Learn entry

Autophagy and the Gut: What Fasting Actually Triggers

Fasting activates autophagy through mTOR inhibition and AMPK activation, enhancing intestinal cell function; defects in autophagy genes drive inflammatory bowel disease.

Understand9 min read
Back to library
How this entry is structured
Definitions first, then mechanisms, then “so what?”. If you are in a hurry, skim the headings and callouts.
Not medical advice
Educational content only. If symptoms are severe, persistent, or worrying, see a clinician.

Cellular Housekeeping at the Molecular Level

Autophagy—literally 'self-eating'—is a conserved cellular process where the cell digests and recycles its own components. Fasting triggers autophagy through two interconnected nutrient-sensing pathways: inhibition of mechanistic target of rapamycin (mTOR) and activation of AMP-activated protein kinase (AMPK), which phosphorylates and activates ULK1 (unc-51-like kinase 1), the master autophagy initiator.

Once activated, ULK1 nucleates autophagosome formation through recruitment of Beclin-1 and the VPS34 complex. These cup-shaped structures engulf cytoplasmic contents and fuse with lysosomes where hydrolytic enzymes catalyse degradation. LC3 inserts into autophagosome membranes and serves as the primary autophagy marker.

In intestinal epithelial cells, autophagy serves specialised functions maintaining barrier integrity. Paneth cells, specialised in secreting antimicrobial peptides, depend critically on autophagy. Paneth cell autophagy defects, induced by ATG16L1 mutations (frequent in Crohn's disease patients), lead to impaired antimicrobial peptide secretion and dysbiosis. Similarly, goblet cells secreting protective mucus rely on autophagy; deficiency impairs mucus layer thickness and epithelial permeability.

Xenophagy—selective autophagy of intracellular bacteria—represents a direct antimicrobial mechanism. Bacteria invading the epithelium trigger recruitment of autophagy machinery to bacterial surfaces; LC3 conjugation marks bacteria for lysosomal degradation. Impaired xenophagy permits intracellular bacterial survival, driving chronic inflammation. IRGM, another Crohn's disease susceptibility gene, regulates xenophagy; loss-of-function variants impair bacterial elimination.

Fasting duration thresholds determine autophagy intensity. In mice, measurable autophagy begins after 12-16 hours of food deprivation; maximal activation requires 24-48 hours. In humans, 24-hour fasting induces substantial autophagy. Shorter fasts (16-18 hours) produce measurable but partial autophagy activation.

Was this entry helpful?

Sources & references

  1. Bagherniya M et al. (2018) The effect of fasting or calorie restriction on autophagy induction: A review of the literature Ageing Research Reviews PMID: 30172870
  2. Shabkhizan R et al. (2023) The Beneficial and Adverse Effects of Autophagic Response to Caloric Restriction and Fasting Advances in Nutrition PMID: 37527766
  3. Neurath MF et al. (2024) The Mucosal Immune System in Inflammatory Bowel Disease Lancet PMID: 38670345
  4. de Souza HSP et al. (2023) Innate and Adaptive Immunity in IBD Pathogenesis Nat Rev Gastroenterol Hepatol PMID: 37236901
  5. Serhan CN et al. (2008) The dual roles of neutrophils and macrophages in inflammation: a critical balance between tissue damage and repair Journal of Clinical Investigation PMID: 17273473

Continue reading

Editorial standards
Every entry is grounded in peer-reviewed research and reviewed for accuracy. How we write →