4.8 Article

Fringe-positive Golgi outposts unite temporal Furin 2 convertase activity and spatial Delta signal to promote dendritic branch retraction

Journal

CELL REPORTS
Volume 40, Issue 12, Pages -

Publisher

CELL PRESS
DOI: 10.1016/j.celrep.2022.111372

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Funding

  1. Basic Neuroscience Program of the NINDS Intramural Research Program of the NIH [Z01-NS003013]
  2. Ministry of Science and Technology [MOST 110-2326-B-001-008, 109-2326-B-001-016]
  3. Academia Sinica

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GOPs in the dendrites of Drosophila neurons have been found to play a role in promoting branch extension, but this study reveals their involvement in dendrite retraction as well. The glycosyltransferase Fng localizes increasingly at GOPs and its interaction with Fur2 affects the number of GOPs. Additionally, the Epidermal Delta ligand and neuronal Notch receptor negatively regulate dendrite growth.
Golgi outposts (GOPs) in dendrites are known for their role in promoting branch extension, but whether GOPs have other functions is unclear. We found that terminal branches of Drosophila class IV dendritic arborization (C4da) neurons actively grow during the early third-instar (E3) larval stage but retract in the late third (L3) stage. Interestingly, the Fringe (Fng) glycosyltransferase localizes increasingly at GOPs in distal dendritic regions through the E3 to the L3 stage. Expression of the endopeptidase Furin 2 (Fur2), which proteolyzes and inactivates Fng, decreases from E3 to L3 in C4da neurons, thereby increasing Fng-positive GOPs in dendrites. The epidermal Delta ligand and neuronal Notch receptor, the substrate for Fng-mediated O-glycosylation, also negatively regulate dendrite growth. Fng inhibits actin dynamics in dendrites, linking dendritic branch retraction to suppression of the C4da-mediated thermal nociception response in late larval stages. Thus, Fng-positive GOPs function in dendrite retraction, which would add another function to the of GOPs in dendrite arborization.

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