Genetic loss of AMPK-glycogen binding destabilises AMPK and disrupts metabolism.

Hoffman, Nolan J; Whitfield, Jamie; Janzen, Natalie R; Belhaj, Mehdi R; Galic, Sandra; Murray-Segal, Lisa; Smiles, William J; Ling, Naomi X Y; Dite, Toby A; Scott, John W; Oakhill, Jonathan S; Brink, Robert; Kemp, Bruce E; Hawley, John A

Hoffman, Nolan J; Whitfield, Jamie; Janzen, Natalie R; Belhaj, Mehdi R; Galic, Sandra; Murray-Segal, Lisa; Smiles, William J; Ling, Naomi X Y; Dite, Toby A; Scott, John W; Oakhill, Jonathan S; Brink, Robert; Kemp, Bruce E; Hawley, John A.

Affiliation

Hoffman NJ; Exercise and Nutrition Research Program, Mary MacKillop Institute for Health Research, Australian Catholic University, Level 5, 215 Spring Street, Melbourne, Victoria 3000, Australia. Electronic address: nolan.hoffman@acu.edu.au.
Whitfield J; Exercise and Nutrition Research Program, Mary MacKillop Institute for Health Research, Australian Catholic University, Level 5, 215 Spring Street, Melbourne, Victoria 3000, Australia.
Janzen NR; Exercise and Nutrition Research Program, Mary MacKillop Institute for Health Research, Australian Catholic University, Level 5, 215 Spring Street, Melbourne, Victoria 3000, Australia.
Belhaj MR; Exercise and Nutrition Research Program, Mary MacKillop Institute for Health Research, Australian Catholic University, Level 5, 215 Spring Street, Melbourne, Victoria 3000, Australia.
Galic S; St. Vincent's Institute of Medical Research and Department of Medicine, University of Melbourne, 9 Princes Street, Fitzroy, Victoria 3065, Australia.
Murray-Segal L; St. Vincent's Institute of Medical Research and Department of Medicine, University of Melbourne, 9 Princes Street, Fitzroy, Victoria 3065, Australia.
Smiles WJ; St. Vincent's Institute of Medical Research and Department of Medicine, University of Melbourne, 9 Princes Street, Fitzroy, Victoria 3065, Australia.
Ling NXY; St. Vincent's Institute of Medical Research and Department of Medicine, University of Melbourne, 9 Princes Street, Fitzroy, Victoria 3065, Australia.
Dite TA; St. Vincent's Institute of Medical Research and Department of Medicine, University of Melbourne, 9 Princes Street, Fitzroy, Victoria 3065, Australia.
Scott JW; Exercise and Nutrition Research Program, Mary MacKillop Institute for Health Research, Australian Catholic University, Level 5, 215 Spring Street, Melbourne, Victoria 3000, Australia; St. Vincent's Institute of Medical Research and Department of Medicine, University of Melbourne, 9 Princes Street, F
Oakhill JS; Exercise and Nutrition Research Program, Mary MacKillop Institute for Health Research, Australian Catholic University, Level 5, 215 Spring Street, Melbourne, Victoria 3000, Australia; St. Vincent's Institute of Medical Research and Department of Medicine, University of Melbourne, 9 Princes Street, F
Brink R; Immunology Division, Garvan Institute of Medical Research, 384 Victoria Street, Darlinghurst, New South Wales 2010, Australia; St. Vincent's Clinical School, UNSW Sydney, Level 5 deLacy Building, St. Vincent's Hospital, Darlinghurst, New South Wales 2010, Australia.
Kemp BE; Exercise and Nutrition Research Program, Mary MacKillop Institute for Health Research, Australian Catholic University, Level 5, 215 Spring Street, Melbourne, Victoria 3000, Australia; St. Vincent's Institute of Medical Research and Department of Medicine, University of Melbourne, 9 Princes Street, F
Hawley JA; Exercise and Nutrition Research Program, Mary MacKillop Institute for Health Research, Australian Catholic University, Level 5, 215 Spring Street, Melbourne, Victoria 3000, Australia. Electronic address: john.hawley@acu.edu.au.

Mol Metab ; 41: 101048, 2020 11.

Article in En | MEDLINE | ID: mdl-32610071

ABSTRACT

ABSTRACT

OBJECTIVE:

Glycogen is a major energy reserve in liver and skeletal muscle. The master metabolic regulator AMP-activated protein kinase (AMPK) associates with glycogen via its regulatory ß subunit carbohydrate-binding module (CBM). However, the physiological role of AMPK-glycogen binding in energy homeostasis has not been investigated in vivo. This study aimed to determine the physiological consequences of disrupting AMPK-glycogen interactions.

METHODS:

Glycogen binding was disrupted in mice via whole-body knock-in (KI) mutation of either the AMPK ß1 (W100A) or ß2 (W98A) isoform CBM. Systematic whole-body, tissue and molecular phenotyping was performed in KI and respective wild-type (WT) mice.

RESULTS:

While ß1 W100A KI did not affect whole-body metabolism or exercise capacity, ß2 W98A KI mice displayed increased adiposity and impairments in whole-body glucose handling and maximal exercise capacity relative to WT. These KI mutations resulted in reduced total AMPK protein and kinase activity in liver and skeletal muscle of ß1 W100A and ß2 W98A, respectively, versus WT mice. ß1 W100A mice also displayed loss of fasting-induced liver AMPK total and α-specific kinase activation relative to WT. Destabilisation of AMPK was associated with increased fat deposition in ß1 W100A liver and ß2 W98A skeletal muscle versus WT.

CONCLUSIONS:

These results demonstrate that glycogen binding plays critical roles in stabilising AMPK and maintaining cellular, tissue and whole-body energy homeostasis.

Subject(s)

AMP-Activated Protein Kinases/metabolism; Energy Metabolism/physiology; Glycogen/metabolism; AMP-Activated Protein Kinases/physiology; Animals; Female; Glucose/metabolism; Glycogen/physiology; Homeostasis; Male; Mice; Mice, Inbred C57BL; Mice, Knockout; Muscle, Skeletal/metabolism; Phosphorylation; Protein Binding

Key words

AMP-activated protein kinase; Carbohydrate-binding module; Cellular energy sensing; Exercise; Liver; Skeletal muscle

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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Energy Metabolism / AMP-Activated Protein Kinases / Glycogen Limits: Animals Language: En Journal: Mol Metab Year: 2020 Document type: Article

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