A BRANCHED SIGNALING PATHWAY FOR NERVE GROWTH-FACTOR IS REVEALED BY SRC-MEDIATED, RAS-MEDIATED, AND RAF-MEDIATED GENE INDUCTIONS

被引:139
作者
DARCANGELO, G [1 ]
HALEGOUA, S [1 ]
机构
[1] SUNY, DEPT NEUROBIOL & BEHAV, STONY BROOK, NY 11794 USA
来源
MOLECULAR AND CELLULAR BIOLOGY | 1993年 / 13卷 / 06期
关键词
D O I
10.1128/MCB.13.6.3146
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
A myriad of gene induction events underlie nerve growth factor (NGF)-induced differentiation of PC12 cells. To dissect the signal transduction pathways which lead to NGF actions, we have assessed the relative roles of NGF receptor, Src, Ras, and Raf activities in mediating specific gene inductions. We have used the PC12 cell line as well as sublines which inducibly express activated forms of either Src, Ras, or Raf or a dominant inhibitory form of Ras (p21N17 Ras) to study the expression of multiple NGF-inducible mRNAs. The NGF induction of NGFI-A, transin, and VGF mRNAs was mimicked by activated forms of Src, Ras, or Raf and was blocked by p21N17 Ras. The NGF induction of SCG10 mRNA was mimicked only by activated Src and Ras and was blocked by p21N17 Ras, while the induction of Thy-1 mRNA was mimicked only by activated Src and was not blocked by p21N17 Ras. The NGF induction of mRNAs for two sodium channel types was neither mimicked by any activated oncoprotein nor blocked by p21N17 Ras. From these and previous results, we suggest a model in which a linear order of NGF receptor, Src, Ras, and Raf activities is used by NGF to elicit gene inductions. These signaling components define branchpoints in the pathway to specific gene induction events, providing a mechanism for generating a host of diverse NGF actions.
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页码:3146 / 3155
页数:10
相关论文
共 60 条
[1]   DIFFERENTIATION OF PC12 PHEOCHROMOCYTOMA CELLS INDUCED BY V-SRC ONCOGENE [J].
ALEMA, S ;
CASALBORE, P ;
AGOSTINI, E ;
TATO, F .
NATURE, 1985, 316 (6028) :557-559
[2]   MICROINJECTION OF THE RAS ONCOGENE PROTEIN INTO PC12 CELLS INDUCES MORPHOLOGICAL-DIFFERENTIATION [J].
BARSAGI, D ;
FERAMISCO, JR .
CELL, 1985, 42 (03) :841-848
[3]   NERVE GROWTH-FACTOR RAPIDLY REGULATES VGF GENE-TRANSCRIPTION THROUGH CYCLOHEXIMIDE SENSITIVE AND INSENSITIVE PATHWAYS [J].
BAYBIS, M ;
SALTON, SRJ .
FEBS LETTERS, 1992, 308 (02) :202-206
[4]   A METHOD FOR ISOLATION OF INTACT, TRANSLATIONALLY ACTIVE RIBONUCLEIC-ACID [J].
CATHALA, G ;
SAVOURET, JF ;
MENDEZ, B ;
WEST, BL ;
KARIN, M ;
MARTIAL, JA ;
BAXTER, JD .
DNA-A JOURNAL OF MOLECULAR & CELLULAR BIOLOGY, 1983, 2 (04) :329-335
[5]   STRUCTURE OF THE NGFI-A GENE AND DETECTION OF UPSTREAM SEQUENCES RESPONSIBLE FOR ITS TRANSCRIPTIONAL INDUCTION BY NERVE GROWTH-FACTOR [J].
CHANGELIAN, PS ;
FENG, P ;
KING, TC ;
MILBRANDT, J .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1989, 86 (01) :377-381
[6]   GROWTH-FACTOR SIGNALING - WHERE IS THE SPECIFICITY [J].
CHAO, MV .
CELL, 1992, 68 (06) :995-997
[7]   MODULATION OF SODIUM-CHANNEL MESSENGER-RNA LEVELS IN RAT SKELETAL-MUSCLE [J].
COOPERMAN, SS ;
GRUBMAN, SA ;
BARCHI, RL ;
GOODMAN, RH ;
MANDEL, G .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1987, 84 (23) :8721-8725
[8]   P1B15 - A CDNA CLONE OF THE RAT MESSENGER-RNA ENCODING CYCLOPHILIN [J].
DANIELSON, PE ;
FORSSPETTER, S ;
BROW, MA ;
CALAVETTA, L ;
DOUGLASS, J ;
MILNER, RJ ;
SUTCLIFFE, JG .
DNA-A JOURNAL OF MOLECULAR & CELLULAR BIOLOGY, 1988, 7 (04) :261-267
[9]  
DARCANGELO G, UNPUB
[10]   BIOLOGICAL AND BIOCHEMICAL-PROPERTIES OF HUMAN RASH GENES MUTATED AT CODON-61 [J].
DER, CJ ;
FINKEL, T ;
COOPER, GM .
CELL, 1986, 44 (01) :167-176
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