| Literature DB >> 33357422 |
José Wojnacki1, Sébastien Nola1, Philippe Bun2, Béatrice Cholley1, Francesca Filippini1, Mary T Pressé1, Joanna Lipecka3, Sin Man Lam4, Julie N'guyen2, Axelle Simon1, Amine Ouslimani1, Guanghou Shui4, Claudio Marcelo Fader5, Maria Isabel Colombo5, Ida Chiara Guerrera3, Thierry Galli6.
Abstract
VAMP7 is involved in autophagy and in exocytosis-mediated neurite growth, two yet unconnected cellular pathways. Here, we find that nutrient restriction and activation of autophagy stimulate axonal growth, while autophagy inhibition leads to loss of neuronal polarity. VAMP7 knockout (KO) neuronal cells show impaired neurite growth, whereas this process is increased in autophagy-null ATG5 KO cells. We find that endoplasmic reticulum (ER)-phagy-related LC3-interacting-region-containing proteins Atlastin 3 and Reticulon 3 (RTN3) are more abundant in autophagy-related protein ATG5 KO and less abundant in VAMP7 KO secretomes. Treatment of neuronal cells with ATG5 or VAMP7 KO conditioned medium does not recapitulate the effect of these KOs on neurite growth. A nanobody directed against VAMP7 inhibits axonal overgrowth induced by nutrient restriction. Furthermore, expression of the inhibitory Longin domain of VAMP7 impairs the subcellular localization of RTN3 in neurons. We propose that VAMP7-dependent secretion of RTN3 regulates neurite growth.Entities:
Keywords: autophagy, ER-phagy, secretion, neuron, development, SNARE, VAMP7, ATG5, RTN3, ATL3
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Year: 2020 PMID: 33357422 DOI: 10.1016/j.celrep.2020.108536
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423