Differential Raf requirement for activation of mitogen-activated protein kinase by growth factors, phorbol esters, and calcium.

T.S Chao,D.A Foster,U.R Rapp,M.R Rosner

doi:10.1016/s0021-9258(17)37289-7

T.S Chao, D.A Foster + Show 2 more

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https://doi.org/10.1016/s0021-9258(17)37289-7

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Journal: The Journal of biological chemistry	Publication Date: Mar 1, 1994
Citations: 152	License type: cc-by

Affiliation: May Institute

Abstract

Although a pathway that requires sequential activation of Ras, Raf, and MAP kinase kinase has been proposed as the major mechanism for stimulation of mitogen-activated protein kinase (MAP kinase), alternative pathways also exist. A wide variety of extracellular stimuli have been shown to activate MAP kinase; however, the precise mechanisms by which these stimuli mediate the signaling events have not been elucidated. Using a Balb/c-derived cell line expressing a dominant-negative mutant of Raf, we determined whether Raf is required for the activation of MAP kinase by growth factors, phorbol esters, and calcium. Insulin-like growth factor I (IGF-I), epidermal growth factor (EGF), and phorbol 12,13-dibutyrate activated Ras in both mutant and control cells. However, stimulation of MAP kinase by IGF-I was nearly abolished in the dominant-negative Raf mutant. Stimulation of MAP kinase by the Ca2+ mobilizer thapsigargin was also inhibited in the presence of the Raf mutant. In contrast, EGF and phorbol 12,13-dibutyrate remained potent stimulators of MAP kinase in the dominant-negative Raf cells. The activation of MAP kinase by these stimuli can be further distinguished by differential requirements for Ca2+ and protein kinase C. These results suggest that Raf is required for the activation of MAP kinase by IGF-I and calcium, whereas EGF and possibly phorbol esters may employ alternative Raf-independent pathways for MAP kinase activation.

Highlights

A pathway that requires sequential activa- ated protein-2 have been docution of Ras, Raf, and MAP kinase kinase has been pro- mented
The ubiquitous distribution as well as diverse function posed as the major mechanism for stimulationof mito- of its substrates underline the significance of MAP kinase in gen-activated protein kinase( M A P kinase), alternative cellular signal transduction
Insulin-like growCath2+(81,can be distinguished by a requirement for intracellufactor I (IGF-I),epidermalgrowthfactor(EGF),and lar Ca2+(2); the stimulationby thrombin, but not basic fibrophorbol 12,13-dibutyrate activatedRas in both mutant blast growth factor, is sensitive to pertussitsoxin inhibition (9); and control cells

Summary

EXPERIMENTAL PROCEDURES

Materials-EGF (receptor grade) was purchased from Biomedical Technologies(Stoughton, MA). IGF-I (0.5-10 ng/ml) confirmed that IGF-I-induced activation of MAP kinase was abolished in the R1 cells (data not shown) These results suggest that the IGF-I signaling pathway involves sequential activation of Ras and Raf. Asdescribedpreviously for humandiploidfibroblasts(2), Time (min) o 2 5 IO 3060 thapsigargin activated MAP kinase in the murine fibroblast MNC cells (Fig. 2C). Like EGF, PDBu activated M A P kinase to comparable levels in both the R1 mutant and the control MNC cells (Fig. 2 E ). These results suggest that PDBu may use an alternative pathway for activationof M A P kinase.

Although we cannot completely rule out the possibility that

Possible Mechanismsfor Activation of MAP Kinase by EGE

Downstreamslgnallng events