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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)
Human thyroid papillary carcinomas are characterized by rearrangements of the
RET
protooncogene with a number of heterologous genes, which generate the
RET
/papillary thyroid carcinoma (PTC) oncogenes. One of the most frequent variants of these recombination events is the fusion of the intracellular kinase-encoding domain of
RET
to the first 101 amino acids of a gene named H4(D10S170). We have characterized the H4(D10S170) gene product, showing that it is a ubiquitously expressed 55 KDa nuclear and cytosolic protein that is phosphorylated following serum stimulation. This phosphorylation was found to depend on mitogen-activated protein kinase (MAPK) Erk1/2 activity and to be associated to the relocation of H4(D10S170) from the nucleus to the cytosol. Overexpression of the H4(D10S170) gene was able to induce apoptosis of thyroid follicular epithelial cells; conversely a carboxy-terminal truncated H4(D10S170) mutant H4(1-101), corresponding to the portion included in the
RET
/
PTC1
oncoprotein, behaved as dominant negative on the proapoptotic function and nuclear localization of H4(D10S170). Furthermore, conditional expression of the H4(D10S170)-dominant negative truncated mutant protected cells from stress-induced apoptosis. The substitution of serine 244 with alanine abrogated the apoptotic function of H4(D10S170). These data suggest that loss of the H4(D10S170) gene function might have a role in thyroid carcinogenesis by impairing apoptosis.
...
PMID:H4(D10S170), a gene frequently rearranged with RET in papillary thyroid carcinomas: functional characterization. 1471 16
Ret oncoproteins expressed in thyroid carcinomas represent possible targets for therapeutic intervention. Oncogenic activation of the receptor tyrosine kinase encoding
RET
gene occurs typically by gene rearrangement in papillary thyroid carcinomas (PTC) and by missense mutation in medullary thyroid carcinomas (MTC). These genetic alterations lead to the expression of deregulated products characterized by ligand-independent activation of the intrinsic tyrosine kinase of Ret. Such features suggest the possibility of using specific tyrosine kinase inhibitors to block the Ret oncoproteins signaling. The present report summarizes the cellular effects of the arylidene 2-indolinone Ret inhibitor RPI-1 (formerly Cpd1) on the human PTC cell line TPC-1 which spontaneously harbors the
RET
/
PTC1
oncogene. The results provide evidence that RPI-1 is able to inhibit cell growth and to interfere with Ret/ptc1-driven signaling. These findings support a role for Ret oncoproteins as therapeutic targets and the pharmacological interest of RPI-1 as a candidate drug for preclinical evaluation on thyroid tumors expressing
RET
oncogenes.
...
PMID:RET/PTC oncoproteins: molecular targets of new drugs. 1487 Jul 76
The large numbers of papillary thyroid carcinomas that have occurred in those exposed to high levels of short-lived isotopes in fallout after Chernobyl provide a unique opportunity to correlate latency and tumour biology. We show that short latency is associated with tumours with a phenotype that is significantly less structurally differentiated, shows significantly less peritumour fibrosis, and significantly more invasive spread when compared to tumours with a longer latent period. In contrast, the type of differentiation (papillary or follicular architecture) is associated with age at exposure. These findings suggest that the initial mutation at the time of exposure played a major role in tumour latency and aggressiveness. We and others have shown that
RET
-PTC3 rearrangements are associated with the solid morphology seen in these short latency tumours, while classical papillary carcinomas more often show
RET
-
PTC1
rearrangements. Studies in transgenic mice show similar findings, and in vitro studies show that
RET
-PTC3 induces more rapid growth than
RET
-
PTC1
. We therefore suggest that the solid morphology, high frequency of
RET
-PTC3 rearrangements and aggressive behaviour noted in early investigations of post-Chernobyl tumours were characteristic of short latency rather than the nature of the mutagen, and that successive overlapping waves of papillary carcinoma with differing latency, differing patterns of mutations and differing clinical behaviour are occurring in those exposed to Chernobyl fallout.
...
PMID:Thyroid carcinoma after Chernobyl latent period, morphology and aggressiveness. 1515 May 80
We show that treatment of a panel of thyroid carcinoma cell lines naturally harboring the
RET
/
PTC1
oncogene, with the
RET
kinase inhibitors PP1 and ZD6474, results in reversible G(1) arrest. This is accompanied by interruption of Shc and mitogen-activated protein kinase (MAPK) phosphorylation, reduced levels of G(1) cyclins, and increased levels of the cyclin-dependent kinase inhibitor p27Kip1 because of a reduced protein turnover. MAP/extracellular signal-regulated kinase 1/2 inhibition by U0126 caused G(1) cyclins down-regulation and p27Kip1 up-regulation as well. Forced expression of
RET
/PTC in normal thyroid follicular cells caused a MAPK- and proteasome-dependent down-regulation of p27Kip1. Reduction of p27Kip1 protein levels by antisense oligonucleotides abrogated the G(1) arrest induced by
RET
/PTC blockade. Therefore, in thyroid cancer,
RET
/PTC-mediated MAPK activation contributes to p27Kip1 deregulation. This pathway is implicated in cell cycle progression and in response to small molecule kinase inhibitors.
...
PMID:Regulation of p27Kip1 protein levels contributes to mitogenic effects of the RET/PTC kinase in thyroid carcinoma cells. 1517 89
Activating germ-line point mutations in the
RET
receptor are responsible for multiple endocrine neoplasia type 2-associated medullary thyroid carcinoma (MTC), whereas somatic
RET
rearrangements are prevalent in papillary thyroid carcinomas (PTCs). Some rare kindreds, carrying point mutations in
RET
, are affected by both cancer types, suggesting that, under specific circumstances, point mutations in
RET
can drive the generation of PTC. Here we describe a family whose siblings, affected by both PTC and MTC, carried a germ-line point mutation in the
RET
extracellular domain, converting cysteine 634 into serine. We tested on thyroid follicular cells the transforming activity of
RET
(C634S),
RET
(K603Q), another mutant identified in a kindred with both PTC and MTC,
RET
(C634R) a commonly isolated allele in MEN2A,
RET
(M918T) responsible for MEN2B and also identified in kindreds with both PTC and MTC, and
RET
/
PTC1
the rearranged oncogene that characterizes bona fide PTC in patients without MTC. We show that the various
RET
point mutants, but not wild-type
RET
, scored constitutive kinase activity and exerted mitogenic effects for thyroid PC Cl 3 cells, albeit at significantly lower levels compared to
RET
/
PTC1
. The low mitogenic activity of
RET
point mutants paralleled their reduced kinase activity compared to
RET
/PTC. Furthermore,
RET
point mutants maintained a protein domain, the intracellular juxtamembrane domain, that exerted negative effects on the mitogenic activity. In conclusion,
RET
point mutants can behave as dominant oncogenes for thyroid follicular cells. Their transforming activity, however, is rather modest, providing a possible explanation for the rare association of MTC with PTC.
...
PMID:The oncogenic activity of RET point mutants for follicular thyroid cells may account for the occurrence of papillary thyroid carcinoma in patients affected by familial medullary thyroid carcinoma. 1527 25
Chimeric
RET
/PTC (rearranged in transformation/papillary thyroid carcinoma) oncoproteins are constitutively active tyrosine kinases found in thyroid papillary carcinoma and nonneoplastic Hashimoto's thyroiditis. Although several proteins have been identified to be substrates of
RET
/PTC kinases, the pathogenic roles played by
RET
/PTC in malignant and benign thyroid diseases and the molecular mechanisms that are involved are not fully understood. We found that
RET
/PTC expression phosphorylates the Y701 residue of STAT1, a type II interferon (IFN)-responsive protein.
RET
/PTC-mediated signal transducer and activator of transcription 1 (STAT1) phosphorylation requires
RET
/PTC kinase activity to be intact but other tyrosine kinases, such as Janus kinases or c-Src, are not involved.
RET
/PTC-induced STAT1 transcriptional activation was not inhibited by suppressor of cytokine signaling-1 or -3, or protein inhibitors of activated STAT3 [(protein inhibitor of activated STAT (PIAS3)], but PIAS1 strongly repressed the
RET
/PTC-induced transcriptional activity of STAT1.
RET
/PTC-induced STAT1 activation caused IFN regulatory factor-1 expression. We found that STAT1 and IFN regulatory factor-1 cooperated to significantly increase transcription from type IV IFN-gamma responsive promoters of class II transactivator genes. Significantly, cells stably expressing
RET
/PTC expressed class II transactivator and showed enhanced de novo membrane expression of major histocompatibility complex (MHC) class II proteins. Furthermore,
RET
/
PTC1
-bearing papillary thyroid carcinoma cells strongly expressed MHC class II (human leukocyte-associated antigen-DR alpha) genes, whereas the surrounding normal tissues did not. Thus,
RET
/PTC is able to phosphorylate and activate STAT1. This may lead to enhanced MHC class II expression, which may explain why the tissues surrounding
RET
/PTC-positive cancers are infiltrated with lymphocytes. Such immune response-promoting activity of
RET
/PTC may also relate to the development of Hashimoto's thyroiditis.
...
PMID:Regulation of signal transducer and activator of transcription 1 (STAT1) and STAT1-dependent genes by RET/PTC (rearranged in transformation/papillary thyroid carcinoma) oncogenic tyrosine kinases. 1529 6
RET
/
PTC1
is a rearranged form of the
RET
tyrosine kinase commonly seen in papillary thyroid carcinomas. It has been shown that
RET
/
PTC1
decreases expression of the sodium/iodide symporter (NIS), the molecule that mediates radioiodide therapy for thyroid cancer. Using proteomic analysis, we identify hsp90 and its co-chaperone p50cdc37 as novel proteins associated with
RET
/
PTC1
. Inhibition of hsp90 function with 17-allylamino-17-demothoxygeldanamycin (17-AAG) reduces
RET
/
PTC1
protein levels. Furthermore, 17-AAG increases radioiodide accumulation in thyroid cells, mediated in part through a protein kinase A-independent mechanism. We show that 17-AAG does not increase the total amount of NIS protein or cell surface NIS localization. Instead, 17-AAG increases radioiodide accumulation by decreasing iodide efflux. Finally, the ability of 17-AAG to increase radioiodide accumulation is not restricted to thyroid cells expressing
RET
/
PTC1
. These findings suggest that 17-AAG may be useful as a chemotherapeutic agent, not only to inhibit proliferation but also to increase the efficacy of radioiodide therapy in patients with thyroid cancer.
...
PMID:Inhibition of heat shock protein 90, a novel RET/PTC1-associated protein, increases radioiodide accumulation in thyroid cells. 1530 66
Rearrangements of the RET proto-oncogene (
RET
/PTC) and BRAF gene mutations are the major genetic alterations in the etiopathogenesis of papillary thyroid carcinoma (PTC). We have analyzed a series of 118 benign and malignant follicular cell-derived thyroid tumors for
RET
/PTC rearrangements and BRAF gene mutations. Oncogenic rearrangements of RET proto-oncogene was revealed by semiquantitative RT-PCR of simultaneously generated fragments corresponding to tyrosine kinase (TK) and extracellular
RET
domains. The clear quantitative shift toward the TK fragment is indicative for the presence of
RET
rearrangements. The overall frequency of
RET
/PTC rearrangements in PTC was 14% (12 of 85), including 7
RET
/
PTC1
, 2
RET
/PTC3, 1 deltaRFP/
RET
and 2 apparently uncharacterized rearrangements. The most common T1796A transversion in BRAF gene was detected in 55 of 91 PTC (60%) using mutant-allele-specific PCR. We also identified two additional mutations: the substitution G1753A (E585K) and a case of 12-bp deletion in BRAF exon 15. Moreover, there was no overlap between PTC harboring BRAF and
RET
/PTC mutations, which altogether were present in 75.8% of cases (69 of 91). Taken together, our observations are consistent with the notion that BRAF mutations appear to be an alternative pathway to oncogenic MAPK activation in PTCs without
RET
/PTC activation. Neither
RET
/PTC rearrangements nor BRAF muta-tions were detected in any of 3 follicular thyroid carcinomas, 11 follicular adenomas and 13 nodular goiters. The high prevalence of BRAF mutations and
RET
/PTC rearrangements in PTCs and the specificity of these alterations to PTC make them potentially important markers for the preoperative tumor diagnosis.
...
PMID:[Molecular analysis of structural abnormalities in papillary thyroid carcinoma gene]. 1545 36
RET
/
PTC1
and
RET
/PTC3 are the markers for papillary thyroid carcinoma. Their reported prevalence varies broadly. Nonrearranged c-
RET
has also been detected in a variable proportion of papillary carcinomas. The published data suggest that a wide range in expression levels may contribute to the different frequency of c-
RET
and, particularly, of
RET
/PTC detection. However, quantitative expression analysis has never been systematically carried out. We have analyzed by real-time RT-PCR 25 papillary carcinoma and 12 normal thyroid samples for
RET
/
PTC1
,
RET
/PTC3 and for
RET
exons 10-11 and 12-13, which are adjacent to the rearrangement site. The variability in mRNA levels was marked and four carcinoma groups were identified: one lacking
RET
/PTC rearrangement with balanced
RET
exon levels similar to those of the normal samples (7/25 cases, 28%), the second (6/25 cases, 24%) with balanced
RET
expression and very low levels of
RET
/
PTC1
, the third with unbalanced
RET
exons 10-11 and 12-13 expression, high
RET
/
PTC1
levels but no
RET
/PTC3 (7/25 cases, 28%), and the fourth with unbalanced
RET
expression, high
RET
/
PTC1
levels and low levels of
RET
/PTC3 (5/25 cases, 20%). Papillary carcinomas with high
RET
/
PTC1
expression showed an association trend for large tumor size (P=0.063). Our results indicate that the variability in c-
RET
and
RET
/PTC mRNA levels contributes to the apparent inconsistencies in their reported detection rates and should be taken into account not only for diagnostic purposes but also to better understand the role of c-
RET
activation in thyroid tumorigenesis.
...
PMID:Real-time quantitative RT-PCR identifies distinct c-RET, RET/PTC1 and RET/PTC3 expression patterns in papillary thyroid carcinoma. 1550 56
RET
/
PTC1
, a thyroid-specific oncogene, has been reported to down-regulate sodium/iodide symporter (NIS) expression and function in vitro and in vivo. Recently,
RET
/
PTC1
has been shown to interfere with TSH signaling at multiple levels in thyroid cells. The objective of this study was to investigate whether
RET
/
PTC1
-mediated NIS reduction can be rescued by activating cAMP-protein kinase A (PKA) pathways. We showed that both forskolin and 8-Br-cAMP increase radioiodide uptake and NIS protein in
RET
/
PTC1
-expressing cells to the same extent as the parental PC Cl 3 cells. We found that
RET
/
PTC1
decreases nuclear localization of catalytic PKA, and forskolin treatment was able to counteract this
RET
/
PTC1
effect. Furthermore, transient expression of catalytic PKA in the nucleus increased radioiodide uptake and NIS protein in
RET
/
PTC1
-expressing cells. Taken together, these studies suggest that
RET
/
PTC1
down-regulates NIS expression by interrupting TSH/cAMP signaling, and this
RET
/
PTC1
effect can be reversed by activating cAMP-PKA pathways.
...
PMID:Forskolin, 8-Br-3',5'-cyclic adenosine 5'-monophosphate, and catalytic protein kinase A expression in the nucleus increase radioiodide uptake and sodium/iodide symporter protein levels in RET/PTC1-expressing cells. 1557 73
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