Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
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Drug
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Target Concepts:
Gene/Protein
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Query: EC:2.7.11.24 (
mitogen-activated protein kinase
)
95,810
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
To evaluate the carcinogenicity of troglitazone in rasH2 mice, 7-week-old male and female rasH2 mice were fed a diet containing 0, 3,000 or 6,000 ppm troglitazone for 26 weeks. An increased tendency in the incidence of vascular tumors was observed in females of the 6,000 ppm group. The preliminary analysis using a high-density oligonucleotide microarray on a splenic
hemangiosarcoma
of a high dose female that could be obtained as a fresh sample showed that several genes related to the ras/
MAPK
pathway activation, angiogenesis, cell cycle and cell multiplication were up-regulated. In addition, most of the genes up-regulated were confirmed by the reverse transcriptase-polymerase chain reaction (RT-PCR). These results may suggest that the carcinogenic susceptibility of rasH2 mice to troglitazone is relatively low and up-regulations of the ras/
MAPK
pathway and angiogenesis-related genes are probably involved in the production of splenic hemangiosarcomas in rasH2 mice given troglitazone.
...
PMID:Carcinogenic susceptibility of rasH2 mice to troglitazone. 1756 31
Angiosarcoma is a rare neoplasm of endothelial origin that has limited treatment options and poor five-year survival. As a model for human angiosarcoma, we studied primary cells and tumorgrafts derived from canine
hemangiosarcoma
(
HSA
), which is also an endothelial malignancy with similar presentation and histology. Primary cells isolated from
HSA
showed constitutive
extracellular signal-regulated kinase
(
ERK
) activation. The mitogen-activated protein/
extracellular signal-regulated kinase
(MEK) inhibitor CI-1040 reduced
ERK
activation and the viability of primary cells derived from visceral, cutaneous, and cardiac
HSA
in vitro.
HSA
-derived primary cells were also sensitive to sorafenib, an inhibitor of B-Raf and multireceptor tyrosine kinases. In vivo, CI-1040 or PD0325901 decreased the growth of cutaneous cell-derived xenografts and cardiac-derived tumorgrafts. Sorafenib decreased tumor size in both in vivo models, although cardiac tumorgrafts were more sensitive. In human angiosarcoma, we noted that 50% of tumors stained positively for phosphorylated
ERK1
/2 and that the expression of several MEK-responsive transcription factors was upregulated. Our data showed that MEK signaling is essential for the growth of
HSA
in vitro and in vivo and provided evidence that the same pathways are activated in human angiosarcoma. This indicates that MEK inhibitors may form part of an effective therapeutic strategy for the treatment of canine
HSA
or human angiosarcoma, and it highlights the use of spontaneous canine cancers as a model of human disease.
...
PMID:Pharmacologic inhibition of MEK signaling prevents growth of canine hemangiosarcoma. 2380 5
Canine
hemangiosarcoma
(
HSA
) is a progressive malignant neoplasm of dogs for which there is currently no effective treatment. A recent study suggested that receptor tyrosine kinases (RTKs), the PI3K/Akt/m-TOR and
MAPK
pathways are all activated in canine and human
HSA
. The aim of the present study was to investigate the overexpression of these proteins by immunohistochemistry in canine splenic
HSA
to identify potential molecular therapeutic targets. A total of 10 splenic HSAs and two normal splenic samples surgically resected from dogs were sectioned and stained with hematoxylin and eosin for histological diagnosis or analyzed using immunohistochemistry. The expression of RTKs, c-kit, VEGFR-2 and PDGFR-2, as well as PI3K/Akt/m-TOR and MEK was higher in canine splenic HSAs compared to normal spleens. These proteins may therefore be potential therapeutic targets in canine splenic
HSA
.
...
PMID:Immunohistochemical detection of a potential molecular therapeutic target for canine hemangiosarcoma. 2668 84
Angiosarcoma (AS) is a rare neoplasm with limited treatment options and a poor survival rate. Development of effective therapies is hindered by the rarity of this disease. Dogs spontaneously develop
hemangiosarcoma
(
HSA
), a common, histologically similar neoplasm. Metastatic disease occurs rapidly and despite chemotherapy, most dogs die several months after diagnosis. These features suggest that
HSA
might provide a tractable model to test experimental therapies in clinical trials. We previously reported whole exome sequencing of 20
HSA
cases. Here we report development of a NGS targeted resequencing panel to detect driver mutations in
HSA
and other canine tumors. We validated the panel by resequencing the original 20 cases and sequenced 30 additional cases. Overall, we identified potential driver mutations in over 90% of the cases, including well-documented (in human cancers) oncogenic mutations in PIK3CA (46%), PTEN (6%), PLCG1(4%), and TP53 (66%), as well as previously undetected recurrent activating mutations in NRAS (24%). The driver role of these mutations is further demonstrated by augmented downstream signaling crucial to tumor growth. The recurrent, mutually exclusive mutation patterns suggest distinct molecular subtypes of
HSA
. Driver mutations in some subtypes closely resemble those seen in some AS cases, including NRAS, PLCG1, PIK3CA and TP53. Furthermore, activation of the
MAPK
and PI3K pathways appear to be key oncogenic mechanisms in both species. Together, these observations suggest that dogs with spontaneous
HSA
could serve as a useful model for testing the efficacy of targeted therapies, some of which could potentially be of therapeutic value in AS.
...
PMID:Molecular subtypes in canine hemangiosarcoma reveal similarities with human angiosarcoma. 3221 Apr 30
