MTORC1 Directly Inhibits AMPK to Promote Cell Proliferation Under Nutrient Stress

Overview

Journal Nat Metab

Publisher Springer Nature

Specialty Endocrinology

Date 2020 Jan 30

PMID 31993556

Citations 67

Authors

Naomi X Y Ling

Adrian Kaczmarek

Ashfaqul Hoque

Elizabeth Davie

Kevin R W Ngoei

Kaitlin R Morrison

William J Smiles

Gabriella M Forte

Tingting Wang

Shervi Lie

Toby A Dite

Christopher G Langendorf

John W Scott

Jonathan S Oakhill

Janni Petersen

Affiliations

Soon will be listed here.

Abstract

Central to cellular metabolism and cell proliferation are highly conserved signalling pathways controlled by mammalian target of rapamycin (mTOR) and AMP-activated protein kinase (AMPK), dysregulation of which are implicated in pathogenesis of major human diseases such as cancer and type 2 diabetes. AMPK pathways leading to reduced cell proliferation are well established and, in part, act through inhibition of TOR complex-1 (TORC1) activity. Here we demonstrate reciprocal regulation, specifically that TORC1 directly down-regulates AMPK signalling by phosphorylating the evolutionarily conserved residue Ser367 in the fission yeast AMPK catalytic subunit Ssp2, and AMPK α1Ser347/α2Ser345 in the mammalian homologs, which is associated with reduced phosphorylation of activation loop Thr172. Genetic or pharmacological inhibition of TORC1 signalling led to AMPK activation in the absence of increased AMP:ATP ratios; under nutrient stress conditions this was associated with growth limitation in both yeast and human cell cultures. Our findings reveal fundamental, bi-directional regulation between two major metabolic signalling networks and uncover new opportunity for cancer treatment strategies aimed at suppressing cell proliferation in the nutrient-poor tumor microenvironment.

Citing Articles

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