Premium
Ral GTP ase and the exocyst regulate autophagy in a tissue‐specific manner
Author(s) -
Tracy Kirsten,
Velentzas Panagiotis D,
Baehrecke Eric H
Publication year - 2016
Publication title -
embo reports
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 4.584
H-Index - 184
eISSN - 1469-3178
pISSN - 1469-221X
DOI - 10.15252/embr.201541283
Subject(s) - exocyst , microbiology and biotechnology , autophagy , gtp' , biology , chemistry , biochemistry , exocytosis , apoptosis , enzyme , secretion
Autophagy traffics cellular components to the lysosome for degradation. Ral GTP ase and the exocyst have been implicated in the regulation of stress‐induced autophagy, but it is unclear whether they are global regulators of this process. Here, we investigate Ral function in different cellular contexts in Drosophila and find that it is required for autophagy during developmentally regulated cell death in salivary glands, but does not affect starvation‐induced autophagy in the fat body. Furthermore, knockdown of exocyst subunits has a similar effect, preventing autophagy in dying cells but not in cells of starved animals. Notch activity is elevated in dying salivary glands, this change in Notch signaling is influenced by Ral, and decreased Notch function influences autophagy. These data indicate that Ral and the exocyst regulate autophagy in a context‐dependent manner, and that in dying salivary glands, Ral mediates autophagy, at least in part, by regulation of Notch.