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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)
While screening a chicken kidney cDNA library for the normal homolog of the yes oncogene, we isolated a clone that encodes a novel
non-receptor type protein tyrosine kinase
of the Src family. We named this gene product
Yrk
(York), as an acronym for Yes-related kinase. As predicted from the cDNA sequence, the
Yrk
protein consists of 536 amino acids and has all the canonical features of a Src kinase. At the amino terminus it contains a myristylation signal, followed by a unique domain, SH3 and SH2 motifs, an ATP binding site, a kinase region and a carboxy-terminal sequence with a potential regulatory tyrosine at position 530. The sequence of the
Yrk
protein showed 79% identity with human Fyn and 72% identity with chicken Yes. To eliminate the possibility that the
Yrk
protein is an avian homolog of mammalian Fyn, we isolated and sequenced the chicken fyn cDNA. The sequence data together with Southern and Northern blot analyses showed that the chicken yrk gene is distinct from the chicken fyn gene. Antibodies generated against the unique domain of the yrk protein expressed in bacteria precipitated a 60-kDa protein that was active in an immune complex kinase assay and was phosphorylated on tyrosine. Expression of the
Yrk
protein in adult chicken tissues was elevated in cerebellum and spleen. Relatively high levels of
Yrk
were also found in lung and skin.
...
PMID:A novel Yes-related kinase, Yrk, is expressed at elevated levels in neural and hematopoietic tissues. 845 40
Protein tyrosine kinases (PTKs) have been implicated in the development of many common human tumours including melanoma. Previously we isolated PTK gene sequences expressed in normal melanocytes. Here we examined expression of 9 of these genes in cell lines derived from defined stages of melanoma progression, by Northern blotting and in some cases immunoblotting. We also tested cells from 2 animal models of particular stages in progression, as well as uncultured biopsies of metastatic melanoma. The expression of 2 receptor kinase family members found in melanocytes,
PTK7
/CCK-4 and SEK/TYRO1, was decreased or lost in advanced melanomas.
PTK7
mRNA was found in only 54% of melanoma cell lines and 20% of melanoma biopsies. Similarly, expression was lost in 2 advanced cell lines selected from an early melanoma line that did express
PTK7
mRNA. SEK/TYRO1 expression was observed in 75% and 17% of cell lines from primary and metastastic melanomas, respectively. Conversely, mRNA for the non-receptor kinase
PTK6
/BRK was not detected in normal melanocytes or primary melanoma lines, but was found in 9% of metastatic melanoma cell lines.
...
PMID:Loss of expression of receptor tyrosine kinase family genes PTK7 and SEK in metastatic melanoma. 918 12
The
brk
gene encodes a non-
receptor protein tyrosine kinase
that consists of single SH3, SH2 and catalytic domains. Although BRK shows strongest sequence similarity to members of the SRC family of PTKs, there are several key structural and regulatory differences that place it on its own amongst non-receptor PTKs. In this study we have isolated genomic DNA clones corresponding to the human
brk
locus and used these to determine the intron-exon structure of the
brk
gene. The genomic structure of
brk
consists of 8 exons, whose boundaries are distinct from other non-receptor
PTK
family members, again indicating a structural and functional divergence. Alternate splicing of the primary
brk
transcript generates a distinct mRNA which encodes a truncated protein consisting of an SH3 domain and a novel C-terminal proline rich sequence. Using an antiserum raised to the SH3 domain, we have demonstrated that the product of this alternate
brk
transcript is expressed in the human breast tumour cell line T-47D. We have previously reported that expression of a tumour derived
brk
cDNA in mouse embryonic fibroblasts and human mammary epithelial cells supports anchorage independent growth, and in the latter potentiates the mitogenic response to epidermal growth factor. The protein encoded by the genomic sequence derived from normal human tissue is identical to that encoded by the tumour derived cDNA, and therefore the altered growth regulation is not associated with mutations within
brk
. In addition, we have identified a 5' genomic region that has promoter activity. The
brk
gene has been assigned to chromosome 20q 13.3 [corrected] using fluorescence in situ hybridisation (FISH).
...
PMID:Characterisation and chromosome mapping of the human non receptor tyrosine kinase gene, brk. 933 26
Partial
PTK6
(also known as Brk) cDNA was initially isolated by reverse transcription-PCR of normal human melanocyte mRNAs and the full-length cDNA encodes a non-
receptor protein tyrosine kinase
with an SH3 domain, an SH2 domain, and a kinase catalytic domain. We have cloned the human
PTK6
gene by screening human genomic lambda libraries using the full-length
PTK6
cDNA as probe. The human
PTK6
gene consists of 8 exons encompassing 8.8 kb and all the splicing junctions followed the conserved GT/AG rule. Coding sequence of the
PTK6
gene was identical to that of the cDNA cloned from T-47D, human breast tumor cell line. Although the amino acid sequence of the
PTK6
polypeptide showed the strongest homology to those of the Src family members of protein tyrosine kinases, exon-intron boundaries of the
PTK6
gene were quite different from those of the Src family genes, which are evolutionarily conserved. The 813-bp 5'-flanking sequence of the
PTK6
gene upstream of a luciferase reporter gene conferred significant promoter activity, at approximately 60% level of the SV40 promoter, in transient expression assays into MCF-7, human breast tumor cell line.
PTK6
mRNA was expressed at very high level in colon and at high levels in small intestine and prostate, and at low levels in some tested fetal tissues. These results suggest that
PTK6
constitutes an evolutionarily distinct family of non-receptor protein tyrosine kinases and may function as an intracellular signal transducer in specific tissues.
...
PMID:Exon-intron structure of the human PTK6 gene demonstrates that PTK6 constitutes a distinct family of non-receptor tyrosine kinase. 974 26
PTK6
(also known as Brk) is a non-
receptor protein tyrosine kinase
, whose mRNA was expressed in the limited normal tissues such as colon and small intestine, and in breast carcinomas and breast cancer cell lines. The 813 bp region upstream from the translation initiation codon, which constitutes a functional promoter of the human
PTK6
gene, was progressively deleted and fused to the luciferase reporter gene and transient expression of the resultant constructs was measured upon transfection into a breast carcinoma cell line, T-47D. Comparative analysis of luciferase activity revealed two major regions, -93 to -76 and -702 to -655, important for transcriptional regulation. The proximal -93 to -76 region was found to be essential for the function of the minimal promoter. By primer extension and PCR, it was shown that a
PTK6
transcript started at the most 5' upstream is located around base -104. Therefore, the proximal -93 to -76 region is thought to function as a downstream cis-acting element. Luciferase analysis showed that the distal -702 to -655 region contained at least two cis-acting elements. Gel mobility shift assays with T-47D nuclear extract including competition analyses with consensus and mutant oligonucleotides and supershift analyses with NF-kappaB and Sp1 antibodies showed that NF-kappaB binds to the sequence from -706 to -688 and Sp1 binds to the sequence from -688 to -669. This study thus provides the first molecular insights into the transcriptional regulation of the human
PTK6
gene.
...
PMID:Characterization of the 5'-flanking region of the human PTK6 gene. 1199 4
The tyrosine kinases Brk/
PTK6
/Sik, Srm, Frk/Rak/Gtk/Iyk/
Bsk
, and Src42A/Dsrc41 have a low degree of sequence homology to other known kinases, including one another. We show here that the exon structure of these kinases, which we will call the Brk family, is highly conserved and distinct from each of the major families of intracellular kinases containing SH3, SH2, and tyrosine kinase domains, including c-Src and Fyn. Brk/Sik and Srm are 1.1 kb apart on human chromosome 20q13.3 and likely are the result of duplication in cis. Several Brk family kinases have an inhibitory effect on Ras pathway signaling from receptor tyrosine kinases. Members of this family can act either in the membrane or at the nucleus, and may change localization patterns depending on external stimuli. Brk has been shown to phosphorylate two proteins in vivo: Sam68. a substrate for Src in mitosis that can substitute for Rev in nuclear export of RNAs; and BKS, a novel adaptor molecule. Brk also functions as a rapid downstream signaling intermediate following calcium-induced differentiation in keratinocytes. It is possible that Brk family kinases may share common functions and interaction partners, which remain for the most part unexamined.
...
PMID:Brk, Srm, Frk, and Src42A form a distinct family of intracellular Src-like tyrosine kinases. 1272 32
Human protein-tyrosine kinase-6 (
PTK6
, also known as
breast tumor kinase
(Brk)) is a member of the non-
receptor protein-tyrosine kinase
family and is expressed in two-thirds of all breast tumors. To understand the structural basis of
PTK6
function, we have determined the solution structure and backbone dynamics of the
PTK6
-Src homology 2 (SH2) domain using multidimensional NMR spectroscopy. The solution structure clearly indicates that the SH2 domain of human
PTK6
contains a consensus alpha/beta-fold and a Tyr(P) peptide binding surface, which are common to other SH2 domains. However, two of the alpha-helices (alphaA and alphaB) are located on opposite faces of the central beta-sheet. In addition, the topological arrangement of a central four-stranded antiparallel beta-sheet (strands betaA, betaB, betaC, and betaD) differs from that of other Src family members. Backbone dynamics and Tyr(P) peptide titration experiments revealed that the putative ligand binding sites of the
PTK6
-SH2 domain undergo distinctive internal motions when compared with other regions of the protein. Surface plasmon resonance analysis showed that the Tyr(P) peptide had a dissociation constant of about 60 microm, which is substantially weaker binding than previously reported for Src family members. The solution structure together with data from the ligand binding mode of
PTK6
-SH2 provides insight into the molecular basis of the autoinhibitory role of
PTK6
.
...
PMID:Solution structure and backbone dynamics of the non-receptor protein-tyrosine kinase-6 Src homology 2 domain. 1505 53
The HER receptors are of therapeutic and prognostic significance in breast cancer, and their function is modulated by cytoplasmic tyrosine kinases like
PTK6
(brk). We performed a retrospective study on archival breast cancer samples from patients with long follow-up and compared the protein expression between individual HERs and between HERs and the
PTK6
. Univariate and multivariate analyses were used to study the prognostic value of parameters. Metastases-free survival of patients for longer than 240 months was inversely associated (P< or =0.05) with nodal status, tumour size, and oestrogen receptor status, but was also directly associated with high protein expression levels of
HER4
and
PTK6
in Kaplan-Meier analysis. In multivariate analysis for metastases-free survival of >240 months, the stepwise selected parameters were tumour size (relative risk 3.1),
PTK6
expression (0.4), and number of positive lymph nodes (1.2). Furthermore, we demonstrated a timedependence of the prognostic value attributed to the parameters. The HER receptors (
HER2
,4), but not
PTK6
, were independent prognostic markers for metastases-free survival at 60 months, whereas at 240 months
PTK6
is the strongest prognostic marker. We demonstrate that
PTK6
is a prognostic marker of metastases-free survival in breast cancer, and is independent of the classical morphological and molecular markers of lymph node involvement, tumour size, and
HER2
status.
...
PMID:PTK (protein tyrosine kinase)-6 and HER2 and 4, but not HER1 and 3 predict long-term survival in breast carcinomas. 1729 91
The cytoplasmic tyrosine kinase
PTK6
(BRK) shows elevated expression in approximately two-thirds of primary breast tumours, and is implicated in EGF receptor-dependent signalling and epithelial tumorigenesis. Using immunohistochemistry, we performed a retrospective study on 426 archival breast cancer samples from patients with long-term follow-up and compared the protein expression levels of
PTK6
, the HER receptors, Sam68 (a substrate of
PTK6
), and signalling proteins including MAP kinase (MAPK), phosphorylated MAPK (P-MAPK), and PTEN. We show that
PTK6
expression is of significant prognostic value in the outcome of breast carcinomas. In multivariate analysis, the disease-free survival of patients of >or=240 months was directly associated with the protein expression level of
PTK6
(P<or=0.001), but was also inversely associated with nodal status (P<or=0.001) and tumour size (P<or=0.01).
PTK6
expression in tumour tissue significantly correlated (P<or=0.05) with the expression of PTEN, MAPK, P-MAPK, and Sam68. To investigate whether these correlations may be due to molecular interactions between
PTK6
and these proteins, we used protein extracts from the T47D cell line for immunoprecipitation and western blot analysis. By this, interactions could be demonstrated between
PTK6
and MAPK, P-MAPK,
HER2
/neu,
HER3
,
HER4
, PTEN, and Sam68. On the basis of these results, we suggest that
PTK6
may serve as a future target for the development of novel treatments in breast cancer.
...
PMID:Prognostic value of protein tyrosine kinase 6 (PTK6) for long-term survival of breast cancer patients. 1878 Nov 81
PTK6
, also known as Brk, is highly expressed in over 80% of breast cancers. In the last decade several substrates and interaction partners were identified localising
PTK6
downstream of HER receptors.
PTK6
seems to be involved in progression of breast tumours, in particular in HER receptor signalling. Here, we show the down-regulation effects of
PTK6
in the T47D, BT474 and JIMT-1 breast cancer cell lines.
PTK6
knockdown leads to a decreased phosphorylation of
HER2
, PTEN, MAPK (
ERK
), p38 MAPK, STAT3 and to a reduced expression of cyclin E. Our findings show that silencing
PTK6
impairs the downstream targets of HER receptors and consequently the activation of signalling molecules. Furthermore, lower levels of
PTK6
result in reduced migration of T47D and JIMT-1 breast cancer cells. Due to decreased migration, the
PTK6
RNA interference might contribute to reduced metastasis and malignant potential of breast cancer cells. Since
PTK6
plays an important role in HER receptor signal transduction, its down-regulation might be suitable for future therapy approaches in breast cancer.
...
PMID:Impact of protein tyrosine kinase 6 (PTK6) on human epidermal growth factor receptor (HER) signalling in breast cancer. 2138 Apr 7
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