Insulin receptor substrate signaling suppresses neonatal autophagy in the heart

Christian Riehle; Adam R. Wende; Sandra Sena; Karla M. Pires; Renata O. Pereira; Yi Zhu; Heiko Bugger; Deborah Frank; Jack Bevins; Dong Chen; Cynthia N. Perry; Xiaocheng C. Dong; Steven Valdez; Monika Rech; Xiaoming Sheng; Bart C. Weimer; Roberta A. Gottlieb; Morris F. White; E. D. Abel

doi:10.1172/JCI71171

Insulin receptor substrate signaling suppresses neonatal autophagy in the heart

Christian Riehle, Adam R. Wende, Sandra Sena, Karla M. Pires, Renata O. Pereira, Yi Zhu, Heiko Bugger, Deborah Frank, Jack Bevins, Dong Chen, Cynthia N. Perry, Xiaocheng C. Dong, Steven Valdez, Monika Rech, Xiaoming Sheng, Bart C. Weimer, Roberta A. Gottlieb, Morris F. White, E. D. Abel

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Abstract

The induction of autophagy in the mammalian heart during the perinatal period is an essential adaptation required to survive early neonatal starvation; however, the mechanisms that mediate autophagy suppression once feeding is established are not known. Insulin signaling in the heart is transduced via insulin and IGF-1 receptors (IGF-1Rs). We disrupted insulin and IGF-1R signaling by generating mice with combined cardiomyocyte- specific deletion of Irs1 and Irs2. Here we show that loss of IRS signaling prevented the physiological suppression of autophagy that normally parallels the postnatal increase in circulating insulin. This resulted in unrestrained autophagy in cardiomyocytes, which contributed to myocyte loss, heart failure, and premature death. This process was ameliorated either by activation ofmTOR with aa supplementation or by genetic suppression of autophagic activation. Loss of IRS1 and IRS2 signaling also increased apoptosis and precipitated mitochondrial dysfunction, which were not reduced when autophagic flux was normalized. Together, these data indicate that in addition to prosurvival signaling, insulin action in early life mediates the physiological postnatal suppression of autophagy, thereby linking nutrient sensing to postnatal cardiac development.

Original language	English (US)
Pages (from-to)	5319-5333
Number of pages	15
Journal	Journal of Clinical Investigation
Volume	123
Issue number	12
DOIs	https://doi.org/10.1172/JCI71171
State	Published - Dec 2 2013

ASJC Scopus subject areas

General Medicine

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Riehle, C., Wende, A. R., Sena, S., Pires, K. M., Pereira, R. O., Zhu, Y., Bugger, H., Frank, D., Bevins, J., Chen, D., Perry, C. N., Dong, X. C., Valdez, S., Rech, M., Sheng, X., Weimer, B. C., Gottlieb, R. A., White, M. F., & Abel, E. D. (2013). Insulin receptor substrate signaling suppresses neonatal autophagy in the heart. Journal of Clinical Investigation, 123(12), 5319-5333. https://doi.org/10.1172/JCI71171

Riehle, C, Wende, AR, Sena, S, Pires, KM, Pereira, RO, Zhu, Y, Bugger, H, Frank, D, Bevins, J, Chen, D, Perry, CN, Dong, XC, Valdez, S, Rech, M, Sheng, X, Weimer, BC, Gottlieb, RA, White, MF & Abel, ED 2013, 'Insulin receptor substrate signaling suppresses neonatal autophagy in the heart', Journal of Clinical Investigation, vol. 123, no. 12, pp. 5319-5333. https://doi.org/10.1172/JCI71171

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title = "Insulin receptor substrate signaling suppresses neonatal autophagy in the heart",

abstract = "The induction of autophagy in the mammalian heart during the perinatal period is an essential adaptation required to survive early neonatal starvation; however, the mechanisms that mediate autophagy suppression once feeding is established are not known. Insulin signaling in the heart is transduced via insulin and IGF-1 receptors (IGF-1Rs). We disrupted insulin and IGF-1R signaling by generating mice with combined cardiomyocyte- specific deletion of Irs1 and Irs2. Here we show that loss of IRS signaling prevented the physiological suppression of autophagy that normally parallels the postnatal increase in circulating insulin. This resulted in unrestrained autophagy in cardiomyocytes, which contributed to myocyte loss, heart failure, and premature death. This process was ameliorated either by activation ofmTOR with aa supplementation or by genetic suppression of autophagic activation. Loss of IRS1 and IRS2 signaling also increased apoptosis and precipitated mitochondrial dysfunction, which were not reduced when autophagic flux was normalized. Together, these data indicate that in addition to prosurvival signaling, insulin action in early life mediates the physiological postnatal suppression of autophagy, thereby linking nutrient sensing to postnatal cardiac development.",

author = "Christian Riehle and Wende, {Adam R.} and Sandra Sena and Pires, {Karla M.} and Pereira, {Renata O.} and Yi Zhu and Heiko Bugger and Deborah Frank and Jack Bevins and Dong Chen and Perry, {Cynthia N.} and Dong, {Xiaocheng C.} and Steven Valdez and Monika Rech and Xiaoming Sheng and Weimer, {Bart C.} and Gottlieb, {Roberta A.} and White, {Morris F.} and Abel, {E. D.}",

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doi = "10.1172/JCI71171",

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AU - Wende, Adam R.

AU - Sena, Sandra

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AU - Pereira, Renata O.

AU - Zhu, Yi

AU - Bugger, Heiko

AU - Frank, Deborah

AU - Bevins, Jack

AU - Chen, Dong

AU - Perry, Cynthia N.

AU - Dong, Xiaocheng C.

AU - Valdez, Steven

AU - Rech, Monika

AU - Sheng, Xiaoming

AU - Weimer, Bart C.

AU - Gottlieb, Roberta A.

AU - White, Morris F.

AU - Abel, E. D.

PY - 2013/12/2

Y1 - 2013/12/2

N2 - The induction of autophagy in the mammalian heart during the perinatal period is an essential adaptation required to survive early neonatal starvation; however, the mechanisms that mediate autophagy suppression once feeding is established are not known. Insulin signaling in the heart is transduced via insulin and IGF-1 receptors (IGF-1Rs). We disrupted insulin and IGF-1R signaling by generating mice with combined cardiomyocyte- specific deletion of Irs1 and Irs2. Here we show that loss of IRS signaling prevented the physiological suppression of autophagy that normally parallels the postnatal increase in circulating insulin. This resulted in unrestrained autophagy in cardiomyocytes, which contributed to myocyte loss, heart failure, and premature death. This process was ameliorated either by activation ofmTOR with aa supplementation or by genetic suppression of autophagic activation. Loss of IRS1 and IRS2 signaling also increased apoptosis and precipitated mitochondrial dysfunction, which were not reduced when autophagic flux was normalized. Together, these data indicate that in addition to prosurvival signaling, insulin action in early life mediates the physiological postnatal suppression of autophagy, thereby linking nutrient sensing to postnatal cardiac development.

AB - The induction of autophagy in the mammalian heart during the perinatal period is an essential adaptation required to survive early neonatal starvation; however, the mechanisms that mediate autophagy suppression once feeding is established are not known. Insulin signaling in the heart is transduced via insulin and IGF-1 receptors (IGF-1Rs). We disrupted insulin and IGF-1R signaling by generating mice with combined cardiomyocyte- specific deletion of Irs1 and Irs2. Here we show that loss of IRS signaling prevented the physiological suppression of autophagy that normally parallels the postnatal increase in circulating insulin. This resulted in unrestrained autophagy in cardiomyocytes, which contributed to myocyte loss, heart failure, and premature death. This process was ameliorated either by activation ofmTOR with aa supplementation or by genetic suppression of autophagic activation. Loss of IRS1 and IRS2 signaling also increased apoptosis and precipitated mitochondrial dysfunction, which were not reduced when autophagic flux was normalized. Together, these data indicate that in addition to prosurvival signaling, insulin action in early life mediates the physiological postnatal suppression of autophagy, thereby linking nutrient sensing to postnatal cardiac development.

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Insulin receptor substrate signaling suppresses neonatal autophagy in the heart

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