| Literature DB >> 33344640 |
Zhuo-Yuan Chen1, Shang-Xing Sun2, Si-Xian Zhu3, Jie Bu4.
Abstract
BACKGROUND: As the important components in polycomb repressive complexes 1 (PRC1) and heterochromatin protein 1 (HP1), Chromobox (CBX) family members are involved in epigenetic regulatory function, transcriptional repression, and other cellular metabolisms. Increasing studies have indicated significant associations between CBX and tumorigenesis, which is a progression in different types of cancers. However, the information about the roles of each CBX in gastric cancer is extremely limited.Entities:
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Year: 2020 PMID: 33344640 PMCID: PMC7732380 DOI: 10.1155/2020/5306509
Source DB: PubMed Journal: Biomed Res Int Impact factor: 3.411
Figure 1Transcriptional levels of the CBX family members in different cancers (Oncomine, P value: 0.001 and fold − change : 1.5).
The transcription levels of CBX family members between different types of gastric cancers and normal gastric tissues (Oncomine).
| Types of gastric cancer vs. normal | Fold-change |
|
| Ref | PMID | |
|---|---|---|---|---|---|---|
| CBX1 | Gastric adenocarcinoma vs. normal | 2.415 | 6.913 | 4.52 | Cho gastric | 21447720 |
| Diffuse gastric adenocarcinoma vs. normal | 1.516 | 6.996 | 2.83 | Chen gastric | 12925757 | |
| Gastric mixed adenocarcinoma vs. normal | 1.66 | 7.026 | 2.25 | Chen gastric | 12925757 | |
| Gastric intestinal-type adenocarcinoma vs. normal | 1.613 | 9.531 | 2.38 | Chen gastric | 12925757 | |
| Gastric intestinal-type adenocarcinoma vs. normal | 2.116 | 10.157 | 2.21 | D'Errico gastric | 19081245 | |
| CBX2 | Diffuse gastric adenocarcinoma vs. normal | 2.29 | 6.862 | 6.01 | Cho gastric | 21447720 |
| Gastric mixed adenocarcinoma vs. normal | 2.077 | 4.349 | 3.75 | Cho gastric | 21447720 | |
| Gastric intestinal type adenocarcinoma vs. normal | 4.485 | 7.31 | 1.7 | D'Errico gastric | 19081245 | |
| CBX3 | Gastric mixed adenocarcinoma vs. normal | 1.998 | 8.875 | 1.62 | Chen gastric | 1292575 |
| Gastric intestinal-type adenocarcinoma vs. normal | 1.878 | 11.061 | 1.13 | Chen gastric | 12925757 | |
| Gastric intestinal-type adenocarcinoma vs. normal | 3.014 | 9.795 | 6.64 | D'Errico gastric | 19081245 | |
| Gastric cancer vs. normal | 1.736 | 3.719 | 6.79 | Wang gastric | 21132402 | |
| CBX4 | Gastric intestinal-type adenocarcinoma vs. normal | 1.783 | 10.753 | 2.55 | Chen gastric | 12925757 |
| Gastric mixed adenocarcinoma vs. normal | 1.955 | 8.08 | 3.03 | Chen gastric | 12925757 | |
| Diffuse gastric adenocarcinoma vs. normal | 1.73 | 4.295 | 4.23 | Chen gastric | 12925757 | |
| Diffuse gastric adenocarcinoma vs. normal | 2.466 | 4.862 | 2.45 | D'Errico gastric | 19081245 | |
| Gastric mixed adenocarcinoma vs. normal | 3.314 | 6.444 | 2.29 | D'Errico gastric | 19081245 | |
| Gastric mixed adenocarcinoma vs. normal | 1.625 | 3.633 | 7.18 | Cho gastric | 21447720 | |
| CBX5 | NA | NA | NA | NA | NA | NA |
| CBX6 | Diffuse gastric adenocarcinoma vs. normal | 1.758 | 4.643 | 8.38E-05 | Chen gastric | 12925757 |
| CBX7 | Diffuse gastric adenocarcinoma vs. normal | -1.656 | -4.072 | 9.09 | Cho gastric | 21447720 |
| CBX8 | NA | NA | NA | NA | NA | NA |
Figure 2mRNA and protein expression of CBXs (UALCAN and Human Protein Atlas): (a) mRNA expression of different CBXs in STAD and normal tissues (UALCAN, ∗P < 0.05, ∗∗P < 0.01, and ∗∗∗P < 0.001); (b) protein expression of different CBXs in GC and the normal tissues (Human Protein Atlas).
Figure 3Clinicopathological parameters and CBX mRNA levels in STAD patients (UALCAN): (a) correlation between the expression level of CBXs and nodal metastatic status in STAD patients (UALCAN, ∗P < 0.05, ∗∗P < 0.01, and ∗∗∗P < 0.001); (b) correlation between expression of CBXs and individual cancer stage in STAD patients (UALCAN, ∗P < 0.05, ∗∗P < 0.01, and ∗∗∗P < 0.001).
Figure 4Prognostic value of mRNA level of CBX family members in GC patients (Kaplan-Meier plotter, P < 0.05 was considered statistically significant).
Figure 5Genetic alterations, interactions, and enrichment analysis of CBXs in GC: (a) summary of CBX alteration in STAD; (b) alterations in CBXs in GC; (c) correction of CBXs with each other (cBioPortal); (d) interaction analysis of CBXs (GeneMANIA). Summary of alterations in CBXs in HCC: (e) GO enrichment analysis; (f) Reactome pathway prediction. BP: biological processes; CC: cellular components; MF: molecular functions.