Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
Restoration of Runx2 in miR-196a-knockdown HCC reverted tumor phenotypes.
|
31614906 |
2019 |
Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
<b>Materials and methods:</b> The levels of 3,4-dihydroxyphenylacetic acid, norepinephrine, serotonin, and 5-hydroxyindoleacetic acid in cancer tissue and in adjacent and non-oncological bone tissue were analysed by high-performance liquid chromatography, and the gene expression of catecholamine receptors and of dopamine β-hydroxylase, monoaminoxidase, ki67, and Runx2 in the osteosarcoma tissue, tissue adjacent to the tumour, non-oncological bone, and human brain tissue was analysed by RT-PCR.
|
31291139 |
2019 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
Moreover, increased RUNX2 expression levels were detected in recurrent CRC tumors, which were closely associated with TMN stages, metastasis, as well as CRC patients' survival.
|
31097689 |
2019 |
Neoplasms
|
0.100 |
GeneticVariation
|
group |
BEFREE |
Moreover, 10k possessing a favorable mouse pharmacokinetic profile prolonged life-span of Ba/F3-NRAS-G12D injected mice and significantly delayed tumor growth of OCI-AML3 xenograft model without causing the prominent level of toxicity found with GNF-7.
|
30153003 |
2018 |
Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
Besides, the RUNX2 function on tumor formation in vivo was investigated by tumor xenograft experiment.
|
30138923 |
2018 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
<i>Pten</i> knockout mice were used to examine the effect of <i>Runx2</i> heterozygous deletion or abiraterone acetate (ABA), a prodrug of the CYP17A1 inhibitor abiraterone on <i>Cyp11a1</i> and <i>Cyp17a1</i> expression, testosterone level and tumor microenvironment (TME) remodeling <i>in vivo</i><b>Results:</b> We uncovered that activation of the AKT-RUNX2-OCN-GPRC6A-CREB signaling axis induced expression of <i>CYP11A1</i> and <i>CYP17A1</i> and testosterone production in PTEN-null prostate cancer cell lines in culture.
|
29167276 |
2018 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
Taken together, our results indicate that miR-302b functions as a tumour repressor in the invasion and migration of osteosarcoma by directly downregulating Runx2 expression and may be a potential therapeutic target for osteosarcoma.
|
29042587 |
2017 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
Its expression in tumor tissue suggests a similar role for RUNX2 in the EMT of metastasis.
|
28631378 |
2018 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
Furthermore, analysis of LC3B protein in clinical breast cancer specimens and tumor xenografts revealed significant association between high Runx2 and low LC3B protein levels.
|
28345763 |
2018 |
Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
In this study, by using a non-contact co-culture system between human colorectal fibroblasts (CCD-18-co) and CRCs (LoVo, SW480, and SW620), we found that fibroblasts existing in tumor microenvironment positively influenced the metabolism of colorectal cancer cells, through its autophagy and oxidative stress pathway which were initially induced by neighboring tumor cells.
|
27841696 |
2017 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
High RUNX2 expression was correlated obviously with poor clinicopathological characteristics including multiple tumor nodes, high histological grading, venous infiltration and advanced tumor-node-metastasis (TNM) stage.
|
27666365 |
2016 |
Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
With TRβ as a tumor suppressor and Runx2 as a tumor promoter, a compelling question is whether there is a functional relationship between these regulatory factors in thyroid tumorigenesis.
|
27253998 |
2016 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
RUNX2 over-expression in LNCaP tumours in vivo decreased the time to tumour presentation and increased tumour growth.
|
26189652 |
2016 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
When expressed in prostate cell lines, wild-type Runx2 increased metastasis-associated gene expression, in vitro migratory and invasive activity as well as in vivo growth of tumor cell xenografts.
|
25867060 |
2016 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
The current study demonstrated that (1) Runx2 expression in primary human MM cells is significantly greater than in plasma cells from healthy donors and patients with monoclonal gammopathy of undetermined significance; (2) high levels of Runx2 expression in MM cells are associated with a high-risk population of MM patients; and (3) overexpression of Runx2 in MM cells enhanced tumor growth and disease progression in vivo.
|
25862559 |
2015 |
Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
These results support a hypothesis whereby RUNX2-mediated repression of the SIRT6 tumor suppressor regulates metabolic pathways that promote BC progression.
|
25808624 |
2015 |
Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
Therefore, our goal was to evaluate the potential for clinical use of Runx2-targeting miRNAs to reduce tumor growth and bone metastatic burden.
|
25634212 |
2015 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
Runx-2, BMP-2, and CAP were abundantly expressed by POFs; 22 of 30 tumors expressed positive staining for Runx-2, twenty-six tumors for BMP-2, and twenty-five tumors for CAP.
|
25359431 |
2015 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
The median expression levels of RUNX2 and miR-10b in tumor tissue normalized using adjacent non-tumor tissue were significantly higher in relapsed patients than in relapse-free patients.
|
25266482 |
2014 |
Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
In vivo, NSG mice tail veins injected with OCI-AML3-luc+ cells showed significantly lower tumor burden following 1 week of daily oral administration of 50 mg/kg NVP-AEW541 (IGF1R inhibitor) combined with 25 mg/kg AZD6244 (MEK inhibitor), as compared with mice treated with either agent alone.
|
25186968 |
2014 |
Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
Intratibial tumors generated from these cells revealed that Runx2-WT-expressing cells resulted in predominantly osteolytic disease, whereas cells expressing mutant proteins exhibited tumors with mixed osteolytic/osteoblastic lesions.
|
25053011 |
2015 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
Moreover, RUNX2 displayed significantly higher expression not only in metastatic tissue, but also in high-grade primary tumors and even in low malignant potential tumors.
|
24124450 |
2013 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
Hypoxia increased RUNX2 expression in vitro, and bicalutamide-treated LNCaP tumours in mice (previously shown to have increased tumour hypoxia) exhibited increased RUNX2 expression.
|
23073173 |
2012 |
Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
Immunohistochemistry analysis of tissue microarray sections containing primary prostatic tumor (grade2-4) detected predominant localization of RUNX2 and phosphorylated Smad 5 in the nuclei.
|
22966907 |
2012 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
We identified 10 genes, including the transcription factor Runx2, a transcriptional partner of Yes-associated protein (YAP1) that displays tumor suppressive activity through competing with the oncogenic TEA domain family of transcription factors (TEAD) for YAP1 association.
|
22710434 |
2012 |