Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
Compared with other endometrial cancers, POLE mutants displayed an enhanced cytotoxic T-cell response, evidenced by increased numbers of CD8(+) tumor-infiltrating lymphocytes and CD8A expression, enrichment for a tumor-infiltrating T-cell gene signature, and strong upregulation of the T-cell cytotoxic differentiation and effector markers T-bet, Eomes, IFNG, PRF, and granzyme B.
|
25878334 |
2015 |
Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
Of the 647 treated women (mean [SD] age, 55.0 [10.8] years), 614 had tumor tissue samples scored for H&E sTILs and 427 for CD8 biomarker assessments.
|
28750133 |
2017 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
LyP-1, a tumor homing peptide, can selectively bind to its receptor p32 protein overexpressed in various tumor-associated cells and atherosclerotic plaque macrophages.
|
30905205 |
2019 |
Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
Because of these results and that no mutations were detected on the two genes in a previous study, we think that Leu1 and Leu2 can be excluded as tumor suppressor genes.
|
10516767 |
1999 |
Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
FFPE sections were macrodissected to enrich for tumor for quantitative assessment of CD274 (PD-L1), PDCD1LG2 (PD-L2), CD8A, and IRF1 by RT-qPCR multiplex mRNA panel.
|
31533832 |
2019 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
Analysis of tumour CD8A expression in the independent validation cohort revealed similar variation in prognostic value across risk strata (P<sub>INTERACTION</sub> = 0.048).
|
31388185 |
2019 |
Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
The bispecific antibodies simultaneously engaged the cognate antigens (murine T cell co-receptor CD3 and hen egg lysozyme) and selectively accumulated on murine tumors in vivo.
|
23032949 |
2014 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
The multi-compartment protein p32 is overexpressed and present at cell surfaces in a variety of tumors, including TNBC, specifically in the malignant cells and endothelial cells, and in macrophages localized in hypoxic areas of the tumor.
|
29721153 |
2018 |
Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
A DOX-loaded polysaccharide-lecithin reverse micelles triglyceride-based oral delivery nanocarrier (D-PL/TG NPs) conjugated with (i) RGD peptide for targeting to β1 integrin of M cells and (ii) Lyp-1 peptide for targeting to the p32 receptor of MDA-MB-231 cells is used to investigate the multistage continuous targeting capabilities of these peptide-conjugated nanocarriers (GLD-PL/TG NPs) for tumor therapy.
|
27634372 |
2017 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
We first demonstrated that the primary homing receptor for linTT1, p32 (or gC1qR), is expressed on the cell surface of peritoneal carcinoma cell lines of gastric (MKN-45P), ovarian (SKOV-3), and colon (CT-26) origin, and that peritoneal tumors in mice and clinical peritoneal carcinoma explants express p32 protein accessible from the IP space.
|
28603028 |
2017 |
Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
We conclude that the Leu1 and Leu2 genes are strong candidates as tumor suppressor gene(s) involved in B-CLL leukemogenesis.
|
9395242 |
1997 |
Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
Two-sided Wilcoxon rank-sum tests showed that: 1) EBV-positive tumors had low mutation burden (median = 2.07 vs 3.13 in log10 scale, P < 10-12) but stronger evidence of immune infiltration (median ImmuneScore 2212 vs 1295, P < 10-4; log2 fold-change of CD8A = 1.85, P < 10-6) compared with MSI tumors, and 2) EBV-positive tumors had higher expression of immune checkpoint pathway (PD-1, CTLA-4 pathway) genes in RNA-seq data (log2 fold-changes: PD-1 = 1.85, PD-L1 = 1.93, PD-L2 = 1.50, CTLA-4 = 1.31, CD80 = 0.89, CD86 = 1.31, P < 10-4 each), and higher lymphocytic infiltration by histology (median tumor-infiltrating lymphocyte score = 3 vs 2, P < .001) compared with MSS tumors.
|
29155997 |
2018 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
Attenuation of p32 expression reduced growth rate of glioma cells expressing Myc and impaired tumor formation in vivo.
|
25528767 |
2015 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
The gene expression of CD4, CD8A and forkhead box protein P3 in the tumor was increased compared with healthy breast tissue, and was positively associated with the prognosis of breast cancer patients.
|
30221739 |
2018 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
CD8A expression was significantly upregulated in POLE category tumors compared with that in nonhypermutators.
|
31240875 |
2019 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
In contrast, we observed decreased HLA-A, -B, and -C expression (<i>p</i> = 0.036, <i>p</i> = 0.026, and <i>p</i> = 0.030, respectively) as well as increased ratios of CTLA-4, PD-1, Tim-3, and LAG3 to CD8A expression (<i>p</i> = 0.0064, <i>p</i> = 0.017, <i>p</i> = 0.033 and <i>p</i> = 0.0136, respectively) in stage I-II tumors with high neoAg frequencies.
|
28920005 |
2017 |
Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
After primary tumour removal, a course of three subcutaneous vaccinations with LLC lysate supplemented with BGs led to a significant increase in overall survival (80% after 84 days of follow‑up vs. 40% in untreated control mice), a significant increase in circulating CD8a+ T cells (16.57 vs. 12.6% in untreated control mice) and a significant decrease in metastasis foci area and incidence.
|
27878261 |
2017 |
Neoplasms
|
0.100 |
Biomarker
|
group |
BEFREE |
<b>Methods:</b> Seven syngeneic mouse tumor models (B16F10, P815, CT26, MC38, Renca, 4T1, Sa1N) were quantified for CD4<sup>+</sup> and CD8a<sup>+</sup> TILs using flow cytometry and immunohistochemistry (IHC), as well as for tumor growth response to Sym021, a humanized PD-1 antibody cross-reactive with mouse PD-1<b>.</b> Radiotracers were generated from F(ab)'2 fragments of rat-anti-mouse CD4 and CD8a antibodies conjugated to the <i>p</i>-SCN-Bn-Desferrioxamine (SCN-Bn-DFO) chelator and radiolabeled with Zirconium-89 (<sup>89</sup>Zr-DFO-CD4/<sup>89</sup>Zr-DFO-CD8a).
|
31754392 |
2019 |
Neoplasms
|
0.100 |
AlteredExpression
|
group |
BEFREE |
LyP-1-SPIONs are promising in treating cancer as they accumulated in the nucleus of MCF-7 cells which expressed p32 and almost stopped tumor growth by combined MIH and targeted therapy.
|
29165044 |
2018 |
Malignant Neoplasms
|
0.080 |
AlteredExpression
|
group |
BEFREE |
LyP-1-SPIONs are promising in treating cancer as they accumulated in the nucleus of MCF-7 cells which expressed p32 and almost stopped tumor growth by combined MIH and targeted therapy.
|
29165044 |
2018 |
Malignant Neoplasms
|
0.080 |
AlteredExpression
|
group |
BEFREE |
Identifying small molecule inhibitors of p32 overexpressed in cancer is a more rational therapeutic strategy.
|
29047383 |
2017 |
Malignant Neoplasms
|
0.080 |
Biomarker
|
group |
BEFREE |
The Cancer Genome Atlas analysis confirmed that patients with a favorable immune and metabolic gene signature (high CD8A, high COX5B, low GLUT1) had improved short- and long-term survival.
|
29107073 |
2018 |
Malignant Neoplasms
|
0.080 |
Biomarker
|
group |
BEFREE |
Within the knowledge of the critical role of p32 receptor in cancer cell metabolism, this study can lead to further developments in anticancer therapy by targeting p32 with LyP-1 derivatives as active targeting moiety.
|
28427307 |
2018 |
Malignant Neoplasms
|
0.080 |
AlteredExpression
|
group |
BEFREE |
LyP-1 is a peptide that binds to the p32 receptor which is highly expressed not only on the lymphatic endothelium but also on the malignant cells; thus, making this peptide ligand a preferable candidate to mediate active targeting of lymphatics and cancer cells.
|
30660694 |
2019 |
Malignant Neoplasms
|
0.080 |
Biomarker
|
group |
BEFREE |
<b>Materials and methods:</b> In the present study, we reanalyzed data from four public datasets (the Cancer Genome Atlas for investigation; and CIT, GSE5287, and GSE31684 for validation) to examine the prognostic significance of CD3D, CD4, CD8A, CD3D/CD4 and CD3D/CD8A in MIBC.
|
31114346 |
2019 |