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PLD2 forms a functional complex with mTOR/raptor to transduce mitogenic signals SCIE SCOPUS

Title
PLD2 forms a functional complex with mTOR/raptor to transduce mitogenic signals
Authors
Ha, SHKim, DHKim, ISKim, JHLee, MNLee, HJKim, JHJang, SKSuh, PGRyu, SH
Date Issued
2006-12
Publisher
ELSEVIER SCIENCE INC
Abstract
Mammalian target-of-rapamycin (mTOR), which is a master controller of cell growth, senses a mitogenic signal in part through the lipid second messenger phosphatidic acid (PA), generated by phospholipase D (PLD). To understand further which isozymes of PLD are involved in this process, we compared the effect of PLD isozymes on mTOR activation. We found that PLD2 has an essential role in mitogen-induced mTOR activation as the siRNA-mediated knockdown of PLD2, not of PLD I, profoundly reduced the phosphorylations of S6K1 and 4EBP1, well-known mTOR effectors. Furthermore, exogenous PA-induced mTOR activation was abrogated by PLD2 knockdown, but not by PLD I knockdown. This abrogation was found to be the result of complex formation between PLD2 and mTOR/raptor. PLD2 possesses a TOS-like motif (Plie-Ght-Val-Gin-Val, a.a. 265269), through which it interacts with raptor independently of the other TOS motif-containing proteins, S6K1 and 4EBP1. PLD2-dependent mTOR activation appears to require PLD2 binding to mTOR/raptor with lipase activity, since lipase-inactive PLD2 cannot trigger mTOR activation despite its ability to interact with mTOR/raptor. Abrogation of mitogen-dependent mTOR activation by PLD2 knockdown was rescued only by wild type PLD2, but not by raptor binding-deficient and lipase-inactive PLD2. Our results demonstrate the importance of localized PA generation for the mitogen-induced activation of mTOR, which is achieved by a specific interaction between PLD2 and mTOR/raptor. (c) 2006 Elsevier Inc. All rights reserved.
Keywords
PLD2; mTOR; raptor; complex formation; KINASE C-DELTA; PROTEIN-KINASE; TUBEROUS-SCLEROSIS; PHOSPHOLIPASE D1; MAMMALIAN TARGET; RAPAMYCIN MTOR; CELL-GROWTH; BINDING PARTNER; HOMOLOGY DOMAIN; RHEB BINDS
URI
https://oasis.postech.ac.kr/handle/2014.oak/23709
DOI
10.1016/j.cellsig.2006.05.021
ISSN
0898-6568
Article Type
Article
Citation
CELLULAR SIGNALLING, vol. 18, no. 12, page. 2283 - 2291, 2006-12
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류성호RYU, SUNG HO
Dept of Life Sciences
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