PKG-Modified TSC2 Regulates mTORC1 Activity to Counter Adverse Cardiac Stress

The mechanistic target of rapamycin complex-1 (mTORC1) coordinates regulation of growth, metabolism, protein synthesis, and autophagy(1). Its hyper-activation contributes to disease in many organs including the heart(1,2), though broad mTORC1 inhibition risks interference with its homeostatic roles....

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Autores principales: Ranek, Mark J., Kokkonen-Simon, Kristen M., Chen, Anna, Dunkerly-Eyring, Brittany L., Vera, Miguel Pinilla, Oeing, Christian U., Patel, Chirag H., Nakamura, Taishi, Zhu, Guangshuo, Bedja, Djahida, Sasaki, Masayuki, Holewinski, Ronald J., Van Eyk, Jennifer E., Powell, Jonathan D., Lee, Dong Ik, Kass, David A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2019
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6426636/
https://www.ncbi.nlm.nih.gov/pubmed/30700906
http://dx.doi.org/10.1038/s41586-019-0895-y
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author Ranek, Mark J.
Kokkonen-Simon, Kristen M.
Chen, Anna
Dunkerly-Eyring, Brittany L.
Vera, Miguel Pinilla
Oeing, Christian U.
Patel, Chirag H.
Nakamura, Taishi
Zhu, Guangshuo
Bedja, Djahida
Sasaki, Masayuki
Holewinski, Ronald J.
Van Eyk, Jennifer E.
Powell, Jonathan D.
Lee, Dong Ik
Kass, David A.
author_facet Ranek, Mark J.
Kokkonen-Simon, Kristen M.
Chen, Anna
Dunkerly-Eyring, Brittany L.
Vera, Miguel Pinilla
Oeing, Christian U.
Patel, Chirag H.
Nakamura, Taishi
Zhu, Guangshuo
Bedja, Djahida
Sasaki, Masayuki
Holewinski, Ronald J.
Van Eyk, Jennifer E.
Powell, Jonathan D.
Lee, Dong Ik
Kass, David A.
author_sort Ranek, Mark J.
collection PubMed
description The mechanistic target of rapamycin complex-1 (mTORC1) coordinates regulation of growth, metabolism, protein synthesis, and autophagy(1). Its hyper-activation contributes to disease in many organs including the heart(1,2), though broad mTORC1 inhibition risks interference with its homeostatic roles. Tuberin (TSC2) is a GTPase-activating protein and prominent intrinsic regulator of mTORC1 by modulating Rheb (Ras homolog enriched in brain). TSC2 constitutively inhibits mTORC1, but this activity is modified by phosphorylation from multiple signaling kinases to in turn inhibit (AMPK, GSK3β) or stimulate (Akt, ERK, RSK-1) mTORC1 activity(3–9). Each kinase requires engagement of multiple serines, impeding analysis of their role in vivo. Here, we reveal phosphorylation or gain-or-loss of function mutations at either of two adjacent serines in TSC2 (S1365/1366 mouse; 1364/1365 human), with no prior known function, is sufficient to bi-directionally potently control growth-factor and hemodynamic-stress stimulated mTORC1 activity and consequent cell growth and autophagy. Basal mTORC1 activity, however, is unchanged. In heart, myocytes, and fibroblasts, phosphorylation occurs by protein kinase G (PKG), a primary effector of nitric oxide and natriuretic peptide signaling whose activation is protective against heart disease(10–13). PKG suppression of hypertrophy and stimulation of autophagy in myocytes requires TSC2 phosphorylation. Homozygous knock-in (KI) mice expressing a phospho-silenced TSC2 (S1365A) mutation develop far worse heart disease and mortality from sustained pressure-overload (PO) due to hyperactive mTORC1 that cannot be rescued by PKG stimulation. Heterozygote SA-KI are rescued, and KI-mice expressing a phospho-mimetic (S1365E) mutation are protected. Neither KI model alters resting mTORC1 activity. Thus, TSC2 phosphorylation is both required and sufficient for PKG-mediated cardiac protection against pressure-overload. These newly identified serines provide a genetic tool to bi-directionally regulate the amplitude of stress-stimulated mTORC1 activity.
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spelling pubmed-64266362019-07-30 PKG-Modified TSC2 Regulates mTORC1 Activity to Counter Adverse Cardiac Stress Ranek, Mark J. Kokkonen-Simon, Kristen M. Chen, Anna Dunkerly-Eyring, Brittany L. Vera, Miguel Pinilla Oeing, Christian U. Patel, Chirag H. Nakamura, Taishi Zhu, Guangshuo Bedja, Djahida Sasaki, Masayuki Holewinski, Ronald J. Van Eyk, Jennifer E. Powell, Jonathan D. Lee, Dong Ik Kass, David A. Nature Article The mechanistic target of rapamycin complex-1 (mTORC1) coordinates regulation of growth, metabolism, protein synthesis, and autophagy(1). Its hyper-activation contributes to disease in many organs including the heart(1,2), though broad mTORC1 inhibition risks interference with its homeostatic roles. Tuberin (TSC2) is a GTPase-activating protein and prominent intrinsic regulator of mTORC1 by modulating Rheb (Ras homolog enriched in brain). TSC2 constitutively inhibits mTORC1, but this activity is modified by phosphorylation from multiple signaling kinases to in turn inhibit (AMPK, GSK3β) or stimulate (Akt, ERK, RSK-1) mTORC1 activity(3–9). Each kinase requires engagement of multiple serines, impeding analysis of their role in vivo. Here, we reveal phosphorylation or gain-or-loss of function mutations at either of two adjacent serines in TSC2 (S1365/1366 mouse; 1364/1365 human), with no prior known function, is sufficient to bi-directionally potently control growth-factor and hemodynamic-stress stimulated mTORC1 activity and consequent cell growth and autophagy. Basal mTORC1 activity, however, is unchanged. In heart, myocytes, and fibroblasts, phosphorylation occurs by protein kinase G (PKG), a primary effector of nitric oxide and natriuretic peptide signaling whose activation is protective against heart disease(10–13). PKG suppression of hypertrophy and stimulation of autophagy in myocytes requires TSC2 phosphorylation. Homozygous knock-in (KI) mice expressing a phospho-silenced TSC2 (S1365A) mutation develop far worse heart disease and mortality from sustained pressure-overload (PO) due to hyperactive mTORC1 that cannot be rescued by PKG stimulation. Heterozygote SA-KI are rescued, and KI-mice expressing a phospho-mimetic (S1365E) mutation are protected. Neither KI model alters resting mTORC1 activity. Thus, TSC2 phosphorylation is both required and sufficient for PKG-mediated cardiac protection against pressure-overload. These newly identified serines provide a genetic tool to bi-directionally regulate the amplitude of stress-stimulated mTORC1 activity. 2019-01-30 2019-02 /pmc/articles/PMC6426636/ /pubmed/30700906 http://dx.doi.org/10.1038/s41586-019-0895-y Text en Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use:http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Ranek, Mark J.
Kokkonen-Simon, Kristen M.
Chen, Anna
Dunkerly-Eyring, Brittany L.
Vera, Miguel Pinilla
Oeing, Christian U.
Patel, Chirag H.
Nakamura, Taishi
Zhu, Guangshuo
Bedja, Djahida
Sasaki, Masayuki
Holewinski, Ronald J.
Van Eyk, Jennifer E.
Powell, Jonathan D.
Lee, Dong Ik
Kass, David A.
PKG-Modified TSC2 Regulates mTORC1 Activity to Counter Adverse Cardiac Stress
title PKG-Modified TSC2 Regulates mTORC1 Activity to Counter Adverse Cardiac Stress
title_full PKG-Modified TSC2 Regulates mTORC1 Activity to Counter Adverse Cardiac Stress
title_fullStr PKG-Modified TSC2 Regulates mTORC1 Activity to Counter Adverse Cardiac Stress
title_full_unstemmed PKG-Modified TSC2 Regulates mTORC1 Activity to Counter Adverse Cardiac Stress
title_short PKG-Modified TSC2 Regulates mTORC1 Activity to Counter Adverse Cardiac Stress
title_sort pkg-modified tsc2 regulates mtorc1 activity to counter adverse cardiac stress
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6426636/
https://www.ncbi.nlm.nih.gov/pubmed/30700906
http://dx.doi.org/10.1038/s41586-019-0895-y
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