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. 2025 Nov;4(11):1487-1500.
doi: 10.1038/s44161-025-00726-x. Epub 2025 Sep 29.

Targeted glycophagy ATG8 therapy reverses diabetic heart disease in mice and in human engineered cardiac tissues

K M Mellor  1   2 U Varma  2 P Koutsifeli  1 C L Curl  2 J V Janssens  2   3 L J Daniels  1 G B Bernasochi  2 A J A Raaijmakers  2 M Annandale  1 X Li  1 S L James  1 D J Taylor  3 K Raedschelders  3 K L Weeks  2   4 R J Mills  5 R G Parton  6 X Hu  7 J R Bell  2   8 T J O'Brien  9   10 R Katare  11 E R Porrello  2   5 J E Hudson  12   13 R P Xiao  7 J E Van Eyk  3 R A Gottlieb  3 L M D Delbridge  14   15
Affiliations

Targeted glycophagy ATG8 therapy reverses diabetic heart disease in mice and in human engineered cardiac tissues

K M Mellor et al. Nat Cardiovasc Res. 2025 Nov.

Abstract

Diabetic heart disease is highly prevalent and is associated with the early development of impaired diastolic relaxation. The mechanisms of diabetic heart disease are poorly understood, and it is a condition for which there are no targeted therapies. Recently, disrupted glycogen autophagy (glycophagy) and glycogen accumulation have been identified in the diabetic heart. Glycophagy involves glycogen receptor binding and linking with an ATG8 protein to locate and degrade glycogen within an intracellular phagolysosome. Here we show that glycogen receptor protein starch binding domain protein 1 (STBD1) is mobilized early in the cardiac glycogen response to metabolic challenge in vivo, and that deficiency of a specific ATG8 family protein, γ-aminobutyric acid type A receptor-associated protein-like 1 (GABARAPL1), is associated with diastolic dysfunction in diabetes. Gabarapl1 gene delivery treatment remediated cardiomyocyte and cardiac diastolic dysfunction in type 2 diabetic mice and the diastolic performance of 'diabetic' human induced pluripotent stem cell-derived cardiac organoids. We identify glycophagy dysregulation as a mechanism and potential treatment target for diabetic heart disease.

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Conflict of interest statement

Competing interests: The authors declare no competing interests.

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References

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