Metabolic and transcriptional adaptations to phagocytosis sustain microglia functionality and regenerative properties

  1. Mar Marquez-Ropero
  2. Jorge Valero
  3. Xabier Cuesta-Puente
  4. Angel Marquez-Galera
  5. Marta Pereira-Iglesias
  6. Alice Louail
  7. Marco Gonzalez-Dominguez
  8. Sol Beccari
  9. Luzia Lopez-Murillo
  10. Amaia San Juan
  11. Guillermo Arrey
  12. Irune Diaz-Aparicio
  13. Montserrat Puigdelloses-Valcobra
  14. Marissa L. Dubbelaar
  15. Alberto Ribera-Ramos
  16. Manuel Sarmiento-Soto
  17. Rocío Ruiz
  18. Leyre Ayerra
  19. Amaia Vilas-Zornoza
  20. Diana Cabrera
  21. Sebastiaan van Liempd
  22. Fernando García-Moreno
  23. Klas Blomgren
  24. Susana González-Granero
  25. Jose M. García-Verdugo
  26. Juan M. Falcón-Pérez
  27. María S. Aymerich
  28. Dolores Hambardzumyan
  29. Iñigo Casafont
  30. Bart Eggen
  31. José L. Venero
  32. Jose P. López-Atalaya
  33. Amanda Sierra
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Abstract

Phagocytosis of apoptotic cells, or efferocytosis, is a tightly regulated process that ensures tissue homeostasis and prevents mounting inflammatory responses. In the brain parenchyma, it is executed by microglia, which are encumbered by large numbers of apoptotic debris generated during development, in adult neurogenic niches, aging, and brain diseases. Emerging evidence suggest that phagocytosis is not limited to garbage disposal, but triggers adaptations in the phagocytes that may have a functional impact. To test it we developed an in vivo model of superphagocytosis induced by low cranial irradiation (LCI, 2Gy) that specifically induced apoptosis in the neurogenic niche of the adult hippocampus, synchronizing microglia in a phagocytic state within 6h and leading to full clearance by 24h. Single cell RNA sequencing and metabolomics revealed an unexpected oxidative stress in post-phagocytic microglia, accompanied by catabolic shutdown, mitochondrial remodeling, increased expression of galectin 3, and production of polyamines that led to cell death and compensatory proliferation. To test whether these changes impaired subsequent microglial phagocytosis, we used a glioblastoma model treated with sequential irradiation to induce tumor cell apoptosis. The phagocytosis efficiency of tumor-associated microglia/macrophages was comparable in the first and second apoptotic challenge, suggesting that the metabolic remodeling induced by phagocytosis was adaptive and destined to sustain their functionality. Finally, we assessed the functional impact of post-phagocytosis adaptations using galectin 3 deficient mice under LCI. We found that the recovery of the neurogenic niche after LCI strongly depended on galectin 3, demonstrating the regenerative capacity of post-phagocytic microglia. Overall, our data unveils the complexity of post-phagocytosis adaptations in microglia, underscoring their unexplored therapeutic potential in brain disorders.

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  1. Version published to 10.1101/2025.09.18.676800 on bioRxiv