TY - JOUR
T1 - RalB and the exocyst mediate the cellular starvation response by direct activation of autophagosome assembly
AU - Bodemann, Brian O.
AU - Orvedahl, Anthony
AU - Cheng, Tzuling
AU - Ram, Rosalyn R.
AU - Ou, Yi Hung
AU - Formstecher, Etienne
AU - Maiti, Mekhala
AU - Hazelett, C. Clayton
AU - Wauson, Eric M.
AU - Balakireva, Maria
AU - Camonis, Jacques H.
AU - Yeaman, Charles
AU - Levine, Beth
AU - White, Michael A.
N1 - Funding Information:
We thank Noboru Mishuzima for GFP-Atg5 and GFP-LC3, Zhenyu Yue for Flag-ATG14L and Flag-RUBICON, and Noriko Okazaki for HA-ULK1 and HA-ULK1(K46N). We thank members of the White and Levine labs for productive discussions. We thank Melanie Cobb for helpful discussion and assistance with kinase assays. This work was supported by grants from the National Institutes of Health (CA71443 and CA129451 to M.W. and CA84254 and CA109618 to B.L.), ARC4845 and GenHomme Network Grant 02490-6088 to J.C., and the Welch Foundation (I-1414 to M.W.). B.B. was supported by DOD Award Number W81XWH-06-1-0749. R.R. was supported by T32GM008203. Y.O. was supported by CPRIT RP101496.
PY - 2011/1/21
Y1 - 2011/1/21
N2 - The study of macroautophagy in mammalian cells has described induction, vesicle nucleation, and membrane elongation complexes as key signaling intermediates driving autophagosome biogenesis. How these components are recruited to nascent autophagosomes is poorly understood, and although much is known about signaling mechanisms that restrain autophagy, the nature of positive inductive signals that can promote autophagy remain cryptic. We find that the Ras-like small G protein, RalB, is localized to nascent autophagosomes and is activated on nutrient deprivation. RalB and its effector Exo84 are required for nutrient starvation-induced autophagocytosis, and RalB activation is sufficient to promote autophagosome formation. Through direct binding to Exo84, RalB induces the assembly of catalytically active ULK1 and Beclin1-VPS34 complexes on the exocyst, which are required for isolation membrane formation and maturation. Thus, RalB signaling is a primary adaptive response to nutrient limitation that directly engages autophagocytosis through mobilization of the core vesicle nucleation machinery.
AB - The study of macroautophagy in mammalian cells has described induction, vesicle nucleation, and membrane elongation complexes as key signaling intermediates driving autophagosome biogenesis. How these components are recruited to nascent autophagosomes is poorly understood, and although much is known about signaling mechanisms that restrain autophagy, the nature of positive inductive signals that can promote autophagy remain cryptic. We find that the Ras-like small G protein, RalB, is localized to nascent autophagosomes and is activated on nutrient deprivation. RalB and its effector Exo84 are required for nutrient starvation-induced autophagocytosis, and RalB activation is sufficient to promote autophagosome formation. Through direct binding to Exo84, RalB induces the assembly of catalytically active ULK1 and Beclin1-VPS34 complexes on the exocyst, which are required for isolation membrane formation and maturation. Thus, RalB signaling is a primary adaptive response to nutrient limitation that directly engages autophagocytosis through mobilization of the core vesicle nucleation machinery.
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U2 - 10.1016/j.cell.2010.12.018
DO - 10.1016/j.cell.2010.12.018
M3 - Article
C2 - 21241894
AN - SCOPUS:78651488777
SN - 0092-8674
VL - 144
SP - 253
EP - 267
JO - Cell
JF - Cell
IS - 2
ER -