HRAS germline mutations impair LKB1/AMPK signaling and mitochondrial homeostasis in Costello syndrome models
Laetitia Dard, … , Didier Lacombe, Rodrigue Rossignol
Laetitia Dard, … , Didier Lacombe, Rodrigue Rossignol
Published March 1, 2022
Citation Information: J Clin Invest. 2022;132(8):e131053. https://doi.org/10.1172/JCI131053.
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Research Article Metabolism

HRAS germline mutations impair LKB1/AMPK signaling and mitochondrial homeostasis in Costello syndrome models

Abstract

Germline mutations that activate genes in the canonical RAS/MAPK signaling pathway are responsible for rare human developmental disorders known as RASopathies. Here, we analyzed the molecular determinants of Costello syndrome (CS) using a mouse model expressing HRAS p.G12S, patient skin fibroblasts, hiPSC-derived human cardiomyocytes, a HRAS p.G12V zebrafish model, and human fibroblasts expressing lentiviral constructs carrying HRAS p.G12S or HRAS p.G12A mutations. The findings revealed alteration of mitochondrial proteostasis and defective oxidative phosphorylation in the heart and skeletal muscle of CS mice that were also found in the cell models of the disease. The underpinning mechanisms involved the inhibition of the AMPK signaling pathway by mutant forms of HRAS, leading to alteration of mitochondrial proteostasis and bioenergetics. Pharmacological activation of mitochondrial bioenergetics and quality control restored organelle function in HRAS p.G12A and p.G12S cell models, reduced left ventricle hypertrophy in CS mice, and diminished the occurrence of developmental defects in the CS zebrafish model. Collectively, these findings highlight the importance of mitochondrial proteostasis and bioenergetics in the pathophysiology of RASopathies and suggest that patients with CS may benefit from treatment with mitochondrial modulators.

Authors

Laetitia Dard, Christophe Hubert, Pauline Esteves, Wendy Blanchard, Ghina Bou About, Lyla Baldasseroni, Elodie Dumon, Chloe Angelini, Mégane Delourme, Véronique Guyonnet-Dupérat, Stéphane Claverol, Laura Fontenille, Karima Kissa, Pierre-Emmanuel Séguéla, Jean-Benoît Thambo, Lévy Nicolas, Yann Herault, Nadège Bellance, Nivea Dias Amoedo, Frédérique Magdinier, Tania Sorg, Didier Lacombe, Rodrigue Rossignol

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Figure 2

Mitochondrial bioenergetics is altered in situ in the CS mouse heart and skeletal muscle.

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Mitochondrial bioenergetics is altered in situ in the CS mouse heart and...
(A) Permeabilized heart muscle fibers bioenergetics evaluation methods. (B) Rate of coupled (ADP-stimulated “state 3”) respiration was determined in situ using high-resolution respirometry (WT, n = 6; Costello, n = 9). (C and D) Rate of mitochondrial ATP synthesis (vATp) determined in heart-permeabilized muscle fibers (WT, n = 5; Costello, n = 6). (E) Electron transport chain (ETC) complex enzymatic activities determined in WT or Costello mouse model hearts (WT, n = 4; Costello, n = 4). (F) Respiratory chain complex enzymatic activities determined in WT or Costello mouse model skeletal muscle (WT, n = 4; Costello, n = 4). (G) Histo-enzymology staining of the respiratory chain complex IV (COX) specific activity. Muscle fibers and their nuclei were stained using H&E. Original magnification, ×1000. (H) Quantification of the COX-positive muscle fibers (WT, n = 3; Costello, n = 3). Data are expressed as the mean ± SEM. *P < 0.05, **P < 0.01, ***P < 0.001 (unpaired t test).