Aberrant Ras regulation and reduced p190 tyrosine phosphorylation in cells lacking p120-Gap

被引:66
作者
vanderGeer, P
Henkemeyer, M
Jacks, T
Pawson, T
机构
[1] MT SINAI HOSP,SAMUEL LUNENFELD RES INST,PROGRAMME MOL BIOL & CANC,TORONTO,ON M5G 1X5,CANADA
[2] UNIV TORONTO,DEPT MOL & MED GENET,TORONTO,ON M5S 1A8,CANADA
[3] MIT,CTR CANC RES,CAMBRIDGE,MA 02139
关键词
GTPASE-ACTIVATING PROTEIN; NEUROFIBROMATOSIS TYPE-1 GENE; GROWTH-FACTOR RECEPTORS; GAP-ASSOCIATED PROTEINS; GUANINE-NUCLEOTIDE EXCHANGE; C-TERMINAL DOMAIN; FACTOR-I RECEPTOR; SH2; DOMAINS; PHOSPHOLIPID-BINDING; SIGNAL-TRANSDUCTION;
D O I
10.1128/MCB.17.4.1840
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The Ras guanine nucleotide-binding protein functions as a molecular switch in signalling downstream of protein-tyrosine kinases. Ras is activated by exchange of GDP for GTP and is turned off by hydrolysis of bound GTP to GDP. Ras itself has a low intrinsic GTPase activity that can be stimulated by GTPase-activating proteins (GAPs), including p120-Gap and neurofibromin. These GAPs possess a common catalytic domain but contain distinct regulatory elements that may couple different external signals to control of the Ras pathway. p120-Gap, for example, has two N-terminal SH2 domains that directly recognize phosphotyrosine motifs on activated growth factor receptors and cytoplasmic phosphoproteins. To analyze the role of p120-Gap in Ras regulation in vivo, we have used fibroblasts derived from mouse embryos with a null mutation in the gene for p120-Gap (Gap). Platelet-derived growth factor stimulation of Gap(-/-) Cells led to an abnormally large increase in the level of Ras-GTP and in the duration of mitogen-activated protein (MAP) kinase activation compared with wild-type cells, suggesting that p120-Gap is specifically activated following growth factor stimulation. Induction of DNA synthesis in response to platelet-derived growth factor and morphological transformation by the v-src and EJ-ras oncogenes were not significantly affected by the absence of p120-Gap. However, we found that normal tyrosine phosphorylation of p190-rhoGap, a cytoplasmic protein that associates with the p120-Gap SH2 domains, was dependent on the presence of p120-Gap. Our results suggest that p120-Gap has specific functions in downregulating the Ras/MAP kinase pathway following growth factor stimulation, and in modulating the phosphorylation of p190-rhoGap, but is not required for mitogenic signalling.
引用
收藏
页码:1840 / 1847
页数:8
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