Thymosin β4 activates integrin-linked kinase and promotes cardiac cell migration, survival and cardiac repair

Ildiko Bock-Marquette; Ankur Saxena; Michael D. White; J. Michael DiMaio; Deepak Srivastava

doi:10.1038/nature03000

Thymosin β4 activates integrin-linked kinase and promotes cardiac cell migration, survival and cardiac repair

Ildiko Bock-Marquette, Ankur Saxena, Michael D. White, J. Michael DiMaio, Deepak Srivastava

Cardio Thoracic Surgery

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

585 Scopus citations

Abstract

Heart disease is a leading cause of death in newborn children and in adults. Efforts to promote cardiac repair through the use of stem cells hold promise but typically involve isolation and introduction of progenitor cells. Here, we show that the G-actin sequestering peptide thymosin β4 promotes myocardial and endothelial cell migration in the embryonic heart and retains this property in postnatal cardiomyocytes. Survival of embryonic and postnatal cardiomyocytes in culture was also enhanced by thymosin β4. We found that thymosin β4 formed a functional complex with PINCH and integrin-linked kinase (ILK), resulting in activation of the survival kinase Akt (also known as protein kinase B). After coronary artery ligation in mice, thymosin β4 treatment resulted in upregulation of ILK and Akt activity in the heart, enhanced early myocyte survival and improved cardiac function. These findings suggest that thymosin β4 promotes cardiomyocyte migration, survival and repair and the pathway it regulates may be a new therapeutic target in the setting of acute myocardial damage.

Original language	English (US)
Pages (from-to)	466-472
Number of pages	7
Journal	Nature
Volume	432
Issue number	7016
DOIs	https://doi.org/10.1038/nature03000
State	Published - Nov 25 2004

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title = "Thymosin β4 activates integrin-linked kinase and promotes cardiac cell migration, survival and cardiac repair",

abstract = "Heart disease is a leading cause of death in newborn children and in adults. Efforts to promote cardiac repair through the use of stem cells hold promise but typically involve isolation and introduction of progenitor cells. Here, we show that the G-actin sequestering peptide thymosin β4 promotes myocardial and endothelial cell migration in the embryonic heart and retains this property in postnatal cardiomyocytes. Survival of embryonic and postnatal cardiomyocytes in culture was also enhanced by thymosin β4. We found that thymosin β4 formed a functional complex with PINCH and integrin-linked kinase (ILK), resulting in activation of the survival kinase Akt (also known as protein kinase B). After coronary artery ligation in mice, thymosin β4 treatment resulted in upregulation of ILK and Akt activity in the heart, enhanced early myocyte survival and improved cardiac function. These findings suggest that thymosin β4 promotes cardiomyocyte migration, survival and repair and the pathway it regulates may be a new therapeutic target in the setting of acute myocardial damage.",

author = "Ildiko Bock-Marquette and Ankur Saxena and White, {Michael D.} and DiMaio, {J. Michael} and Deepak Srivastava",

note = "Funding Information: Acknowledgements The authors wish to thank A. L. Goldstein for his advice and RegeneRx Biopharmaceuticals Inc. for providing the synthetic thymosin b4 protein; J. Richardson and the histopathology core for histological support; G. A. Adams for technical asssistance; E. N. Olson and members of the Srivastava laboratory for discussions and critical review; and S. Johnson and J. E. Marquette for graphical help and suggestions. D.S. was supported by grants from the NHLBI/ NIH, March of Dimes Birth Defects Foundation, American Heart Association and Donald W. Reynolds Clinical Cardiovascular Research Center.",

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AU - Srivastava, Deepak

N1 - Funding Information: Acknowledgements The authors wish to thank A. L. Goldstein for his advice and RegeneRx Biopharmaceuticals Inc. for providing the synthetic thymosin b4 protein; J. Richardson and the histopathology core for histological support; G. A. Adams for technical asssistance; E. N. Olson and members of the Srivastava laboratory for discussions and critical review; and S. Johnson and J. E. Marquette for graphical help and suggestions. D.S. was supported by grants from the NHLBI/ NIH, March of Dimes Birth Defects Foundation, American Heart Association and Donald W. Reynolds Clinical Cardiovascular Research Center.

PY - 2004/11/25

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N2 - Heart disease is a leading cause of death in newborn children and in adults. Efforts to promote cardiac repair through the use of stem cells hold promise but typically involve isolation and introduction of progenitor cells. Here, we show that the G-actin sequestering peptide thymosin β4 promotes myocardial and endothelial cell migration in the embryonic heart and retains this property in postnatal cardiomyocytes. Survival of embryonic and postnatal cardiomyocytes in culture was also enhanced by thymosin β4. We found that thymosin β4 formed a functional complex with PINCH and integrin-linked kinase (ILK), resulting in activation of the survival kinase Akt (also known as protein kinase B). After coronary artery ligation in mice, thymosin β4 treatment resulted in upregulation of ILK and Akt activity in the heart, enhanced early myocyte survival and improved cardiac function. These findings suggest that thymosin β4 promotes cardiomyocyte migration, survival and repair and the pathway it regulates may be a new therapeutic target in the setting of acute myocardial damage.

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Thymosin β4 activates integrin-linked kinase and promotes cardiac cell migration, survival and cardiac repair

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