TORC1-mediated sensing of chaperone activity alters glucose metabolism and extends lifespan

Matea Perić; Anita Lovrić; Ana Šarić; Marina Musa; Peter Bou Dib; Marina Rudan; Andrea Nikolić; Sandra Sobočanec; Ana Matea Mikecin; Sven Dennerlein; Ira Milošević; Kristian Vlahoviček; Nuno Raimundo; Anita Kriško

doi:10.1111/acel.12623

TORC1-mediated sensing of chaperone activity alters glucose metabolism and extends lifespan

Matea Perić, Anita Lovrić, Ana Šarić, Marina Musa, Peter Bou Dib, Marina Rudan, Andrea Nikolić, Sandra Sobočanec, Ana Matea Mikecin, Sven Dennerlein, Ira Milošević, Kristian Vlahoviček, Nuno Raimundo, Anita Kriško

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

21 Scopus citations

Abstract

Protein quality control mechanisms, required for normal cellular functioning, encompass multiple functions related to protein production and maintenance. However, the existence of communication between proteostasis and metabolic networks and its underlying mechanisms remain elusive. Here, we report that enhanced chaperone activity and consequent improved proteostasis are sensed by TORC1 via the activity of Hsp82. Chaperone enrichment decreases the level of Hsp82, which deactivates TORC1 and leads to activation of Snf1/AMPK, regardless of glucose availability. This mechanism culminates in the extension of yeast replicative lifespan (RLS) that is fully reliant on both TORC1 deactivation and Snf1/AMPK activation. Specifically, we identify oxygen consumption increase as the downstream effect of Snf1 activation responsible for the entire RLS extension. Our results set a novel paradigm for the role of proteostasis in aging: modulation of the misfolded protein level can affect cellular metabolic features as well as mitochondrial activity and consequently modify lifespan. The described mechanism is expected to open new avenues for research of aging and age-related diseases.

Original language	English (US)
Pages (from-to)	994-1005
Number of pages	12
Journal	Aging cell
Volume	16
Issue number	5
DOIs	https://doi.org/10.1111/acel.12623
State	Published - Oct 2017

All Science Journal Classification (ASJC) codes

Aging
Cell Biology

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10.1111/acel.12623

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@article{99f4e525d7af4036b441bc53651d7d1e,

title = "TORC1-mediated sensing of chaperone activity alters glucose metabolism and extends lifespan",

abstract = "Protein quality control mechanisms, required for normal cellular functioning, encompass multiple functions related to protein production and maintenance. However, the existence of communication between proteostasis and metabolic networks and its underlying mechanisms remain elusive. Here, we report that enhanced chaperone activity and consequent improved proteostasis are sensed by TORC1 via the activity of Hsp82. Chaperone enrichment decreases the level of Hsp82, which deactivates TORC1 and leads to activation of Snf1/AMPK, regardless of glucose availability. This mechanism culminates in the extension of yeast replicative lifespan (RLS) that is fully reliant on both TORC1 deactivation and Snf1/AMPK activation. Specifically, we identify oxygen consumption increase as the downstream effect of Snf1 activation responsible for the entire RLS extension. Our results set a novel paradigm for the role of proteostasis in aging: modulation of the misfolded protein level can affect cellular metabolic features as well as mitochondrial activity and consequently modify lifespan. The described mechanism is expected to open new avenues for research of aging and age-related diseases.",

author = "Matea Peri{\'c} and Anita Lovri{\'c} and Ana {\v S}ari{\'c} and Marina Musa and {Bou Dib}, Peter and Marina Rudan and Andrea Nikoli{\'c} and Sandra Sobo{\v c}anec and Mikecin, {Ana Matea} and Sven Dennerlein and Ira Milo{\v s}evi{\'c} and Kristian Vlahovi{\v c}ek and Nuno Raimundo and Anita Kri{\v s}ko",

note = "Funding Information: This work was supported by the Fondation Nelia et Amedeo Barletta, NAOS Group, and the Mediterranean Institute for Life Sciences to AV, MP, MM, MR, AN, and AK; Croatian Ministry of Science, Education and Sports, Grant No. 098-0982464-1647 to A{\v S} and SS; European Commission Seventh Framework Program, Integra-Life; grant 315997 to KV; FP7-REGPOT-2012-2013-1, Grant No. 316289, InnoMol to AMM; grant 337327 from the European Research Council to NR and PBD; IM is supported by an Emmy Noether Award from the Deutsche Forschungsgemeinschaft. The authors would like to thank Tea Copi{\'c} and Iva Pe{\v s}un Me{\d}imorec for their excellent technical contribution. AK is grateful to Miroslav Radman, Tobias Warnecke, and Fran Supek for valuable discussions and reading the manuscript. Publisher Copyright: {\textcopyright} 2017 The Authors. Aging Cell published by the Anatomical Society and John Wiley & Sons Ltd.",

year = "2017",

month = oct,

doi = "10.1111/acel.12623",

language = "English (US)",

volume = "16",

pages = "994--1005",

journal = "Aging cell",

issn = "1474-9718",

publisher = "Wiley-Blackwell",

number = "5",

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TY - JOUR

T1 - TORC1-mediated sensing of chaperone activity alters glucose metabolism and extends lifespan

AU - Perić, Matea

AU - Lovrić, Anita

AU - Šarić, Ana

AU - Musa, Marina

AU - Bou Dib, Peter

AU - Rudan, Marina

AU - Nikolić, Andrea

AU - Sobočanec, Sandra

AU - Mikecin, Ana Matea

AU - Dennerlein, Sven

AU - Milošević, Ira

AU - Vlahoviček, Kristian

AU - Raimundo, Nuno

AU - Kriško, Anita

N1 - Funding Information: This work was supported by the Fondation Nelia et Amedeo Barletta, NAOS Group, and the Mediterranean Institute for Life Sciences to AV, MP, MM, MR, AN, and AK; Croatian Ministry of Science, Education and Sports, Grant No. 098-0982464-1647 to AŠ and SS; European Commission Seventh Framework Program, Integra-Life; grant 315997 to KV; FP7-REGPOT-2012-2013-1, Grant No. 316289, InnoMol to AMM; grant 337327 from the European Research Council to NR and PBD; IM is supported by an Emmy Noether Award from the Deutsche Forschungsgemeinschaft. The authors would like to thank Tea Copić and Iva Pešun Međimorec for their excellent technical contribution. AK is grateful to Miroslav Radman, Tobias Warnecke, and Fran Supek for valuable discussions and reading the manuscript. Publisher Copyright: © 2017 The Authors. Aging Cell published by the Anatomical Society and John Wiley & Sons Ltd.

PY - 2017/10

Y1 - 2017/10

N2 - Protein quality control mechanisms, required for normal cellular functioning, encompass multiple functions related to protein production and maintenance. However, the existence of communication between proteostasis and metabolic networks and its underlying mechanisms remain elusive. Here, we report that enhanced chaperone activity and consequent improved proteostasis are sensed by TORC1 via the activity of Hsp82. Chaperone enrichment decreases the level of Hsp82, which deactivates TORC1 and leads to activation of Snf1/AMPK, regardless of glucose availability. This mechanism culminates in the extension of yeast replicative lifespan (RLS) that is fully reliant on both TORC1 deactivation and Snf1/AMPK activation. Specifically, we identify oxygen consumption increase as the downstream effect of Snf1 activation responsible for the entire RLS extension. Our results set a novel paradigm for the role of proteostasis in aging: modulation of the misfolded protein level can affect cellular metabolic features as well as mitochondrial activity and consequently modify lifespan. The described mechanism is expected to open new avenues for research of aging and age-related diseases.

AB - Protein quality control mechanisms, required for normal cellular functioning, encompass multiple functions related to protein production and maintenance. However, the existence of communication between proteostasis and metabolic networks and its underlying mechanisms remain elusive. Here, we report that enhanced chaperone activity and consequent improved proteostasis are sensed by TORC1 via the activity of Hsp82. Chaperone enrichment decreases the level of Hsp82, which deactivates TORC1 and leads to activation of Snf1/AMPK, regardless of glucose availability. This mechanism culminates in the extension of yeast replicative lifespan (RLS) that is fully reliant on both TORC1 deactivation and Snf1/AMPK activation. Specifically, we identify oxygen consumption increase as the downstream effect of Snf1 activation responsible for the entire RLS extension. Our results set a novel paradigm for the role of proteostasis in aging: modulation of the misfolded protein level can affect cellular metabolic features as well as mitochondrial activity and consequently modify lifespan. The described mechanism is expected to open new avenues for research of aging and age-related diseases.

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U2 - 10.1111/acel.12623

DO - 10.1111/acel.12623

M3 - Article

C2 - 28613034

AN - SCOPUS:85020653431

SN - 1474-9718

VL - 16

SP - 994

EP - 1005

JO - Aging cell

JF - Aging cell

IS - 5

ER -

TORC1-mediated sensing of chaperone activity alters glucose metabolism and extends lifespan

Abstract

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