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Literature DB >> 7760835

14-3-3 is not essential for Raf-1 function: identification of Raf-1 proteins that are biologically activated in a 14-3-3- and Ras-independent manner.

N R Michaud¹, J R Fabian, K D Mathes, D K Morrison.

Abstract

Recent reports have demonstrated the in vivo association of Raf-1 with members of the 14-3-3 protein family. To address the significance of the Raf-1-14-3-3 interaction, we investigated the enzymatic activity and biological function of Raf-1 in the presence and absence of associated 14-3-3. The interaction between these two molecules was disrupted in vivo and in vitro with a combination of molecular and biochemical techniques. Biochemical studies demonstrated that the enzymatic activities of Raf-1 were equivalent in the presence and absence of 14-3-3. Furthermore, mixing of purified Raf-1 and 14-3-3 in vitro was not sufficient to activate Raf-1. With a molecular approach, Cys-165 and Cys-168 as well as Ser-259 were identified as residues of Raf-1 required for the interaction with 14-3-3. Cys-165 and Cys-168 are located within the conserved cysteine-rich region of the CR1 domain, and Ser-259 is a conserved site of serine phosphorylation found within the CR2 domain. Mutation of either Cys-165 and Cys-168 or Ser-259 prevented the stable interaction of Raf-1 with 14-3-3 in vivo. Consistent with the model in which a site of serine phosphorylation is involved in the Raf-1-14-3-3 interaction, dephosphorylated Raf-1 was unable to associate with 14-3-3 in vitro. Phosphorylation may represent a general mechanism mediating 14-3-3 binding, because dephosphorylation of the Bcr kinase (known to interact with 14-3-3) also eliminated its association with 14-3-3. Finally, mutant Raf-1 proteins unable to stably interact with 14-3-3 exhibited enhanced enzymatic activity in human 293 cells and Xenopus oocytes and were biologically activated, as demonstrated by their ability to induced meiotic maturation of Xenopus oocytes. However, in contrast to wild-type Raf-1, activation of these mutants was independent of Ras. Our results therefore indicate that interaction with 14-3-3 is not essential for Raf-1 function.

Entities: Chemical Gene Species

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Year: 1995 PMID： 7760835 PMCID： PMC230573 DOI： 10.1128/MCB.15.6.3390

Source DB: PubMed Journal: Mol Cell Biol ISSN： 0270-7306 Impact factor: 4.272

49 in total

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Authors: U R Rapp
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Review 3. The Raf-1 kinase as a transducer of mitogenic signals.

Authors: D K Morrison
Journal: Cancer Cells Date: 1990-12

4. Requirement for Ras in Raf activation is overcome by targeting Raf to the plasma membrane.

Authors: S J Leevers; H F Paterson; C J Marshall
Journal: Nature Date: 1994-06-02 Impact factor: 49.962

Review 5. 14-3-3: modulators of signaling proteins?

Authors: D Morrison
Journal: Science Date: 1994-10-07 Impact factor: 47.728

6. Expression, purification and characterization of recombinant mitogen-activated protein kinase kinases.

Authors: P Dent; Y H Chow; J Wu; D K Morrison; R Jove; T W Sturgill
Journal: Biochem J Date: 1994-10-01 Impact factor: 3.857

7. The eukaryotic host factor that activates exoenzyme S of Pseudomonas aeruginosa is a member of the 14-3-3 protein family.

Authors: H Fu; J Coburn; R J Collier
Journal: Proc Natl Acad Sci U S A Date: 1993-03-15 Impact factor: 11.205

8. Direct interaction of Ras and the amino-terminal region of Raf-1 in vitro.

Authors: P H Warne; P R Viciana; J Downward
Journal: Nature Date: 1993-07-22 Impact factor: 49.962

9. A protein kinase similar to MAP kinase activator acts downstream of the raf kinase in Drosophila.

Authors: L Tsuda; Y H Inoue; M A Yoo; M Mizuno; M Hata; Y M Lim; T Adachi-Yamada; H Ryo; Y Masamune; Y Nishida
Journal: Cell Date: 1993-02-12 Impact factor: 41.582

10. Raf functions downstream of Ras1 in the Sevenless signal transduction pathway.

Authors: B Dickson; F Sprenger; D Morrison; E Hafen
Journal: Nature Date: 1992-12-10 Impact factor: 49.962

61 in total

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Journal: Mol Cell Biol Date: 1999-09 Impact factor: 4.272

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Review 9. The 14-3-3 proteins: gene, gene expression, and function.

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Review 10. Mechanistic principles of RAF kinase signaling.

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