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Query: EC:2.7.10.1 (
ERK
)
95,504
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Raf kinase inhibitor protein
(
RKIP
) is a member of the
phosphatidylethanolamine-binding protein
(
PEBP
) family.
RKIP
plays a pivotal modulatory role in several protein kinase signaling cascades.
RKIP
binds inhibits Raf-1-mediated phosphorylation of MEK through binding to Raf-1. Protein kinase C (PKC) phosphorylates
RKIP
, resulting in release of Raf-1 and activation of MEK and
ERK
. The phosphorylated
RKIP
binds to and inhibits G-protein-coupled receptor kinase, resulting in sustained G-protein signaling. The regulatory role that
RKIP
has in cell signaling is reflected in its role in physiology and pathophysiology.
RKIP
is involved in neural development, cardiac function and spermatogenesis and appears to have serine protease activity. In addition to its roles in physiology, dysregulated
RKIP
expression has the potential to contribute to pathophysiological processes including Alzheimer's disease and diabetic nephropathy.
RKIP
has been shown to fit the criteria of being a metastasis suppressor gene, including having decreased expression in prostate cancer metastases and restoring
RKIP
expression in a prostate cancer cell line diminishes metastasis in a murine model. Clearly,
RKIP
has multiple molecular and cellular functions. In this review,
RKIP
's molecular roles in intracellular signaling, its physiological functions and its role in disease are described.
...
PMID:The role of Raf kinase inhibitor protein (RKIP) in health and disease. 1531
The acquisition of resistance to conventional therapies such as radiation and chemotherapeutic drugs remains the major obstacle in the successful treatment of cancer patients. Tumor cells acquire resistance to apoptotic stimuli and it has been demonstrated that conventional therapies exert their cytotoxic activities primarily by inducing apoptosis in the cells. Resistance to radiation and chemotherapeutic drugs has led to the development of immunotherapy and gene therapy approaches with the intent of overcoming resistance to drugs and radiation as well as enhancing the specificity to eliminate tumor cells. However, cytotoxic lymphocytes primarily kill by apoptosis and, therefore, drug-resistant tumor cells may also be cross-resistant to immunotherapy. To evade apoptosis, tumor cells have adopted various mechanisms that interfere with the apoptotic signaling pathways and promote constitutive activation of cellular proliferation and survival pathways. Thus, modifications of the antiapoptotic genes in cancer cells are warranted for the effectiveness of conventional therapies as well as novel immunotherapeutic approaches. Such modifications will avert the resistant phenotype of the tumor cells and will render them susceptible to apoptosis. Current studies, both in vitro and preclinically in vivo, have been aimed at the modification and regulation of expression of apoptosis-related gene products and their activities. A novel protein designated Raf-1 kinase inhibitor protein (RKIP) has been partially characterized. RKIP is a member of the
phosphatidylethanolamine-binding protein
family. RKIP has been shown to disrupt the Raf-1-MEK1/2 [mitogen-activated protein kinase-
ERK
(extracellular signal-regulated kinase) kinase-1/2]-ERK1/2 and NF-kappaB signaling pathways, via physical interaction with Raf-1-MEK1/2 and NF-kappaB-inducing kinase or transforming growth factor beta-activated kinase-1, respectively, thereby abrogating the survival and antiapoptotic properties of these signaling pathways. In addition, RKIP has been shown to act as a signal modifier that enhances receptor signaling by inhibiting G protein-coupled receptor kinase-2. By regulating cell signaling, growth, and survival through its expression and activity, RKIP is considered to play a pivotal role in cancer, regulating apoptosis induced by drugs or immune-mediated stimuli. Overexpression of RKIP sensitizes tumor cells to chemotherapeutic drug-induced apoptosis. Also, induction of RKIP by drugs or anti-receptor antibodies sensitizes cancer cells to drug-induced apoptosis. In this review, we discuss the discovery, structure, function, and significance of RKIP in cancer.
...
PMID:Raf-1 kinase inhibitor protein: structure, function, regulation of cell signaling, and pivotal role in apoptosis. 1532 91
The Raf-MEK-
ERK
protein kinase cascade is a highly conserved signaling pathway that is pivotal in relaying environmental cues from the cell surface to the nucleus. Three Raf isoforms, which share great sequence and structure similarities, have been identified in mammalian cells. We have previously identified
Raf kinase inhibitor protein
(
RKIP
) as a negative regulator of the Raf-MEK-
ERK
signaling pathway by specifically binding to the Raf-1 isoform. We show here that
RKIP
also antagonizes kinase activity of the B-Raf isoform. Yeast two-hybrid and coimmunoprecipitation experiments indicated that
RKIP
specifically interacted with B-Raf. Ectopic expression of
RKIP
antagonized the kinase activity of B-Raf. We showed that the effects of
RKIP
on B-Raf functions were independent of its known inhibitory action on Raf-1. The expression levels of
RKIP
in melanoma cancer cell lines are low relative to primary melanocytes. Forced expression of
RKIP
partially reverted the oncogenic B-Raf kinase-transformed melanoma cancer cell line SK-Mel-28. The low expression of
RKIP
and its antagonistic action on B-Raf suggests that
RKIP
may play an important role in melanoma turmorgenesis.
...
PMID:RKIP downregulates B-Raf kinase activity in melanoma cancer cells. 1578 37
Differential gene expression analysis of human blood monocytes has identified the
Raf kinase inhibitor protein
(
RKIP
) as a continuously upregulated gene in macrophage and dendritic cell maturation. Using realtime RT-PCR and Western blot analysis we were able to confirm the initial DNA-microarray findings of
RKIP
induction on mRNA and protein levels.
RKIP
upregulation in primary cells and overexpression in THP-1 cells did not alter
ERK
activity but strongly reduced the amount of the NFkappaB subunit p65 in the nucleus. mRNA levels and cell surface expression of maturation markers including the integrin CD11c and the scavenger receptor CD36 were significantly increased in
RKIP
transfected THP-1 cells. Our data show for the first time that
RKIP
is upregulated during macrophage and dendritic cell differentiation on mRNA and protein levels and we conclude that
RKIP
contributes to the monocytic differentiation process via inhibition of the NFkappaB signaling cascade independent from the canonical Ras/Raf/MEK/
ERK
pathway.
...
PMID:Induction of Raf kinase inhibitor protein contributes to macrophage differentiation. 1651 87
The
Raf kinase inhibitor protein
(
RKIP
) belongs to an evolutionarily conserved family of phosphatidylethanolamine-binding proteins (PEBPs), which have important functions as inhibitors of kinase signaling pathways and metastasis. Most notably,
RKIP
can interrupt signaling through the Ras-Raf-MEK-
ERK
pathway by dissociating the interaction between Raf-1 and its substrate MEK, highlighting the importance of protein interactions as regulatory interfaces. Furthermore,
RKIP
was shown to inhibit IkappaB kinases (IKKs) interfering with the activation of nuclear factor kappa B (NFkappaB), and G-protein coupled receptor-kinase 2 (GRK2), impeding receptor downregulation and prolonging signaling. More recently,
RKIP
has emerged as an important suppressor of metastasis. Here, we review the functions of
RKIP
and present methods to detect and measure
RKIP
expression and activity in cells and tissues.
...
PMID:Raf kinase inhibitor protein regulation of raf and MAPK signaling. 1675 29
Raf kinase inhibitory protein
(RKIP or PEBP) is an inhibitor of the Raf/MEK/MAP kinase signaling cascade and a suppressor of cancer metastasis. We now show that RKIP associates with centrosomes and kinetochores and regulates the spindle checkpoint in mammalian cells. RKIP depletion causes decreases in the mitotic index, the number of metaphase cells, and traversal times from nuclear envelope breakdown to anaphase, and an override of mitotic checkpoints induced by spindle poisons. Raf-1 depletion or MEK inhibition reverses the reduction in the mitotic index, whereas hyperactivation of Raf mimics the RKIP-depletion phenotype. Finally, RKIP depletion or Raf hyperactivation reduces kinetochore localization and kinase activity of Aurora B, a regulator of the spindle checkpoint. These results indicate that RKIP regulates Aurora B kinase and the spindle checkpoint via the Raf-1/MEK/
ERK
cascade and demonstrate that small changes in the MAP kinase (MAPK) pathway can profoundly impact the fidelity of the cell cycle.
...
PMID:Raf kinase inhibitory protein regulates aurora B kinase and the spindle checkpoint. 1691 43
Mathematical modelling of kinetic processes with different time scales allows a reduction of the governing equations using quasi-steady-state approximations (QSSA). A QSSA theorem is applied to a mathematical model of the influence that
Raf kinase inhibitor protein
(
RKIP
) has on the
ERK
signalling pathway. On the basis of previously published parameter values, the system of 11 ordinary differential equations is rewritten in a form suitable for model reduction. In accordance with the terminology of the QSSA theorem, it is established that four of the protein and protein-complex concentrations are 'fast varying', such that the corresponding kinetic equations form an attached system. Another concentration is 'medium varying' such that the corresponding equation is reduced with respect to the four fast ones. The other six concentrations are 'slow varying', which means the corresponding kinetic equations also present a reduced system with respect to the others. Analytical solutions, relating the steady-state values of the fast varying protein concentrations and the slow varying ones, are derived and interpreted as restrictions on the regulatory role of
RKIP
on
ERK
-pathway.
...
PMID:Reduction of nonlinear dynamic systems with an application to signal transduction pathways. 1737 Apr 24
Rituximab (chimeric anti-CD20 monoclonal antibody) is the first Food and Drug Administration approved antitumor antibody and is used in the treatment of B-non-Hodgkin's lymphoma (B-NHL). It is used as single monotherapy or in combination with chemotherapy and has improved the treatment outcome of patients with B-NHL. The in vivo mechanisms of rituximab-mediated antitumor effects include antibody-dependent cellular cytotoxicity (ADCC), complement-dependent cell cytotoxicity (CDC), growth-inhibition and apoptosis. A subset of patients does not initially respond to rituximab and several responsive patients develop resistance to further rituximab treatment. The mechanism of rituximab unresponsiveness is not known. Besides the above-postulated mechanisms, rituximab has been shown to trigger the cells via CD-20. Studies performed with B-NHL cell lines as model systems revealed several novel mechanisms of rituximab-mediated effects that are involved in chemo/immunosensitization and the development of resistance to rituximab. Rituximab has been shown to inhibit the p38 mitogen-activated protein kinase, nuclear factor-kappaB (NF-kappaB), extracellular signal-regulated kinase 1/2 (
ERK
1/2) and AKT antiapoptotic survival pathways, all of which result in upregulation of phosphatase and tensin homolog deleted on chromosome ten and
Raf kinase inhibitor protein
and in the downregulation of antiapoptotic gene products (particularly Bcl-2, Bcl-(xL) and Mcl-1), and resulting in chemo/immunosensitization. Further, rituximab treatment inhibits the overexpressed transcription repressor Yin Yang 1 (YY1), which negatively regulates Fas and DR5 expression and its inhibition leads to sensitization to Fas ligand and tumor necrosis factor-related apoptosis-inducing ligand-induced apoptosis. Rituximab-resistant clones were generated as model to examine the mechanism of in vivo rituximab unresponsiveness. These clones showed reduced expression of CD20 and hyperactivation of the above antiapoptotic signaling pathways and failure of rituximab to trigger the cells leading to inhibition of ADCC, CDC and chemo/immunosensitization. Interference with the hyperactivated pathways with various pharmacological and proteasome inhibitors reversed resistance. Furthermore, the above findings have identified several gene products that can serve as new prognostic/diagnostic biomarkers as well as targets for therapeutic intervention in B-NHL.
...
PMID:Rituximab-induced inhibition of antiapoptotic cell survival pathways: implications in chemo/immunoresistance, rituximab unresponsiveness, prognostic and novel therapeutic interventions. 1753 16
The
Raf kinase inhibitory protein
1 (RKIP-1) and its orthologs are conserved throughout evolution and widely expressed in eukaryotic organisms. In its non-phosphorylated form RKIP-1 negatively regulates the Raf/MEK/
ERK
pathway by interfering with the activity of Raf-1. In its phosphorylated state, RKIP-1 dissociates from Raf-1 and inhibits GRK-2, a negative regulator of G-protein coupled receptors (GPCRs). Available data indicate that the phosphorylation of RKIP-1 by PKC can stimulate both the Raf/MEK/
ERK
and GPCR pathways. RKIP-1 has also been implicated as a negative regulator of the NF-kappaB pathway. Recent studies have shown that phosphorylated RKIP-1 binds to the centrosomal and kinetochore regions of metaphase chromosomes, where it may be involved in regulating the partitioning of chromosomes and the progression through mitosis. The collective evidence indicates that RKIP-1 regulates the activity and mediates the crosstalk between several important cellular signaling pathways. A variety of ablative interventions suggest that reduced RKIP-1 function may influence metastasis, angiogenesis, resistance to apoptosis, and genome integrity. Attenuation of RKIP-1 may also affect cardiac and neurological functions, spermatogenesis, sperm decapacitation, and reproductive behavior. In this review, the role of RKIP-1 in cellular signaling, and especially its functions revealed using a mouse knockout model, are discussed.
...
PMID:Signaling crossroads: the function of Raf kinase inhibitory protein in cancer, the central nervous system and reproduction. 1770 25
The Raf-MEK-
ERK
pathway regulates many fundamental biological processes, and its activity is finely tuned at multiple levels. The
Raf kinase inhibitory protein
(
RKIP
) is a widely expressed negative modulator of the Raf-MEK-
ERK
signaling pathway. We have previously shown that
RKIP
inhibits the phosphorylation of MEK by Raf-1 through interfering with the formation of a kinase-substrate complex by direct binding to both Raf-1 and MEK. Here, we show that the evolutionarily conserved ligand-binding pocket of
RKIP
is required for its inhibitory activity towards the Raf-1 kinase mediated activation of MEK. Single amino acid substitutions of two of the conserved residues form the base and the wall of the pocket confers a loss-of-function phenotype on
RKIP
. Loss-of-function
RKIP
mutants still appear to bind to Raf-1. However the stability of the complexes formed between mutants and the N-region Raf-1 phosphopeptide were drastically reduced. Our results therefore suggest that the
RKIP
conserved pocket may constitute a novel phosphoamino-acid binding motif and is absolutely required for
RKIP
function.
...
PMID:The RKIP (Raf-1 Kinase Inhibitor Protein) conserved pocket binds to the phosphorylated N-region of Raf-1 and inhibits the Raf-1-mediated activated phosphorylation of MEK. 1829 16
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