INVOLVEMENT OF RAL GTPASE IN V-SRC-INDUCED PHOSPHOLIPASE-D ACTIVATION

被引：250

作者：

JIANG, H

LUO, JQ

URANO, T

FRANKEL, P

LU, ZM

FOSTER, DA

FEIG, LA

机构：

[1] CUNY HUNTER COLL,INST BIOMOLEC STRUCT & FUNCT,NEW YORK,NY 10021

[2] CUNY HUNTER COLL,DEPT SCI BIOL,NEW YORK,NY 10021

[3] TUFTS UNIV,SCH MED,DEPT BIOCHEM,BOSTON,MA 02111

来源：

NATURE | 1995年 / 378卷 / 6555期

关键词：

D O I：

10.1038/378409a0

中图分类号：

O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

AN early response to the tyrosine kinase activity of v-Src is an increase in phospholipase D (PLD) activity(1), which leads to the generation of biologically active lipid second messengers, including phosphatidic acid, lysophosphatidic acid and diacylglycerol(2). We have recently demonstrated that v-Src-induced PLD activity is mediated by Ras(3), although Ras involvement was indirect, requiring a cytosolic factor for PLD activation(3). Ras interacts with(4-6) and activates Ral-GDS(13), the exchange factor responsible for the activation of Ral GTPases. Here we report that this newly identified Ras/Ral signalling pathway mediates PLD activation by v-Src. PLD activity could be precipitated from v-Src-transformed cell lysates with immobilized RalA protein and with an anti-Ral antibody. A mutation to the region of RalA analogous to the 'effector domain' of Ras did not reduce the ability of RalA to complex with PLD, although deletion of a Ral-specific amino-terminal region did. Overexpression of RalA potentiated PLD activation by v-Src, and expression of dominant negative RalA mutants inhibited both v-Src- and v-Ras-induced PLD activity. Thus RalA is involved in the tyrosine kinase activation of PLD through its unique N terminus, and that PLD is a downstream target of a Ras/Ral GTPase cascade.

引用

页码：409 / 412

页数：4

共 25 条

[1] BOWMAN EP, 1993, J BIOL CHEM, V268, P21509
[2] ADP-RIBOSYLATION FACTOR, A SMALL GTP-DEPENDENT REGULATORY PROTEIN, STIMULATES PHOSPHOLIPASE-D ACTIVITY
BROWN, HA
GUTOWSKI, S
MOOMAW, CR
SLAUGHTER, C
STERNWEIS, PC
[J]. CELL, 1993, 75 (06) : 1137 - 1144
[3] CAMERO A, 1994, ONCOGENE, V9, P1387
[4] CANTOR SB, 1995, MOL CELL BIOL, V15, P4578
[5] PHOSPHOLIPASE-D - A DOWNSTREAM EFFECTOR OF ARF IN GRANULOCYTES
COCKCROFT, S
THOMAS, GMH
FENSOME, A
GENY, B
CUNNINGHAM, E
GOUT, I
HILES, I
TOTTY, NF
TRUONG, Q
HSUAN, JJ
[J]. SCIENCE, 1994, 263 (5146) : 523 - 526
[6] EMKEY R, 1991, J BIOL CHEM, V266, P9703
[7] DOMINANT INHIBITORY MUTATIONS IN THE MG-2+-BINDING SITE OF RASH PREVENT ITS ACTIVATION BY GTP
FARNSWORTH, CL
FEIG, LA
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1991, 11 (10) : 4822 - 4829
[8] INHIBITION OF NIH-3T3 CELL-PROLIFERATION BY A MUTANT RAS PROTEIN WITH PREFERENTIAL AFFINITY FOR GDP
FEIG, LA
COOPER, GM
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1988, 8 (08) : 3235 - 3243
[9] INTRACELLULAR SIGNALING MEDIATED BY PROTEIN-TYROSINE KINASES - NETWORKING THROUGH PHOSPHOLIPID-METABOLISM
FOSTER, DA
[J]. CELLULAR SIGNALLING, 1993, 5 (04) : 389 - 399
[10] MONOCLONAL-ANTIBODIES TO THE P21 PRODUCTS OF THE TRANSFORMING GENE OF HARVEY MURINE SARCOMA-VIRUS AND OF THE CELLULAR RAS GENE FAMILY
FURTH, ME
DAVIS, LJ
FLEURDELYS, B
SCOLNICK, EM
[J]. JOURNAL OF VIROLOGY, 1982, 43 (01) : 294 - 304

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