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Query: UMLS:C0025202 (
melanoma
)
69,561
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
In melanocytes and
melanoma
cells, cAMP activates extracellular signal-regulated kinases (ERKs) and MEK-1 by an unknown mechanism. We demonstrate that
B-Raf
is activated by cAMP in melanocytes. A dominant-negative mutant of
B-Raf
, but not of Raf-1, blocked the cAMP-induced activation of ERK, indicating that
B-Raf
is the MEK-1 upstream regulator mediating this cAMP effect. Studies using Clostridium sordelii lethal toxin and Clostridium difficile toxin B have suggested that Rap-1 or Ras might transduce cAMP action. We show that Ras, but not Rap-1, is activated cell-specifically and mediates the cAMP-dependent activation of ERKs, while Rap-1 is not involved in this process in melanocytes. Our results suggest a novel, cell-specific mechanism involving Ras small GTPase and
B-Raf
kinase as mediators of ERK activation by cAMP. Also, in melanocytes, Ras or ERK activation by cAMP is not mediated through protein kinase A activation. Neither the Ras exchange factor, Son of sevenless (SOS), nor the cAMP-responsive Rap-1 exchange factor, Epac, participate in the cAMP-dependent activation of Ras. These findings suggest the existence of a melanocyte-specific Ras exchange factor directly regulated by cAMP.
...
PMID:Ras mediates the cAMP-dependent activation of extracellular signal-regulated kinases (ERKs) in melanocytes. 1085 35
Cancers arise owing to the accumulation of mutations in critical genes that alter normal programmes of cell proliferation, differentiation and death. As the first stage of a systematic genome-wide screen for these genes, we have prioritized for analysis signalling pathways in which at least one gene is mutated in human cancer. The RAS RAF MEK ERK MAP kinase pathway mediates cellular responses to growth signals. RAS is mutated to an oncogenic form in about 15% of human cancer. The three RAF genes code for cytoplasmic serine/threonine kinases that are regulated by binding RAS. Here we report
BRAF
somatic missense mutations in 66% of malignant melanomas and at lower frequency in a wide range of human cancers. All mutations are within the kinase domain, with a single substitution (V599E) accounting for 80%. Mutated
BRAF
proteins have elevated kinase activity and are transforming in NIH3T3 cells. Furthermore, RAS function is not required for the growth of cancer cell lines with the V599E mutation. As
BRAF
is a serine/threonine kinase that is commonly activated by somatic point mutation in human cancer, it may provide new therapeutic opportunities in
malignant melanoma
.
...
PMID:Mutations of the BRAF gene in human cancer. 2339 51
Using a genome-scanning approach to search for oncogenes, a recent report identifies somatic mutations in the signaling gene
BRAF
that are particularly prevalent in
melanoma
.
...
PMID:A genome-based strategy uncovers frequent BRAF mutations in melanoma. 1215 Aug 18
To evaluate the timing of mutations in
BRAF
(v-raf murine sarcoma viral oncogene homolog B1) during melanocytic neoplasia, we carried out mutation analysis on microdissected
melanoma
and nevi samples. We observed mutations resulting in the V599E amino-acid substitution in 41 of 60 (68%)
melanoma
metastases, 4 of 5 (80%) primary melanomas and, unexpectedly, in 63 of 77 (82%) nevi. These data suggest that mutational activation of the RAS/RAF/MAPK pathway in nevi is a critical step in the initiation of melanocytic neoplasia but alone is insufficient for
melanoma
tumorigenesis.
...
PMID:High frequency of BRAF mutations in nevi. 1244 72
BRAF
encodes a RAS-regulated kinase that mediates cell growth and malignant transformation kinase pathway activation. Recently, we have identified activating
BRAF
mutations in 66% of melanomas and a smaller percentage of many other human cancers. To determine whether
BRAF
mutations account for the MAP kinase pathway activation common in non-small cell lung carcinomas (NSCLCs) and to extend the initial findings in
melanoma
, we screened DNA from 179 NSCLCs and 35 melanomas for
BRAF
mutations (exons 11 and 15). We identified
BRAF
mutations in 5 NSCLCs (3%; one V599 and four non-V599) and 22 melanomas (63%; 21 V599 and 1 non-V599). Three
BRAF
mutations identified in this study are novel, altering residues important in AKT-mediated
BRAF
phosphorylation and suggesting that disruption of AKT-induced
BRAF
inhibition can play a role in malignant transformation. To our knowledge, this is the first report of mutations documenting this interaction in human cancers. Although >90% of
BRAF
mutations in
melanoma
involve codon 599 (57 of 60), 8 of 9
BRAF
mutations reported to date in NSCLC are non-V599 (89%; P < 10(-7)), strongly suggesting that
BRAF
mutations in NSCLC are qualitatively different from those in
melanoma
; thus, there may be therapeutic differences between lung cancer and
melanoma
in response to RAF inhibitors. Although uncommon,
BRAF
mutations in human lung cancers may identify a subset of tumors sensitive to targeted therapy.
...
PMID:BRAF and RAS mutations in human lung cancer and melanoma. 1246 Sep 18
Dysregulated activation of Ras or its downstream effectors such as mitogen-activated protein kinase kinase and ERK has been shown to play a critical role in tumorigenesis of many cancer types. However, in
melanoma
, activating mutations in Ras are rarely observed and are limited to N-Ras in UV-exposed cells. In this study, we identify constitutively activated ERK in almost all
melanoma
cell lines and in tumor tissues tested, which is in contrast to normal melanocytes and several early stage radial growth phase
melanoma
lines where ERK can be activated by serum or growth factors. Constitutive activation of ERK is preceded by phosphorylation of mitogen-activated protein kinase kinase and c-RAF. In all of the
melanoma
cell lines tested, Ras is constitutively activated without underlying mutations. On the contrary, activating mutations in the kinase domain of
BRAF
are present in the majority of the cell lines tested. Furthermore, ERK activation can be partially inhibited from the cell surface using inhibitors of fibroblast growth factor and hepatocyte growth factor but not interleukin 8 signaling pathways. These data suggest that
melanoma
growth, invasion, and metastasis are attributable to constitutively activated ERK apparently mediated by excessive growth factors through autocrine mechanisms and
BRAF
kinase activation.
...
PMID:Constitutive mitogen-activated protein kinase activation in melanoma is mediated by both BRAF mutations and autocrine growth factor stimulation. 1259 21
During the process of oncogenic transformation,
melanoma
cells escape from normal growth-control mechanisms and acquire the ability to invade surrounding tissues and organs. The Ras/Raf/MEK/ERK pathway is a major pathway involved in the control of growth signals, cell survival and invasion.
Melanomas
are known to harbour activating mutations of both Ras and
BRAF
, suggesting that the downstream effector ERK may be playing a major role in the oncogenic behaviour of these tumours. The past few years have seen a growth in the understanding of the role of ERK and the MAP kinase pathway in
melanoma
. The aim of the current review is to assess the role of ERK in
melanoma
behaviour and to determine whether modulation of these kinases could offer new therapeutic opportunities.
...
PMID:A pivotal role for ERK in the oncogenic behaviour of malignant melanoma? 1259 6
We have analyzed DNA from peripheral blood of 42 cases of familial
melanoma
for germline mutations in exon 15 of the
BRAF
gene. No evidence of mutation was found. We have also analyzed DNA extracted from secondary
melanoma
from two members of these families. These results were also negative. In addition we have searched for exon 15
BRAF
mutations in 24 samples of secondary
melanoma
from 22 cases of sporadic
melanoma
and detected the 1796T>A
BRAF
mutation which leads to a substitution of valine by glutamic acid at position 599 (V599E) in six samples. Peripheral blood DNA from two of these tumor-positive cases of sporadic
melanoma
were negative for the V599E
BRAF
mutation. This mutation therefore appears to be a somatic mutation associated with
melanoma
development and/or progression in a proportion of affected individuals.
...
PMID:Absence of exon 15 BRAF germline mutations in familial melanoma. 1261 20
The
BRAF
gene has been found to be activated by mutation in human cancers, predominantly in
malignant melanoma
. We tested 476 primary tumors, including 214 lung, 126 head and neck, 54 thyroid, 27 bladder, 38 cervical, and 17 prostate cancers, for the
BRAF
T1796A mutation by polymerase chain reaction (PCR)-restriction enzyme analysis of
BRAF
exon 15. In 24 (69%) of the 35 papillary thyroid carcinomas examined, we found a missense thymine (T)-->adenine (A) transversion at nucleotide 1796 in the
BRAF
gene (T1796A). The T1796A mutation was detected in four lung cancers and in six head and neck cancers but not in bladder, cervical, or prostate cancers. Our data suggest that activating
BRAF
mutations may be an important event in the development of papillary thyroid cancer.
...
PMID:BRAF mutation in papillary thyroid carcinoma. 1269 56
A recent report has shown that activating mutations in the
BRAF
gene are present in a large percentage of human malignant melanomas and in a proportion of colon cancers. The vast majority of these mutations represent a single nucleotide change of T-A at nucleotide 1796 resulting in a valine to glutamic acid change at residue 599 within the activation segment of
B-Raf
. This exciting new discovery is the first time that a direct association between any RAF gene and human cancer has been reported. Raf proteins are also indirectly associated with cancer as effectors of activated Ras proteins, oncogenic forms of which are present in approximately one-third of all human cancers.
BRAF
and RAS mutations are rarely both present in the same cancers but the cancer types with
BRAF
mutations are similar to those with RAS mutations. This has been taken as evidence that the inappropriate regulation of the downstream ERKs (the p42/p44 MAP kinases) is a major contributing factor in the development of these cancers. Recent studies in mice with targeted mutations of the raf genes have confirmed that
B-Raf
is a far stronger activator of ERKs than its better studied Raf-1 homologue, even in cell types in which the protein is barely expressed. The explanation for this lies in a number of key differences in the regulation of
B-Raf
and Raf-1 activity. Constitutive phosphorylation of serine 445 of
B-Raf
leads to this protein having a higher basal kinase activity than Raf-1. Phosphorylation of threonine 598 and serine 601 within the activation loop of
B-Raf
at the plasma membrane also regulates its activity. The V599E mutation is thought to mimic these phosphorylations, resulting in a protein with high activity, leading to constitutive ERK activation.
B-Raf
now provides a critical new target to which drugs for treating
malignant melanoma
can be developed and, with this in mind, it is now important to gain clear insight into the biochemical properties of this relatively little characterised protein.
...
PMID:Raf proteins and cancer: B-Raf is identified as a mutational target. 1278 69
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