Meis1 regulates postnatal cardiomyocyte cell cycle arrest

Ahmed I. Mahmoud; Fatih Kocabas; Shalini A. Muralidhar; Wataru Kimura; Ahmed S. Koura; Suwannee Thet; Enzo R. Porrello; Hesham A. Sadek

doi:10.1038/nature12054

Meis1 regulates postnatal cardiomyocyte cell cycle arrest

Ahmed I. Mahmoud, Fatih Kocabas, Shalini A. Muralidhar, Wataru Kimura, Ahmed S. Koura, Suwannee Thet, Enzo R. Porrello, Hesham A. Sadek

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Abstract

The neonatal mammalian heart is capable of substantial regeneration following injury through cardiomyocyte proliferation. However, this regenerative capacity is lost by postnatal day 7 and the mechanisms of cardiomyocyte cell cycle arrest remain unclear. The homeodomain transcription factor Meis1 is required for normal cardiac development but its role in cardiomyocytes is unknown. Here we identify Meis1 as a critical regulator of the cardiomyocyte cell cycle. Meis1 deletion in mouse cardiomyocytes was sufficient for extension of the postnatal proliferative window of cardiomyocytes, and for re-activation of cardiomyocyte mitosis in the adult heart with no deleterious effect on cardiac function. In contrast, overexpression of Meis1 in cardiomyocytes decreased neonatal myocyte proliferation and inhibited neonatal heart regeneration. Finally, we show that Meis1 is required for transcriptional activation of the synergistic CDK inhibitors p15, p16 and p21. These results identify Meis1 as a critical transcriptional regulator of cardiomyocyte proliferation and a potential therapeutic target for heart regeneration.

Original language	English (US)
Pages (from-to)	249-253
Number of pages	5
Journal	Nature
Volume	497
Issue number	7448
DOIs	https://doi.org/10.1038/nature12054
State	Published - 2013

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title = "Meis1 regulates postnatal cardiomyocyte cell cycle arrest",

abstract = "The neonatal mammalian heart is capable of substantial regeneration following injury through cardiomyocyte proliferation. However, this regenerative capacity is lost by postnatal day 7 and the mechanisms of cardiomyocyte cell cycle arrest remain unclear. The homeodomain transcription factor Meis1 is required for normal cardiac development but its role in cardiomyocytes is unknown. Here we identify Meis1 as a critical regulator of the cardiomyocyte cell cycle. Meis1 deletion in mouse cardiomyocytes was sufficient for extension of the postnatal proliferative window of cardiomyocytes, and for re-activation of cardiomyocyte mitosis in the adult heart with no deleterious effect on cardiac function. In contrast, overexpression of Meis1 in cardiomyocytes decreased neonatal myocyte proliferation and inhibited neonatal heart regeneration. Finally, we show that Meis1 is required for transcriptional activation of the synergistic CDK inhibitors p15, p16 and p21. These results identify Meis1 as a critical transcriptional regulator of cardiomyocyte proliferation and a potential therapeutic target for heart regeneration.",

author = "Mahmoud, {Ahmed I.} and Fatih Kocabas and Muralidhar, {Shalini A.} and Wataru Kimura and Koura, {Ahmed S.} and Suwannee Thet and Porrello, {Enzo R.} and Sadek, {Hesham A.}",

note = "Funding Information: Acknowledgements WethankJ.Sheltonfor help withhistology,J. Cabrerafor helpwith figures,N.Copeland andN.Jenkinsfor providingtheMeis1 KOmice,S. Das for statistics consultation, K. Luby-Phelps for help with microscopy, A. Bugde for confocal assistance, D. Farrar for discussions, H. Nguyen for help with echocardiography, as well asK.Sheth,A. MercadelandZ.Sadekfor technicalassistance.Thisworkissupportedby grants from the American Heart Association (Grant in Aid) (H.A.S.), the Gilead Research Scholars Program in Cardiovascular Disease (H.A.S.), the Foundation for Heart Failure Research, NY, and the National Institutes of Health (1R01HL115275-01) (H.A.S.).",

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doi = "10.1038/nature12054",

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T1 - Meis1 regulates postnatal cardiomyocyte cell cycle arrest

AU - Mahmoud, Ahmed I.

AU - Kocabas, Fatih

AU - Muralidhar, Shalini A.

AU - Kimura, Wataru

AU - Koura, Ahmed S.

AU - Thet, Suwannee

AU - Porrello, Enzo R.

AU - Sadek, Hesham A.

N1 - Funding Information: Acknowledgements WethankJ.Sheltonfor help withhistology,J. Cabrerafor helpwith figures,N.Copeland andN.Jenkinsfor providingtheMeis1 KOmice,S. Das for statistics consultation, K. Luby-Phelps for help with microscopy, A. Bugde for confocal assistance, D. Farrar for discussions, H. Nguyen for help with echocardiography, as well asK.Sheth,A. MercadelandZ.Sadekfor technicalassistance.Thisworkissupportedby grants from the American Heart Association (Grant in Aid) (H.A.S.), the Gilead Research Scholars Program in Cardiovascular Disease (H.A.S.), the Foundation for Heart Failure Research, NY, and the National Institutes of Health (1R01HL115275-01) (H.A.S.).

PY - 2013

Y1 - 2013

N2 - The neonatal mammalian heart is capable of substantial regeneration following injury through cardiomyocyte proliferation. However, this regenerative capacity is lost by postnatal day 7 and the mechanisms of cardiomyocyte cell cycle arrest remain unclear. The homeodomain transcription factor Meis1 is required for normal cardiac development but its role in cardiomyocytes is unknown. Here we identify Meis1 as a critical regulator of the cardiomyocyte cell cycle. Meis1 deletion in mouse cardiomyocytes was sufficient for extension of the postnatal proliferative window of cardiomyocytes, and for re-activation of cardiomyocyte mitosis in the adult heart with no deleterious effect on cardiac function. In contrast, overexpression of Meis1 in cardiomyocytes decreased neonatal myocyte proliferation and inhibited neonatal heart regeneration. Finally, we show that Meis1 is required for transcriptional activation of the synergistic CDK inhibitors p15, p16 and p21. These results identify Meis1 as a critical transcriptional regulator of cardiomyocyte proliferation and a potential therapeutic target for heart regeneration.

AB - The neonatal mammalian heart is capable of substantial regeneration following injury through cardiomyocyte proliferation. However, this regenerative capacity is lost by postnatal day 7 and the mechanisms of cardiomyocyte cell cycle arrest remain unclear. The homeodomain transcription factor Meis1 is required for normal cardiac development but its role in cardiomyocytes is unknown. Here we identify Meis1 as a critical regulator of the cardiomyocyte cell cycle. Meis1 deletion in mouse cardiomyocytes was sufficient for extension of the postnatal proliferative window of cardiomyocytes, and for re-activation of cardiomyocyte mitosis in the adult heart with no deleterious effect on cardiac function. In contrast, overexpression of Meis1 in cardiomyocytes decreased neonatal myocyte proliferation and inhibited neonatal heart regeneration. Finally, we show that Meis1 is required for transcriptional activation of the synergistic CDK inhibitors p15, p16 and p21. These results identify Meis1 as a critical transcriptional regulator of cardiomyocyte proliferation and a potential therapeutic target for heart regeneration.

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Meis1 regulates postnatal cardiomyocyte cell cycle arrest

Abstract

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