Atrogin-1 deficiency promotes cardiomyopathy and premature death via impaired autophagy
Tania Zaglia, Giulia Milan, Aaron Ruhs, Mauro Franzoso, Enrico Bertaggia, Nicola Pianca, Andrea Carpi, Pierluigi Carullo, Paola Pesce, David Sacerdoti, Cristiano Sarais, Daniele Catalucci, Marcus Krüger, Marco Mongillo, Marco Sandri
Tania Zaglia, Giulia Milan, Aaron Ruhs, Mauro Franzoso, Enrico Bertaggia, Nicola Pianca, Andrea Carpi, Pierluigi Carullo, Paola Pesce, David Sacerdoti, Cristiano Sarais, Daniele Catalucci, Marcus Krüger, Marco Mongillo, Marco Sandri
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Research Article Cardiology

Atrogin-1 deficiency promotes cardiomyopathy and premature death via impaired autophagy

Abstract

Cardiomyocyte proteostasis is mediated by the ubiquitin/proteasome system (UPS) and autophagy/lysosome system and is fundamental for cardiac adaptation to both physiologic (e.g., exercise) and pathologic (e.g., pressure overload) stresses. Both the UPS and autophagy/lysosome system exhibit reduced efficiency as a consequence of aging, and dysfunction in these systems is associated with cardiomyopathies. The muscle-specific ubiquitin ligase atrogin-1 targets signaling proteins involved in cardiac hypertrophy for degradation. Here, using atrogin-1 KO mice in combination with in vivo pulsed stable isotope labeling of amino acids in cell culture proteomics and biochemical and cellular analyses, we identified charged multivesicular body protein 2B (CHMP2B), which is part of an endosomal sorting complex (ESCRT) required for autophagy, as a target of atrogin-1–mediated degradation. Mice lacking atrogin-1 failed to degrade CHMP2B, resulting in autophagy impairment, intracellular protein aggregate accumulation, unfolded protein response activation, and subsequent cardiomyocyte apoptosis, all of which increased progressively with age. Cellular proteostasis alterations resulted in cardiomyopathy characterized by myocardial remodeling with interstitial fibrosis, with reduced diastolic function and arrhythmias. CHMP2B downregulation in atrogin-1 KO mice restored autophagy and decreased proteotoxicity, thereby preventing cell death. These data indicate that atrogin-1 promotes cardiomyocyte health through mediating the interplay between UPS and autophagy/lysosome system and its alteration promotes development of cardiomyopathies.

Authors

Tania Zaglia, Giulia Milan, Aaron Ruhs, Mauro Franzoso, Enrico Bertaggia, Nicola Pianca, Andrea Carpi, Pierluigi Carullo, Paola Pesce, David Sacerdoti, Cristiano Sarais, Daniele Catalucci, Marcus Krüger, Marco Mongillo, Marco Sandri

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Figure 7

CHMP2B overexpression causes an impairment in the autophagy flux per se.

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CHMP2B overexpression causes an impairment in the autophagy flux per se....
(A and B) Confocal immunofluorescence analysis of neonatal WT cardiomyocytes transfected either with (A) LC3-YFP (green signal) or (B) LC3-YFP/CHMP2B and stained with an antibody against CHMP2B (red signal). (C) Cultured neonatal cardiomyocytes were transfected either with YFP-LC3 (green signal, –CHMPB) or cotransfected with YFP-LC3– and CHMP2B-expressing vectors (+CHMP2B). Autophagosomes were analyzed by confocal microscopy. The same analysis was performed also in the presence of the autophagy inhibitor bafilomycin (+BFL). The right-most images in AC show high-magnification views of the white boxes in the left images. Scale bar: 10 μm (left and middle images); 1 μm (right images). (D) Quantification of the total number of YFP-LC3 vesicles in cardiomyocytes both at baseline and upon CHMP2B overexpression both in presence and absence of bafilomycin. Error bars indicate SEM (**P < 0.01; n = 50 cardiomyocytes for each group).