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Galectins induced from hemocytes bridge phosphatidylserine and N-glycosylated Drpr/CED-1 receptor during dendrite pruning.

Hsin-Ho SungHsun LiYi-Chun HuangChun-Lu AiMing-Yen HsiehHau-Ming JanYu-Ju PengHsien-Ya LinChih-Hsuan YehShu-Yu LinChun-Yen YehYing-Ju ChengKai-Hooi KhooChun-Hung LinCheng-Ting Chien
Published in: Nature communications (2024)
During neuronal pruning, phagocytes engulf shed cellular debris to avoid inflammation and maintain tissue homeostasis. How phagocytic receptors recognize degenerating neurites had been unclear. Here, we identify two glucosyltransferases Alg8 and Alg10 of the N-glycosylation pathway required for dendrite fragmentation and clearance through genetic screen. The scavenger receptor Draper (Drpr) is N-glycosylated with complex- or hybrid-type N-glycans that interact specifically with galectins. We also identify the galectins Crouching tiger (Ctg) and Hidden dragon (Hdg) that interact with N-glycosylated Drpr and function in dendrite pruning via the Drpr pathway. Ctg and Hdg are required in hemocytes for expression and function, and are induced during dendrite injury to localize to injured dendrites through specific interaction with exposed phosphatidylserine (PS) on the surface membrane of injured dendrites. Thus, the galectins Ctg and Hdg bridge the interaction between PS and N-glycosylated Drpr, leading to the activation of phagocytosis.
Keyphrases
  • high glucose
  • diabetic rats
  • oxidative stress
  • poor prognosis
  • drug induced
  • genome wide
  • endothelial cells
  • gene expression
  • high throughput
  • dna methylation
  • single cell