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Literature DB >> 9889195

PI 3-kinase gamma and protein kinase C-zeta mediate RAS-independent activation of MAP kinase by a Gi protein-coupled receptor.

H Takeda¹, T Matozaki, T Takada, T Noguchi, T Yamao, M Tsuda, F Ochi, K Fukunaga, K Inagaki, M Kasuga.

Abstract

Receptors coupled to the inhibitory G protein Gi, such as that for lysophosphatidic acid (LPA), have been shown to activate MAP kinase through a RAS-dependent pathway. However, LPA (but not insulin) has now been shown to activate MAP kinase in a RAS-independent manner in CHO cells that overexpress a dominant-negative mutant of the guanine nucleotide exchange protein SOS (CHO-DeltaSOS cells). LPA also induced the activation of MAP kinase kinase (MEK), but not that of RAF1, in CHO-DeltaSOS cells. The RAS-independent activation of MAP kinase by LPA was blocked by inhibitors of phosphatidylinositol 3-kinase (PI3K) or by overexpression of a dominant-negative mutant of the gamma isoform of PI3K. Furthermore, LPA induced the activation of the atypical zeta isoform of protein kinase C (PKC-zeta) in CHO-DeltaSOS cells in a manner that was sensitive to wortmannin or to the dominant-negative mutant of PI3Kgamma, and overexpression of a dominant-negative mutant of PKC-zeta inhibited LPA-induced activation of MAP kinase. These observations indicate that Gi protein-coupled receptors induce activation of MEK and MAP kinase through a RAS-independent pathway that involves PI3Kgamma-dependent activation of atypical PKC-zeta.

Entities: Chemical Disease Gene

Mesh：

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Year: 1999 PMID： 9889195 PMCID： PMC1171133 DOI： 10.1093/emboj/18.2.386

Source DB: PubMed Journal: EMBO J ISSN： 0261-4189 Impact factor: 11.598

44 in total

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Journal: Curr Opin Cell Biol Date: 1995-04 Impact factor: 8.382

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27 in total

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8. Role of atypical protein kinase C in estradiol-triggered G1/S progression of MCF-7 cells.

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Review 9. Mechanisms linking obesity and cancer.

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10. Phosphorylation of adaptor protein-2 mu2 is essential for Na+,K+-ATPase endocytosis in response to either G protein-coupled receptor or reactive oxygen species.

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