Liver lipophagy ameliorates nonalcoholic steatohepatitis through extracellular lipid secretion.
Yoshito MinamiAtsushi HoshinoYusuke HiguchiMasahide HamaguchiYusaku KanekoYuhei KiritaShunta TaminishiToshiyuki NishijiAkiyuki TarunoMichiaki FukuiZoltan AranySatoaki MatobaPublished in: Nature communications (2023)
Nonalcoholic steatohepatitis (NASH) is a progressive disorder with aberrant lipid accumulation and subsequent inflammatory and profibrotic response. Therapeutic efforts at lipid reduction via increasing cytoplasmic lipolysis unfortunately worsens hepatitis due to toxicity of liberated fatty acid. An alternative approach could be lipid reduction through autophagic disposal, i.e., lipophagy. We engineered a synthetic adaptor protein to induce lipophagy, combining a lipid droplet-targeting signal with optimized LC3-interacting domain. Activating hepatocyte lipophagy in vivo strongly mitigated both steatosis and hepatitis in a diet-induced mouse NASH model. Mechanistically, activated lipophagy promoted the excretion of lipid from hepatocytes, thereby suppressing harmful intracellular accumulation of nonesterified fatty acid. A high-content compound screen identified alpelisib and digoxin, clinically-approved compounds, as effective activators of lipophagy. Administration of alpelisib or digoxin in vivo strongly inhibited the transition to steatohepatitis. These data thus identify lipophagy as a promising therapeutic approach to prevent NASH progression.
Keyphrases
- fatty acid
- oxidative stress
- signaling pathway
- adipose tissue
- cell death
- multiple sclerosis
- high throughput
- insulin resistance
- type diabetes
- mass spectrometry
- drug delivery
- mouse model
- liver injury
- big data
- quality improvement
- artificial intelligence
- heavy metals
- simultaneous determination
- high resolution
- skeletal muscle
- protein protein
- high resolution mass spectrometry
- tandem mass spectrometry
- anaerobic digestion