Hepatic mTORC1 signaling activates ATF4 as part of its metabolic response to feeding and insulin

Hepatic mTORC1 signaling activates ATF4 as part of its metabolic response to feeding and insulin

Objective: The mechanistic target of rapamycin complex 1 (mTORC1) is dynamically regulated by fasting and feeding cycles in the liver to promote protein and lipid synthesis while suppressing autophagy. However, beyond these functions, the metabolic response of the liver to feeding and insulin signal...

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Main Authors: Vanessa Byles, Yann Cormerais, Krystle Kalafut, Victor Barrera, James E. Hughes Hallett, Shannan Ho Sui, John M. Asara, Christopher M. Adams, Gerta Hoxhaj, Issam Ben-Sahra, Brendan D. Manning
Format: Article
Language:English
Published: Elsevier 2021-11-01
Series:Molecular Metabolism
Subjects:
mTORC1
ATF4
Liver
Feeding
Insulin
Methionine metabolism
Online Access:http://www.sciencedirect.com/science/article/pii/S2212877821001563
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spelling doaj-9bc1252e0f6b4fe8816ee31294ba42c12021-08-16T04:16:32ZengElsevierMolecular Metabolism2212-87782021-11-0153101309Hepatic mTORC1 signaling activates ATF4 as part of its metabolic response to feeding and insulinVanessa Byles0Yann Cormerais1Krystle Kalafut2Victor Barrera3James E. Hughes Hallett4Shannan Ho Sui5John M. Asara6Christopher M. Adams7Gerta Hoxhaj8Issam Ben-Sahra9Brendan D. Manning10Department of Molecular Metabolism, Harvard T.H. Chan School of Public Health, Boston, MA, USADepartment of Molecular Metabolism, Harvard T.H. Chan School of Public Health, Boston, MA, USADepartment of Molecular Metabolism, Harvard T.H. Chan School of Public Health, Boston, MA, USADepartment of Biostatistics, Harvard T.H. Chan School of Public Health, Boston, MA, USADepartment of Molecular Metabolism, Harvard T.H. Chan School of Public Health, Boston, MA, USADepartment of Biostatistics, Harvard T.H. Chan School of Public Health, Boston, MA, USADivision of Signal Transduction, Beth Israel Deaconess Medical Center and Department of Medicine, Harvard Medical School, Boston, MA, USADivision of Endocrinology, Metabolism and Nutrition, Mayo Clinic, Rochester, MN, USADepartment of Molecular Metabolism, Harvard T.H. Chan School of Public Health, Boston, MA, USA; Children's Medical Center Research Institute, University of Texas Southwestern Medical Center, Dallas, TX, USADepartment of Biochemistry and Molecular Genetics, Northwestern University Feinberg School of Medicine and Robert H. Lurie Comprehensive Cancer Center, Northwestern University, Chicago, IL, USADepartment of Molecular Metabolism, Harvard T.H. Chan School of Public Health, Boston, MA, USA; Corresponding author.Objective: The mechanistic target of rapamycin complex 1 (mTORC1) is dynamically regulated by fasting and feeding cycles in the liver to promote protein and lipid synthesis while suppressing autophagy. However, beyond these functions, the metabolic response of the liver to feeding and insulin signaling orchestrated by mTORC1 remains poorly defined. Here, we determine whether ATF4, a stress responsive transcription factor recently found to be independently regulated by mTORC1 signaling in proliferating cells, is responsive to hepatic mTORC1 signaling to alter hepatocyte metabolism. Methods: ATF4 protein levels and expression of canonical gene targets were analyzed in the liver following fasting and physiological feeding in the presence or absence of the mTORC1 inhibitor, rapamycin. Primary hepatocytes from wild-type or liver-specific Atf4 knockout (LAtf4KO) mice were used to characterize the effects of insulin-stimulated mTORC1-ATF4 function on hepatocyte gene expression and metabolism. Both unbiased steady-state metabolomics and stable-isotope tracing methods were employed to define mTORC1 and ATF4-dependent metabolic changes. RNA-sequencing was used to determine global changes in feeding-induced transcripts in the livers of wild-type versus LAtf4KO mice. Results: We demonstrate that ATF4 and its metabolic gene targets are stimulated by mTORC1 signaling in the liver, in a hepatocyte-intrinsic manner by insulin in response to feeding. While we demonstrate that de novo purine and pyrimidine synthesis is stimulated by insulin through mTORC1 signaling in primary hepatocytes, this regulation was independent of ATF4. Metabolomics and metabolite tracing studies revealed that insulin-mTORC1-ATF4 signaling stimulates pathways of nonessential amino acid synthesis in primary hepatocytes, including those of alanine, aspartate, methionine, and cysteine, but not serine. Conclusions: The results demonstrate that ATF4 is a novel metabolic effector of mTORC1 in the liver, extending the molecular consequences of feeding and insulin-induced mTORC1 signaling in this key metabolic tissue to the control of amino acid metabolism.http://www.sciencedirect.com/science/article/pii/S2212877821001563mTORC1ATF4LiverFeedingInsulinMethionine metabolism
collection DOAJ
language English
format Article
sources DOAJ
author Vanessa Byles
Yann Cormerais
Krystle Kalafut
Victor Barrera
James E. Hughes Hallett
Shannan Ho Sui
John M. Asara
Christopher M. Adams
Gerta Hoxhaj
Issam Ben-Sahra
Brendan D. Manning
spellingShingle Vanessa Byles
Yann Cormerais
Krystle Kalafut
Victor Barrera
James E. Hughes Hallett
Shannan Ho Sui
John M. Asara
Christopher M. Adams
Gerta Hoxhaj
Issam Ben-Sahra
Brendan D. Manning
Hepatic mTORC1 signaling activates ATF4 as part of its metabolic response to feeding and insulin
Molecular Metabolism
mTORC1
ATF4
Liver
Feeding
Insulin
Methionine metabolism
author_facet Vanessa Byles
Yann Cormerais
Krystle Kalafut
Victor Barrera
James E. Hughes Hallett
Shannan Ho Sui
John M. Asara
Christopher M. Adams
Gerta Hoxhaj
Issam Ben-Sahra
Brendan D. Manning
author_sort Vanessa Byles
title Hepatic mTORC1 signaling activates ATF4 as part of its metabolic response to feeding and insulin
title_short Hepatic mTORC1 signaling activates ATF4 as part of its metabolic response to feeding and insulin
title_full Hepatic mTORC1 signaling activates ATF4 as part of its metabolic response to feeding and insulin
title_fullStr Hepatic mTORC1 signaling activates ATF4 as part of its metabolic response to feeding and insulin
title_full_unstemmed Hepatic mTORC1 signaling activates ATF4 as part of its metabolic response to feeding and insulin
title_sort hepatic mtorc1 signaling activates atf4 as part of its metabolic response to feeding and insulin
publisher Elsevier
series Molecular Metabolism
issn 2212-8778
publishDate 2021-11-01
description Objective: The mechanistic target of rapamycin complex 1 (mTORC1) is dynamically regulated by fasting and feeding cycles in the liver to promote protein and lipid synthesis while suppressing autophagy. However, beyond these functions, the metabolic response of the liver to feeding and insulin signaling orchestrated by mTORC1 remains poorly defined. Here, we determine whether ATF4, a stress responsive transcription factor recently found to be independently regulated by mTORC1 signaling in proliferating cells, is responsive to hepatic mTORC1 signaling to alter hepatocyte metabolism. Methods: ATF4 protein levels and expression of canonical gene targets were analyzed in the liver following fasting and physiological feeding in the presence or absence of the mTORC1 inhibitor, rapamycin. Primary hepatocytes from wild-type or liver-specific Atf4 knockout (LAtf4KO) mice were used to characterize the effects of insulin-stimulated mTORC1-ATF4 function on hepatocyte gene expression and metabolism. Both unbiased steady-state metabolomics and stable-isotope tracing methods were employed to define mTORC1 and ATF4-dependent metabolic changes. RNA-sequencing was used to determine global changes in feeding-induced transcripts in the livers of wild-type versus LAtf4KO mice. Results: We demonstrate that ATF4 and its metabolic gene targets are stimulated by mTORC1 signaling in the liver, in a hepatocyte-intrinsic manner by insulin in response to feeding. While we demonstrate that de novo purine and pyrimidine synthesis is stimulated by insulin through mTORC1 signaling in primary hepatocytes, this regulation was independent of ATF4. Metabolomics and metabolite tracing studies revealed that insulin-mTORC1-ATF4 signaling stimulates pathways of nonessential amino acid synthesis in primary hepatocytes, including those of alanine, aspartate, methionine, and cysteine, but not serine. Conclusions: The results demonstrate that ATF4 is a novel metabolic effector of mTORC1 in the liver, extending the molecular consequences of feeding and insulin-induced mTORC1 signaling in this key metabolic tissue to the control of amino acid metabolism.
topic mTORC1
ATF4
Liver
Feeding
Insulin
Methionine metabolism
url http://www.sciencedirect.com/science/article/pii/S2212877821001563
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AT jamesehugheshallett hepaticmtorc1signalingactivatesatf4aspartofitsmetabolicresponsetofeedingandinsulin
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