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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)
Gastrointestinal stromal tumors (GISTs), generally
KIT
-positive and
KIT
/
PDGFRA
mutation-driven mesenchymal neoplasms, most commonly originate from the stomach or small intestine, but in rare examples they involve the omentum. In this study, we analyzed 95 GISTs surgically designated as the omental masses. These tumors occurred in 49 males and 46 females with a median age of 60 years (range: 27 to 88 y). They formed single (n=51) or multiple masses (n=39); 5 cases were equivocal in this respect. Of the single tumors, 21 had no evidence of gastrointestinal tract involvement, 25 were attached to stomach, and 3 were attached to small intestine. Clinicopathologic parameters and prognosis of the 2 former groups were similar.
Single tumor
cases showed a median mitotic count of 2/50 HPFs and median tumor size was 14 cm. Their histologic features were similar to gastric GISTs in 22 cases, and to small intestinal GISTs in 6 cases. These tumors were
KIT
positive 38/41, CD34 positive 20/33, 8 had
PDGFRA
mutations, and 6 had
KIT
exon 11 mutations. The median survival was 129 months (range: 0 to 397 mo) and 14 patients were alive at the end of follow-up. Multiple tumor cases showed median mitotic count of 14/50 HPFs and the main tumor median size was 16 cm. The histologic features were similar to small intestinal GISTs in 21 cases and to gastric GISTs in 7 cases; small intestinal attachment or history of a previous small intestinal GIST were noted in 5 cases, whereas no tumor was attached to stomach. The multiple GISTs were
KIT
positive 23/24, CD34 positive 7/21, and 5 had
KIT
exon 11 mutations, 3 had
KIT
exon 9 mutations, and 2 had
PDGFRA
mutations. The median survival was for 8 months and all patients died. Omental GISTs are clinicopathologically heterogenous. Patients with solitary tumors usually have gastric GIST-like morphology and a better prognosis than those with multiple tumors, whose tumor usually has small intestinal GIST-like histology. Omental GISTs unattached to gastrointestinal tract often resemble gastric GISTs suggesting that they may be gastric GISTs directly extending or parasitically attached into the omentum, whereas multiple omental GISTs more often resemble small intestinal GISTs suggesting that they may be metastatic or detached from this source.
KIT
positive Cajal cells were not found in normal omental tissues failing to support the presence of these ancestral cells for GIST in the omentum.
...
PMID:Gastrointestinal stromal tumors presenting as omental masses--a clinicopathologic analysis of 95 cases. 1944 Jan 46
Introduction:
The identification of tumor cells that can be potential metastatic seeds would reach two key aims-prognosis of metastasis risk and appointment of the optimal adjuvant therapy to prevent metastatic disease.
Single tumor
cells (STCs) located out of multicellular structures can most likely demonstrate features that are needed to initiate metastasis.
Methods:
One-hundred-and-thirty-five patients with invasive breast carcinoma of no special type have been enrolled. Molecular subtypes of breast cancer were categorized according to St. Gallen recommendations. Hematoxylin and eosin staining was used to identify STCs with epithelial-like morphology (eSTCs) in breast tumors. Immunofluorescence staining was applied to evaluate stemness and epithelial-mesenchymal transition (EMT) in STCs. The correlation between STCs and recurrence and metastasis-free survival (MFS) was performed using the Kaplan-Meier method and the log-rank test.
Results:
Distant metastasis was more frequent in eSTC-positive than eSTC-negative patients (28.0% vs. 9.4%,
p
= 0.007). When tumor types were analyzed separately, distant metastasis tended to be more frequent in eSTC-positive than eSTC-negative patients for
HER2
-positive cancer [75.0% (3/4) vs. 12.5% (1/8),
p
= 0.066]. In luminal A [22.7% (5/22) vs. 10.0% (3/30),
p
= 0.259], luminal B [21.1% (4/19) vs. 6.7% (2/30),
p
= 0.189], and triple-negative [40.0% (2/5) vs. 11.8% (2/17),
p
= 0.209] cancers, distance metastasis was not associated with eSTCs. Median MFS was not reached in eSTC-positive and eSTC-negative patients. eSTC-positive patients had a higher risk of breast cancer metastasis [hazard ratio (HR) 3.57, 95% confidence interval (CI): 1.46-8.71;
p
= 0.001]. When tumor types were analyzed separately, a higher risk of breast cancer metastasis occurred only in
HER2
-positive patients (HR 8.49, 95% CI: 1.29-55.59;
p
= 0.016). Immunofluorescence analysis revealed mesenchymal-like STCs (mSTCs) and inter- and intra-tumor heterogeneity in STCs. There were breast tumors with either eSTCs or mSTCs and tumors with both types of STCs. Both eSTCs and mSTCs were represented by cells with different stem and/or EMT phenotypes.
Conclusions:
STCs with epithelial-like morphology contribute to breast cancer metastasis and represent an attractive model for studying mechanisms of metastatic seeding. The assessment of STCs in histological sections of breast tumors can be a simple and effective method for the prediction of metastasis risk.
...
PMID:Single Tumor Cells With Epithelial-Like Morphology Are Associated With Breast Cancer Metastasis. 3215 61
