keshet, E, Lupu, F, Herbert, JM, Smits, JFM, Shapiro, SD, Baes, M, Borgers, M, Collen, D, Daemen, MJAP & Carmeliet, P 1999, 'Inhibition of plasminogen activators or matrix metalloproteinases prevents cardiac rupture but impairs therapeutic angiogenesis and causes cardiac failure', Nature Medicine, vol. 5, no. 10, pp. 1135-1142. https://doi.org/10.1038/13459

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T1 - Inhibition of plasminogen activators or matrix metalloproteinases prevents cardiac rupture but impairs therapeutic angiogenesis and causes cardiac failure

AU - Heymans, S.

AU - Luttun, A.

AU - Nuyens, D.

AU - Theilmeier, G.

AU - Creemers, E.

AU - Moons, L.

AU - Dyspersin, G. D.

AU - Cleutjens, J. P.M.

AU - Shipley, M.

AU - Angellilo, A.

AU - Levi, M.

AU - Nübe, O.

AU - Baker, A.

AU - Keshet, E.

AU - Lupu, F.

AU - Herbert, J. M.

AU - Smits, J. F.M.

AU - Shapiro, S. D.

AU - Baes, M.

AU - Borgers, M.

AU - Collen, D.

AU - Daemen, M. J.A.P.

AU - Carmeliet, P.

PY - 1999/10

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AB - Cardiac rupture is a fatal complication of acute myocardial infarction lacking treatment. Here, acute myocardial infarction resulted in rupture in wild-type mice and in mice lacking tissue-type plasminogen activator, urokinase receptor, matrix metalloproteinase stromelysin-1 or metalloelastase. Instead, deficiency of urokinase-type plasminogen activator u-PA(-/-) completely protected against rupture, whereas lack of gelatinase-B partially protected against rupture. However, u-PA(-/-) mice showed impaired scar formation and infarct revascularization, even after treatment with vascular endothelial growth factor, and died of cardiac failure due to depressed contractility, arrhythmias and ischemia. Temporary administration of PA inhibitor-1 or the matrix metalloproteinase-inhibitor TIMP-1 completely protected wild-type mice against rupture but did not abort infarct healing, thus constituting a new approach to prevent cardiac rupture after acute myocardial infarction.

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Inhibition of plasminogen activators or matrix metalloproteinases prevents cardiac rupture but impairs therapeutic angiogenesis and causes cardiac failure

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