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

Michaud, Neil R.; Fabian, John R.; Mathes, K D; Morrison, Deborah K.

doi:10.1128/mcb.15.6.3390

Cited by 212 publications

(211 citation statements)

References 48 publications

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“…mean, n=6) are given relative to a control sample (100%) that was incubated without peptide. The results have been pooled from three experiments The e ect of PS/Ca is also quite distinct from the two documented e ects that detergents have on Raf-1: RIPA bu er displaces 14-3-3 from Raf-1 without a ecting kinase activity (Michaud et al, 1995), whereas Empigen-BB displaces 14-3-3 and inactivates Raf-1 (Thorson et al, 1998). Clearly the e ect of PS/ Ca mimics neither of these.…”

Section: Discussionmentioning

confidence: 92%

“…The isolated RafCRD binds to 14-3-3 in vitro (Clark et al, 1997) and C165S,C168S mutations that disrupt the zinc ®nger within the RafCRD (RafCC/SS), have been reported to abrogate all binding of 14-3-3 to full-length Raf-1 in vitro (Michaud et al, 1995). However, when anti-Flag immunoprecipitates prepared from the NP-40 soluble fraction of COS cells expressing FlagRafCC/SS were immunoblotted for 14-3-3 we found a substantial amount of 14-3-3 was present, comparable to the amount of 14-3-3 in immunoprecipitates prepared from cells expressing wild type FlagRaf (Figure 1).…”

Section: Resultsmentioning

confidence: 99%

“…These data indicate that an intact zinc ®nger is required for some aspect of Raf-1 activation that occurs at the plasma membrane. In addition to Ras, two other CRD ligands have been identi®ed: 14-3-3 proteins, which bind to two phosphoserine-containing sites on Raf-1 (Muslin et al, 1996) as well as to the RafCRD (Michaud et al, 1995;Clark et al, 1997), and phosphatidylserine (PS), a plasma membrane inner lea¯et phospholipid (Ghosh et al, 1994) that can activate Raf-1 in vitro (Force et al, 1994).…”

Section: Introductionmentioning

confidence: 99%

“…The e ect of 14-3-3 proteins on the kinase activity of Raf-1 is contentious, since in vitro they have been reported to either have no e ect on Raf-1 kinase activity (Fu et al, 1994;Michaud et al, 1995;Suen et al, 1995) or to activate Raf-1 (Fantl et al, 1994;Freed et al, 1994;Irie et al, 1994;Li et al, 1995). Genetic studies have identi®ed dominant negative 14-3-3 mutants that can inhibit signalling downstream of Ras and Raf-1 (Chang and Rubin, 1997) and have con®rmed that 14-3-3 proteins are required for Rasmediated Raf-1 activation (Kockel et al, 1997).…”

Section: Introductionmentioning

confidence: 99%

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Interactions of c-Raf-1 with phosphatidylserine and 14-3-3

et al. 1999

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Section: Discussionmentioning

confidence: 92%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Interactions of c-Raf-1 with phosphatidylserine and 14-3-3

et al. 1999

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“…This family of ubiquitously expressed, highly conserved proteins can exist as dimers and are known to complex with a variety of proteins (BCR, cdc25, A20, PKC) suggesting that they may act as an adaptor proteins (Braselmann and McCormick, 1995;Conklin et al, 1995;Vincenz and Dixit, 1996). The role of 14-3-3 in Raf-1 regulation remains controversial (Michaud et al, 1995;Suen et al, 1995;Li et al, 1995;Irie et al, 1994;Freed et al, 1994;Fantl et al, 1994;Chang and Rubin, 1997;Luo et al, 1996;Braselmann and McCormick, 1995;Shimizu et al, 1994). This may be due, at least in part, to the complex nature of the Raf-1/14-3-3 interaction which involves multiple binding sites, including the Raf-1 CRD and two sites containing a phospho-serine consensus sequence for 14-3-3 at positions 259 and 621 of Raf-1 (Clark et al, 1997b;Li et al, 1993).…”

Section: Introductionmentioning

confidence: 99%

Increasing complexity of Ras signaling

et al. 1998

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The initial discovery that ras genes endowed retroviruses with potent carcinogenic properties and the subsequent determination that mutated ras genes were present in a wide variety of human cancers, prompted a strong suspicion that the growth-promoting actions of mutated Ras proteins contribute to their aberrant regulation of growth stimulatory signaling pathways. In 1993, a remarkable convergence of experimental observations from genetic analyses of Drosophila, S. cerevisiae and C. elegans as well as biochemical and biological studies in mammalian cells came together to de®ne a clear role for Ras in signal transduction. What emerged was an elegant linear signaling pathway where Ras functions as a relay switch that is positioned downstream of cell surface receptor tyrosine kinases and upstream of a cytoplasmic cascade of kinases that included the mitogen-activated protein kinases (MAPKs). Activated MAPKs in turn regulated the activities of nuclear transcription factors. Thus, a signaling cascade where every component between the cell surface and the nucleus was de®ned and conserved in worms,¯ies and man. This was a remarkable achievement in our e orts to appreciate how the aberrant function of Ras proteins may contribute to the malignant growth properties of the cancer cell. However, the identi®cation of this pathway has proven to be just the beginning, rather than the culmination, of our understanding of Ras in signal transduction. Instead, we now appreciate that this simple linear pathway represents but a minor component of a very complex signaling circuitry. Ras signaling has emerged to involve a complex array of signaling pathways, where cross-talk, feedback loops, branch points and multi-component signaling complexes are recurring themes. The simplest concept of a signaling cascade, where each component simply relays the same message to the next, is clearly not the case. In this review, we summarize our current understanding of Ras signal transduction with an emphasis on new complexities associated with the recognition and/or activation of cellular e ectors, and the diverse array of signaling pathways mediated by interaction between Ras and Ras-subfamily proteins with multiple e ectors.

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Developmental regulation of 14-3-3 ε isoform in rat heart

Luk¹,

Ngai²,

Tsui³

et al. 1998

J. Cell. Biochem.

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Human heart cDNA sequencing yielded a cDNA clone that is similar in DNA and amino acid sequences to that of mouse 14-3-3 epsilon isoform. The 6xHis-tagged H1433 epsilon recombinant protein was expressed in Escherichia coli and its size was approximately 30 kDa. From Northern blot results with human multiple tissues, human skeletal muscle was found to have the highest level of h1433 epsilon mRNA expression, whereas Northern blots of human cancer cell lines detected the highest mRNA level of h1433 epsilon in colorectal adenocarcinoma SW480. The protein expression level of h1433 epsilon and Raf-1 is found to be regulated coordinately during rat heart development, and their protein expression was highest from 14.5 to 16.5 days postcoitum.

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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

Cited by 212 publications

References 48 publications

Interactions of c-Raf-1 with phosphatidylserine and 14-3-3

Interactions of c-Raf-1 with phosphatidylserine and 14-3-3

Increasing complexity of Ras signaling

Developmental regulation of 14-3-3 ε isoform in rat heart

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